Robbins Essential Pathology [1 ed.] 9780323640251
Cleaned version with corrected pagination and bookmarks.
250 6 76MB
English Pages 340 [447] Year 2020
Cover
Inside Front Cover
Title Page
Robbins Essential Pathology
Copyright
Preface
Acknowledgments
Contents
Chapter 1: Cell Injury and Cell Death
Overview of Cell Injury
Causes of Cell Injury
Reversible Cell Injury
Cell Death
Necrosis
Apoptosis
Causes of Apoptosis
Mechanisms of Apoptosis
Other Pathways of Cell Death
Mechanisms of Cell Injury and Death
Oxidative Stress
Hypoxia and Ischemia
Ischemia–Reperfusion Injury
Toxin-Mediated Cell Injury
Endoplasmic Reticulum (ER) Stress
DNA Damage
Cellular Aging
Cellular Adaptations to Stress
Pathologic Accumulations in Cells
Chapter 2: Inflammation and Repair
Overview of Inflammation
Causes of Inflammation
Sequence of Events in Inflammation
Features of Acute and Chronic Inflammation
Cells of Inflammation
Acute Inflammation
Vascular Reactions
Cellular Reactions
Resolution of Acute Inflammation
Mediators of Inflammation
Clinicopathologic Features of Acute Inflammation
Outcomes of Acute Inflammation
Chronic Inflammation
Cellular Reactions of Chronic Inflammation
Clinicopathologic Features of Chronic Inflammation
Systemic Manifestations
Tissue Repair
Angiogenesis
Clinicopathologic Features of Tissue Repair
Chapter 3: Hemodynamic Disorders, Thromboembolism, and Shock
Hyperemia, Congestion, and Edema
Edema
Hemostasis and Hemorrhage
Platelets
Coagulation Cascade
Coagulation Control
Thrombosis
Embolism
Pulmonary Thromboembolism
Systemic Thromboembolism
Nonthrombotic Emboli
Infarction
Shock
Septic Shock
Chapter 4: Diseases of the Immune System
Hypersensitivity Disorders
Immediate (Type I) Hypersensitivity
Antibody-Mediated (Type II) Hypersensitivity
Activation and Functions of Complement
Immune Complex–Mediated (Type III) Hypersensitivity
T Cell-Mediated (Type IV) Hypersensitivity
Autoimmune Diseases
Mechanisms of Autoimmunity
Genetic Susceptibility
Environmental Factors
Systemic Lupus Erythematosus (SLE)
Systemic Sclerosis (Scleroderma)
Sjögren Syndrome
Rejection of Transplants
Immune Responses to Organ Allografts
Mechanisms of Rejection of Solid-Organ Allografts
Treatment of Graft Rejection
Hematopoietic Stem Cell Transplantation
Immunodeficiency Disorders
Primary (Congenital) Immunodeficiencies
Acquired Immunodeficiency Syndrome
Human Immunodeficiency Virus: Structure and Life Cycle
Amyloidosis
Chapter 5: Neoplasia
Definition of Neoplasia
Benign and Malignant Neoplasms
Nomenclature
Nomenclature of Benign Tumors
Nomenclature of Malignant Tumors
Characteristics of Benign and Malignant Neoplasms
Differentiation of Neoplasms
Local Invasion
Metastasis
Molecular Basis of Neoplasia
Cancer Genes and “Driver” Mutations
Epigenetic Alterations in Cancer
Carcinogenesis: A Multistep Process Directed by Darwinian Evolution
Origin of Carcinogenic Mutations
Role of Infectious Agents in Cancer
Significance of Passenger Mutations
Hallmarks of Cancer
Self-Sufficiency in Growth Signals
Insensitivity to Growth-Inhibitory Signals
RB: Governor of Cellular Proliferation
TP53: Guardian of the Genome
Cell Lineage–Specific Tumor Suppressor Genes
Altered Cellular Metabolism
Evasion of Cell Death
Limitless Replicative Potential (Immortality)
Sustained Angiogenesis
Invasion and Metastasis
Invasion of the Extracellular Matrix
Vascular Dissemination and Homing of Tumor Cells
Metastasis
Evasion of Immune Surveillance
Tumor Antigens
Immune Mechanisms of Tumor Destruction
Immune Escape
Genomic Instability as an Enabler of Malignancy
Hereditary Nonpolyposis Colon Cancer Syndrome
Xeroderma Pigmentosum
Diseases with Defects in DNA Repair by Homologous Recombination
Tumor-Promoting Inflammation as an Enabler of Malignancy
Clinical Aspects of Neoplasia
Clinical Effects of Tumors
Grading and Staging of Cancer
Cancer Diagnosis
Morphologic Methods
Protein Markers
Cytogenetic Markers
Nucleic Acid Markers
Chapter 6: Genetic Diseases
Mendelian Disorders: Diseases Caused by Single-Gene Defects
Transmission Patterns of Single-Gene Disorders
Autosomal Dominant Disorders
Disorders of Autosomal Recessive Inheritance
X-Linked Disorders
Diseases Caused by Mutations in Genes Encoding Structural Proteins
Marfan Syndrome
Ehlers-Danlos Syndromes
Diseases Caused by Mutations in Genes Encoding Receptor Proteins or Channels
Familial Hypercholesterolemia
Cystic Fibrosis
Diseases Caused by Mutations in Genes Encoding Enzyme Proteins
Phenylketonuria
Lysosomal Storage Diseases
Niemann-Pick Disease Types A and B
Niemann-Pick Disease Type C
Gaucher Disease
Mucopolysaccharidoses
Glycogen Storage Diseases (Glycogenoses)
Complex Multigenic Disorders
Cytogenetic Disorders
Numerical Abnormalities
Structural Abnormalities
Cytogenetic Disorders Involving Autosomes
Trisomy 21 (Down Syndrome)
22q11 Deletion Syndrome
Cytogenetic Disorders Involving Sex Chromosomes
Klinefelter Syndrome
Turner Syndrome
Single-Gene Disorders with Atypical Patterns of Inheritance
Trinucleotide Repeat Mutation Diseases
Diseases Caused by Mutations in Mitochondrial Genes
Diseases Caused by Alterations of Imprinted Regions: Prader-Willi and Angelman Syndromes
Diagnosis of Genetic Disorders
Genetic Test Modalities and Applications
Indications for Genetic Analysis
Chapter 7: Diseases of Blood Vessels
Mechanisms of Vascular Diseases
Congenital Vascular Anomalies
Hypertension
Atherosclerosis
Aneurysms and Dissections
Aortic Aneurysms
Aortic Dissections
Vasculitis
Giant Cell (Temporal) Arteritis
Takayasu Arteritis
Polyarteritis Nodosa
Kawasaki Disease
Thromboangiitis Obliterans (Buerger Disease)
Small-Vessel Vasculitides
Infectious Vasculitis
Disorders of Veins
Varicose Veins
Thrombophlebitis
Tumors of Blood Vessels and Lymphatics
Hemangiomas
Kaposi Sarcoma
Angiosarcomas
Chapter 8: Heart
Congenital Heart Disease
Malformations Associated with Left-to-Right Shunts
Atrial Septal Defects and Patent Foramen Ovale
Ventricular Septal Defects
Patent Ductus Arteriosus
Malformations Associated with Right-to-Left Shunts
Tetralogy of Fallot
Transposition of the Great Vessels
Malformations Leading to Obstruction
Aortic Coarctation
Ischemic Heart Disease
Angina Pectoris
Myocardial Infarction
Chronic Ischemic Heart Disease
Arrhythmia
Hypertensive Heart Disease
Systemic (Left-Sided) Hypertensive Heart Disease
Right-Sided (Pulmonary) Hypertensive Heart Disease
Valvular Heart Disease
Degenerative Valve Disease
Calcific Aortic Degeneration
Myxomatous Mitral Valve Disease
Rheumatic Valvular Disease
Infective Endocarditis
Nonbacterial Thrombotic Endocarditis
Cardiomyopathies and Myocarditis
Dilated Cardiomyopathy
Hypertrophic Cardiomyopathy
Restrictive Cardiomyopathy
Myocarditis
Other Causes of Myocardial Disease
Congestive Heart Failure
Left-Sided Heart Failure
Right-Sided Heart Failure
Cardiac Tumors
Chapter 9: Hematopoietic and Lymphoid Systems
Red Blood Cell Disorders
Anemias
Hemolytic Anemias
Hereditary Spherocytosis
Sickle Cell Anemia
Thalassemias
Glucose-6-Phosphate Dehydrogenase (G6PD) Deficiency
Immunohemolytic Anemia
Hemolytic Disease of the Fetus and Newborn
Mechanical Trauma to Red Cells
Malaria
Underproduction Anemias
Anemia of Chronic Inflammation
Iron Deficiency Anemia
Folate and Vitamin B12 Deficiency Anemias (Megaloblastic Anemias)
Aplastic Anemia
Anemia due to Marrow Infiltration
White Blood Cell Disorders
Nonneoplastic Disorders of White Cells
Leukopenia
Reactive Leukocytosis
Infectious Mononucleosis
Reactive Lymphadenitis
Neoplastic Proliferations of White Cells
Acute Leukemias
Myelodysplastic Syndromes
Myeloproliferative Neoplasms
Chronic Myeloid Leukemia
Polycythemia Vera
Primary Myelofibrosis
Non-Hodgkin Lymphomas and Chronic Lymphoid Leukemias
Chronic Lymphocytic Leukemia/Small Lymphocytic Lymphoma
Follicular Lymphoma
Mantle Cell Lymphoma
Extranodal Marginal Zone Lymphoma
Diffuse Large B Cell Lymphoma
Burkitt Lymphoma
Other Neoplasms of Mature Lymphoid Cells
Hodgkin Lymphoma
Plasma Cell Neoplasms and Related Entities
Multiple Myeloma
Other Plasma Cell Neoplasms and Related Entities
Histiocytic Neoplasms
Bleeding Disorders
Thrombocytopenia
Immune Thrombocytopenic Purpura
Heparin-Induced Thrombocytopenia
Thrombotic Microangiopathies
Coagulation Disorders
Von Willebrand Disease
Hemophilia A
Hemophilia B–Factor IX Deficiency
Disseminated Intravascular Coagulation
Disorders of Spleen and Thymus
Splenomegaly
Disorders of the Thymus
Thymic Follicular Hyperplasia
Thymoma
Chapter 10: Lung and Upper Respiratory Tract
Acute Respiratory Distress Syndrome
Obstructive Lung Diseases
Chronic Obstructive Pulmonary Disease
Asthma
Bronchiectasis
Restrictive Lung Diseases
Fibrosing Diseases
Idiopathic Pulmonary Fibrosis
Pneumoconioses
Silicosis
Asbestosis
Granulomatous Diseases
Sarcoidosis
Hypersensitivity Pneumonitis
Pulmonary Diseases of Vascular Origin
Pulmonary Embolism, Hemorrhage, and Infarction
Pulmonary Hypertension
Diffuse Alveolar Hemorrhage Syndromes
Goodpasture Syndrome
Granulomatosis and Polyangiitis
Pulmonary Infections
Community-Acquired Bacterial Pneumonias
Nosocomial Bacterial Pneumonias
Aspiration Pneumonias
Lung Abscess
Tuberculosis
Community-Acquired Viral Pneumonias
Influenza
Fungal Infections
Histoplasmosis, Coccidioidomycosis, and Blastomycosis
Opportunistic Infections
Cytomegalovirus Infection
Pneumocystis Infection
Candidiasis
Cryptococcosis
Opportunistic Molds
Lung, Pleural, and Upper Airway Tumors
Lung Carcinoma
Carcinoid Tumors
Malignant Mesothelioma
Nasopharyngeal Carcinoma
Carcinoma of the Larynx
Chapter 11: Kidney
Overview of Renal Diseases
Diseases of Glomeruli
Mechanisms of Glomerular Injury
Minimal Change Disease
Membranous Nephropathy
Focal Segmental Glomerulosclerosis
Membranoproliferative Glomerulonephritis
C3 Glomerulopathies
Diabetic Nephropathy
Acute Poststreptococcal Glomerulonephritis
Lupus Nephritis
Rapidly Progressive Glomerulonephritis
IgA Nephropathy
Hereditary Nephritis
Diseases of Tubules and Interstitium
Acute Pyelonephritis
Chronic Pyelonephritis
Drug-Induced Tubulointerstitial Nephritis
Acute Tubular Injury
Cystic Diseases
Autosomal Dominant Polycystic Kidney Disease
Autosomal Recessive Polycystic Kidney Disease
Other Cystic Kidney Diseases
Diseases of Blood Vessels
Nephrosclerosis
Malignant Hypertension
Thrombotic Microangiopathies
Renal Stones (Urolithiasis)
Hydronephrosis
Tumors of the Kidney
Renal Cell Carcinoma
Wilms Tumor
Chapter 12: Gastrointestinal System
Congenital Anomalies of the Gastrointestinal Tract
Disorders of the Esophagus
Esophageal Obstruction
Esophageal Varices
Esophagitis
Reflux Esophagitis (Gastroesophageal Reflux Disease)
Barrett Esophagus
Eosinophilic Esophagitis
Chemical and Infectious Esophagitis
Esophageal Lacerations
Esophageal Tumors
Disorders of the Stomach
Gastritis and Peptic Ulcer Disease
Acute Gastritis
Stress-Related Gastritis
Helicobacter pylori Gastritis
Autoimmune Gastritis
Peptic Ulcer Disease
Tumors of the Stomach
Gastric Polyps and Adenomas
Gastric Adenocarcinoma
Gastric Lymphoma
Neuroendocrine Tumors (Carcinoid Tumors)
Gastrointestinal Stromal Tumor
Disorders of the Small and Large Intestines
Diarrheal Diseases
Malabsorptive and Osmotic Diarrhea
Infectious Diarrhea
Inflammatory Bowel Disease
Crohn Disease
Ulcerative Colitis
Other Inflammatory Diseases
Celiac Disease (Gluten Enteropathy)
Sigmoid Diverticulitis
Appendicitis
Necrotizing Enterocolitis
Tumors and Related Conditions of the Intestines
Polyps
Adenomas
Adenocarcinoma
Obstructive and Vascular Diseases
Intestinal Obstruction
Vascular Diseases
Disorders of the Oral Cavity and Salivary Glands
Inflammatory Disorders of the Oral Cavity
Tumors and Tumor-like Lesions of the Oral Cavity
Diseases of the Salivary Glands
Chapter 13: Liver, Biliary System, and Pancreas
Disorders of the Liver
Clinical Consequences of Liver Disease
Viral Hepatitis
Hepatitis A Virus
Hepatitis B Virus
Hepatitis C Virus
Hepatitis D Virus
Hepatitis E Virus
Other Infections of the Liver
Alcoholic Liver Disease
Nonalcoholic Fatty Liver Disease
Other Forms of Hepatitis
Autoimmune Hepatitis
Drug- and Toxin-Induced Hepatitis
Inherited Diseases of the Liver
Hemochromatosis
Wilson Disease
α1-Antitrypsin Deficiency
Circulatory Disorders of the Liver
Nodules and Tumors of the Liver
Focal Nodular Hyperplasia
Hepatic Adenoma
Hepatocellular Carcinoma
Cholangiocarcinoma
Disorders of the Biliary System
Cholangitis
Primary Biliary Cholangitis
Primary Sclerosing Cholangitis
Congenital Disorders Causing Jaundice
Cholelithiasis and Cholecystitis
Cholelithiasis
Cholecystitis
Tumors of the Biliary System
Cholangiocarcinoma
Carcinoma of the Gallbladder
Disorders of the Pancreas
Pancreatitis
Acute Pancreatitis
Chronic Pancreatitis
Pseudocyst
Tumors of the Pancreas
Cystic Tumors
Adenocarcinoma
Chapter 14: Male Genital Tract, Prostate, and Bladder
Penis
Malformations and Inflammatory Lesions
Neoplasms
Scrotum, Testis, and Epididymis
Cryptorchidism
Infections
Testicular Neoplasms
Prostate
Benign Prostatic Hyperplasia
Carcinoma of the Prostate
Ureter, Bladder, and Urethra
Ureter
Urinary Bladder
Bladder Cancer
Sexually Transmitted Diseases
Syphilis
Gonorrhea
Nongonococcal Urethritis and Cervicitis
Trichomoniasis
Genital Herpes Simplex
Human Papillomavirus (HPV) Infection
Chapter 15: Female Genital Tract and Breast
Vulva
Vulvitis
Tumors
Condyloma Acuminatum
Carcinoma of the Vulva
Vagina
Vaginitis
Cervix
Cervicitis
Neoplasia of the Cervix
Squamous Intraepithelial Lesion
Invasive Carcinoma of the Cervix
Uterus
Endometritis
Endometriosis
Abnormal Uterine Bleeding
Proliferative Lesions of the Endometrium and Myometrium
Endometrial Hyperplasia
Endometrial Carcinoma
Leiomyoma
Leiomyosarcoma
Fallopian Tubes
Ovaries
Tumors of the Ovary
Surface Epithelial Tumors
Other Ovarian Tumors
Diseases of Pregnancy
Placental Inflammations and Infections
Ectopic Pregnancy
Gestational Trophoblastic Disease
Hydatidiform Mole: Complete and Partial
Gestational Choriocarcinoma
Preeclampsia and Eclampsia
Breast
Inflammatory Processes
Stromal Neoplasms
Benign Epithelial Lesions
Carcinoma
Epidemiology
Chapter 16: Endocrine System
Overview of the Endocrine System
Pituitary Gland
Hyperpituitarism
Lactotroph Adenoma
Somatotroph Adenoma
Corticotroph Adenoma
Other Pituitary Adenomas
Hypopituitarism
Posterior Pituitary Syndromes
Craniopharyngioma
Thyroid
Clinical Syndromes of Thyroid Dysfunction
Hyperthyroidism
Hypothyroidism
Autoimmune Thyroid Disease
Chronic Lymphocytic (Hashimoto) Thyroiditis
Graves Disease
Other Forms of Inflammatory Thyroid Disease
Goiter
Tumors of the Thyroid Gland
Thyroid Adenoma
Thyroid Carcinoma
Parathyroid Glands
Endocrine Pancreas: Diabetes
Overview of Diabetes
Insulin Physiology
Pathogenesis of Diabetes
Type 1 Diabetes
Type 2 Diabetes
Other Forms of Diabetes
Clinicopathologic Features of Diabetes
Vascular Lesions
Diabetic Nephropathy
Diabetic Retinopathy
Diabetic Neuropathy
Acute Diabetic Ketoacidosis and Nonketotic Hyperosmolar Coma
Adrenal Glands
Cushing Syndrome: Hypercortisolism
Hyperaldosteronism
Adrenogenital Syndromes
Adrenal Cortical Insufficiency
Chronic Adrenal Insufficiency (Addison Disease)
Acute Adrenal Insuficiency
Tumors of the Adrenal Medulla
Pheochromocytoma
Neuroblastoma
Multiple Endocrine Neoplasia Syndromes
Chapter 17: Disorders of the Nervous System
Congenital Malformations of the CNS
Cerebral Edema, Herniation, and Hydrocephalus
Cerebrovascular Diseases
Cerebral Artery Thrombosis, Embolism, and Brain Infarction
Intracranial Hemorrhage
Other Vascular Diseases
CNS Trauma
Parenchymal Brain Injury
Chronic Traumatic Encephalopathy
Perinatal Brain Injury
CNS Infections
Prion Diseases
Demyelinating Diseases
Multiple Sclerosis
Other Acquired Demyelinating Disorders
Leukodystrophies
Neurodegenerative Diseases
Alzheimer Disease
Frontotemporal Lobar Degeneration (FTLD)
Parkinson Disease
Huntington Disease
Spinocerebellar Ataxias
Amyotrophic Lateral Sclerosis
CNS Tumors
General Features and Pathogenesis of Astrocytoma
Classification of Astrocytomas
Other CNS Tumors
Inherited Syndromes Associated with CNS Tumors
Retinoblastoma
Disorders of Peripheral Nerves
Peripheral Neuropathy
Peripheral Nerve Tumors
Diseases of Neuromuscular Junctions
Chapter 18: Musculoskeletal System and Skin
Bones
Congenital Disorders
Dwarfism
Osteogenesis Imperfecta
Osteopetrosis
Metabolic Diseases
Osteoporosis
Rickets and Osteomalacia
Hyperparathyroidism
Paget Disease of Bone
Fractures and Avascular Necrosis
Fractures
Avascular Necrosis of Bone
Osteomyelitis
Acute Pyogenic Osteomyelitis
Tuberculous Osteomyelitis
Tumors
Osteochondroma
Giant Cell Tumor
Osteosarcoma
Chondrosarcoma
Ewing Sarcoma
Metastatic Tumors
Joints
Arthritis
Osteoarthritis
Rheumatoid Arthritis
Other Forms of Arthritis
Gout
Calcium Pyrophosphate Crystal Deposition Disease
Skeletal Muscle
Muscular Dystrophies
Duchenne Muscular Dystrophy and Becker Muscular Dystrophy
Myositis
Tumors of Muscle and Soft Tissue
Skin
Acute Inflammatory Dermatoses
Acute Eczematous Dermatitis
Erythema Multiforme
Chronic Inflammatory Dermatoses
Psoriasis
Blistering (Bullous) Disorders
Pemphigus (Vulgaris and Foliaceus)
Bullous Pemphigoid
Dermatitis Herpetiformis
Tumors
Squamous Cell Carcinoma
Basal Cell Carcinoma
Melanoma
Chapter 19: Environmental Disease
Metals as Environmental Pollutants
Lead
Mercury
Tobacco
Alcohol
Injury by Therapeutic Drugs and Drugs of Abuse
Injury by Therapeutic Drugs: Adverse Drug Reactions
Menopausal Hormone Therapy (MHT)
Oral Contraceptives (OCs)
Injury by Drugs of Abuse
Opioids
Cocaine
Marijuana
Injury Produced by Ionizing Radiation
Acute and Chronic Effects of Radiation on Organ Systems
Nutritional Diseases
Malnutrition
Severe Acute Malnutrition
Vitamin Deficiencies
Vitamin A
Vitamin D
Vitamin C (Ascorbic Acid)
Obesity
Index
a
B
C
D
E
F
G
H
I
J
K
L
M
N
O
P
R
S
T
U
V
W
X
Y
Z
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RO B B I N S
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RO B B I N S
ES S ENTIA L
PAT H O LO GY Vinay
A lice
Kumar,
Hogge
a nd
Depa r t ment
Biolog ic
of
Prit zker
The
Universit y
Chicago,
Abul
K.
Universit y
C.
Professor
Brig ha m
Boston,
of
Med ici ne
Chicago
Emeritus
Pat holog y
Ca lifornia
Sa n
Fra ncisco
Ca lifornia
Aster,
of
MBBS
Cha irma n
of
of
MD,
PhD
Pat holog y
a nd
Women’s
Med ica l
Hospita l
School
Massachuset ts
Andrea
A ssociate
T.
Deyrup,
of
Pat holog y
Universit y
Durha m,
MD,
Professor
Depa r t ment
Du ke
of
Abbas,
Fra ncisco,
Ha r va rd
FRCPath
Dist i ng uished
Div ision
School
a nd
Depa r t ment
Jon
MD,
Baer
Il li nois
Professor
Sa n
A.
Pat holog y
Science
The
MBBS ,
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ESSENTIAL
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To
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us.
C O N T E N T S
1
Cell
Injury
and
2
Inflammation
3
Hemodynamic
4
Diseases
5
Neoplasia,
6
Genetic
7
Diseases
8
Heart,
9
Hematopoietic
of
Cell
and
the
Immune
Diseases,
of
Blood
14
Thromboembolism,
System,
and
41
88
Vessels,
105
118
and
and
11
Kidney,
12
Gastrointestinal
13
Liver,
Biliary
14
Male
Genital
15
Female
16
Endocrine
17
Disorders
18
Musculoskeletal
19
Environmental
viii
1
63
Lung
327
Repair,
Disorders,
10
Index,
Death,
Upper
Lymphoid
Respiratory
Systems,
Tract,
137
163
186
System,
System,
Tract,
Genital
of
the
and
Pancreas,
Prostate,
Tract
System,
205
and
and
Breast,
222
Bladder,
250
264
Nervous
System
Disease,
System,
and
314
280
Skin,
296
240
Shock,
30
1
Cell
Injury
and
Cell
Death
O U T L I N E
Overview
of
Causes
Reversible
Cell
Cell
of
Cell
Death,
oer
sck
a
on
Cell
Injury
dseases
advances
e
cell
er
aler
e
Death,
and
s
n
e
cells
o
cells
sck.
bolog y
rs
o
s
“evl
unconal
all
One
medcne
un
sare
e
“masma, ”
o
was
o
dseases:
srucure.
an
umors, ”
causes.
and
dseases
and
medcne
s
and
All
8
Injury,
Reticulum
9
(ER)
Stress,
9
9
Aging,
9
Pathologic Accumulations in Cells, 12
underle
uncon
and
eme
n
7
unprovable
srucural
Cell
Cellular Adaptations to Stress, 11
arbued
and
uman
are
cellular
6
Death,
were
nebulous
paoog y
njured,
Cell
abnormales
ey
o
of
7
Ischemia,
Damage,
Cellular
mes,
because
Stress,
and
Toxin-Mediated
3
equally
a
and
1
DNA
of
undamenal
sms
Injury,
Pathways
medeval
zaon
Hypoxia
3
Mechanisms
and
Oxidative
1
Endoplasmic
Apoptosis,
In
1
Injury,
2
Necrosis,
Other
Injury,
Cell
e
e
lvng
ereore,
undersandng
o
e
aso
real-
organ-
Indvduals
common
bo
mos
bud
ces
are
o
oxygen
and,
nurens
and
n
e
oxc
case
o
scema,
meaboes
are
ces
are
aowed
o
up
Toxns, wc abound n e envronmen, as we as some terapeu-
•
Envronmenta nsuts, suc as pysca rauma, radaon exposure,
•
Genetc abnormates, ncudng muaons a mpar e uncon
tc
ounda-
ow
ssues
essena
•
are
eaure
deprve
dened
drugs
and
caper.
o
nurona
varous
mbaances
essena
accumuaon
o
proens
damaged
and
DNA
oer
or
muaons
abnorma,
a
ead
msoded
o
e
proens,
bo o wc cause ce dea ey canno be repared or correced
OVERVIEW
OF
CELL
INJURY •
In
response
and
recover,
Ces
beng
Ces
are
•
to
stress,
or
may
normay
consany
dea
w
grouped
cells
be
manan
ree
adapt,
irreversibly
exposed
exerna
no
may
a
o
or
seady
be
damaged
sae,
couness
nerna
broad
may
injured
and
caed
sresses
by
or
njur y,
die.
omeostass,
poenay
Immunoogc
eases)
reversibly
despe
damagng
undergong
•
reactons
agans
envronmena
oten
by
se
angens
rggerng
angens
(as
n
(as
n
auommune
aerges),
wc
ds-
cause
ce
nlammaon
Agng, a orm o sow, progressve ce njur y
agens.
canges
a
caegores.
REVERSIBLE
CELL
INJURY
Adaptatons are aeraons a enabe ces o cope w sresses w-
Reversible ou
damage,
suc
as
ncreased
musce
mass
n
response
o
changes workoad.
e
major
ceuar
adapaons
and
er
pysoogc
sgncance
are
summarzed
a
e
end
o
e
in
cells
is
that
characterized
are
not
by
functional
and
structural
permanent.
and
e paoogc
injury
ncreased
eares
canges
assocaed
w
ce
njur y
mosy
afec
cyo-
caper.
pasmc srucures bu do no damage nuce (nucear damage s usuay
•
Reversbe njury reers o srucura and uncona abnormaes a
rreversbe)
and
ncude
e
oowng:
can be correced e njurous agen s removed. I e njury s per-
• ssen
or
severe,
can
become
rreversbe
and
ead
o
ce
dea.
Sweng of ce s as a resu o n ux o waer. Ts s usu a y c aus e d
In +
by many
cases,
ces
de
wou
raversng
a
deecabe
reversbe
a ure
o
e
adenos ne
r pospae
( ATP) -d ep enden
Na
pase. +
K
•
Ce
deat
wo
major
s
e
end
resu
o
njur y.
As
we
dscuss
aer,
ere
p asma
membrane
pump
due
o
d e cre as e d
genera on
o
are +
ATP paways
o
ce
dea,
necross
and
apoposs,
and
or
p asma
membrane
d amage.
Te
oss
o
n rac e u ar
K
ey +
occur
Causes
Diverse
of
Cell
erng
responses
•
cause
e
Hypoxa
suppy),
nsus
crca
a
a
varey
o
njurous
injury
or
death
and
result
in
(reduced
are
osmo c
dr a
disease.
wc
njure
ces
uncons,
neced
and
og c
ces
n
by
or
e
producng
by
oxns,
smuang
course
o
r yng
and
ner-
mmune
o
•
eads
oxygen
caused
suppy)
by
and
bockage
scema
o
areres
(reduced
or
oss
o
bood
bood;
•
e
o
Na
ver,
o
n
are
o
o
In
sub e,
br ngs
oxc
waer
e
p asma
re c u um
bu
a
organs
o
are
njur y
accumuaon
n
mcrov
compresson
organs
ear),
rapd
resu ng
oss
endop as m c
(due
cange.
Eosnopa.
(red
b a ance,
bebbng ,
canges
p a e
Fatty
(e.g.,
erad-
necon
wc
an
n ux
w
o
man-
agens.
ncude:
ceuar
damage
comp ens aor y
ncudng
cell
patogens,
w
o
Injury
njurous
Infectous
cae
exposure
insults
ese
•
upon
and
o
cyopasm
and
membrane
swe ng
(E R)
may
(Fg .
app e ar
o
1.1).
m o con -
Te
g rossy
so -
swo en
c ap ar es ) .
acvey
dsrups
nvoved
meaboc
rgycerde-ed
emaoxyn-and-eosn
a er a ons ,
o
njured
[H&E]
ces
n
pd
appears
sans)
meabosm
paways
and
vacuoes.
eosnopc
because
o
oss
o
1
2
CHAPTER
Cell
1
Injury
and
Cell
Death
NORMAL
CELL
Reversible Recovery injury
Swelling
Condensation
of
of
endoplasmic
reticulum
chromatin
and
mitochondria
Membrane
blebs
Myelin
figure Membrane
blebs
Progressive
Breakdown
plasma
injury
of
membrane, Cellular
organelles,
and fragmentation
nucleus;
of
leakage
contents
Inflammation
APOPTOSIS Apoptotic
body
Phagocytosis
of
Phagocyte
apoptotic
and
cells
fragments
NECROSIS
Fig.
1.1
injury
Reversible
that
layers
released
amorphous
RNA,
wc
becomes
•
bnds
more
e
cell
culminate
from
bue
injury,
visible
emaoxyn
w
necrosis,
necrosis
damaged
densities
pronounced
in
or
plasma
by
apoptosis.
e
oward
Myelin
membranes.
electron
san.
progresson
and
apoptosis.
In
microscopy,
eosnopa
necross.
The
figure
figures
cells
of
are
illustrates
undergoing
unknown
or g na
njur y ;
brane
cromatn
n
•
e mtocondra may swe.
•
e
ER
may
become
e
daed,
cyoso.
w
deacmen
o
rbosomes
and
o
poysomes,
ang
proen
Nucear
•
ese aeraons become more severe e njur y progresses o e
rreversbe
brane
W
p ass
a
nebu ous
o
nomena:
ere
o
and
p erssen
A oug
re aes
pase
negry
may
necross,
or
no
r re versb y,
e
nabty
o
no
d e n ve
to
s
o
e
reur n”
oss
o
pasma
and
mem-
njure d
u ndergo
or
ce
by
f unc ton
ce s
de a .
bo cem c a
carac er z e d
mtocondr a
causes,
mitochondria
in
cell
concentric
often
contain
and
AT P
atered
ntraceuar
str uc tura
genera on )
str uc ture
and
membranes;
e ven
a er
f unc ton
and
of
DNA
res ou on
te
pa sma
damage
and
o
e
mem-
oss
of
nteg r ty
re e
cor-
pe-
(oxd a ve
and
apoptosis,
mechanisms,
the
and
two
main
functional
forms
of
cell
death,
differ
in
consequences.
Necross and apoposs are usuay dsnc orms o ce dea, w d-
eren
exp osures ,
mor poog c
conssen y
restore
n
nuceus.
noxous
in
DEATH
Necrosis
cumnang
excessve
“p o n
are
cump.
breakdown
events
syness.
•
cromatn
of
and
CELL dssocaon
sequence
phospholipids
necrosis,
pospor y a on
ceuar
appear
of
significance.
“Myen gures” composed o pospopds derved rom damaged
membranes
the
collections
morpoogc
Necross
may
be
canges
oug
and
o
as
oer
dsngusng
“accdena”
ce
eaures
dea,
(T abe
relecng
1.1).
severe
njury a rreparaby damages so many ceuar componens a e ces
smpy
ory
ss
“a
apar” .
response
s
a
“reguaed”
Wen
cears
ce
ces
e
dea,
de
scene
by
o
because
necross,
e
s
ere
“accden. ”
medaed
s
a
By
by
oca
nlamma-
conras,
dened
apopo-
moecuar
CHAPTER
Table
1.1
Features
of
Necrosis
and
Necrosis
Cell
size
Enlarged
Pyknosis
Plasma
membrane
Disrupted
Cellular
contents
Enzymatic
inflammation
or
(swelling)
→
Reduced
karyorrhexis
digestion;
→
may
karyolysis
role
leak
out
of
cell
Intact;
altered
Intact;
may
pathologic
cell
(culmination
of
Often
injury)
a
are
acvaed
under
specc
crcumsances
and
k
damage.
In
precson,
some
wou
suaons,
ce
nlammaon
dea
may
3
or
sow
nucleosome-sized
be
released
especially
in
fragments
orientation
apoptotic
of
lipids
bodies
may
e
assocaed
eaures
o
be
means
of
pathologic
especially
DNA
eliminating
after
and
some
protein
unwanted
forms
of
cell
damage
ces ces
surgca
into
structure,
physiologic
cells;
injury,
w
Death
No
Invariably
irreversible
paways
Cell
(shrinkage)
Fragmentation
Frequent
pathologic
and
Apoptosis
Nucleus
Physiologic
Injury
Apoptosis
Feature
Adjacent
Cell
1
are
dead
(Fg.
1.3).
s
orm
o
necross
s
caracersc
coaera
bo
o
ypoxa-nduced
o
bood
ce
dea,
caused
mos
commony
by
a
oss
necross suppy
(scema).
e
resuan
necross,
caed
nfarc-
and apoposs, or may sar w apoposs and progress o necross, so e ton,
s
seen
n
mos
sod
organs,
suc
as
e
ear
and
kdneys.
dsncons may no be as absoue as once oug. Nevereess, s use-
•
u
o
consder
e
wo
orms
as
argey
nonoverappng
paways
o
In
quefactve
because
er
prncpa
mecansms
and
uncona
e
dead
ces
are
dgesed
by
reeased
ce enzymes
dea
necross,
(Fg.
1.4).
s
s
seen
n
necross
resung
rom
bac-
consequences era
and
unga
necons
and
n
scemc
narcs
o
e
bran
are usuay dferen. (even
•
sere).
Gangrenous necross s a cnca erm used or e dea o sot s-
Necrosis sue
Necrosis
is
the
result
of
severe
injury
and
is
a
pathologic
process
and
s
oten
apped
o
a
mb
a
as
os
s
bood
suppy
and
in as undergone coaguave necross nvovng mupe ssue ayers.
which
cells
spill
their
contents
into
the
extracellular
milieu,
causI resus rom scema (e.g., rom dabec vascuar dsease, afec-
ing
local
inammation. ng
e
amarks
o
necross
e
ower
remans
•
Dssouton
of
ceuar
mbs)
and
s
caed
dry
gangrene
e
dead
ssue
are:
membranes,
ncudng
e
pasma
nac
or
wet
gangrene
e
ssue
quees,
as
s
common
membrane oowng supermposed bacera necon.
and
ysosoma
membranes,
because
o
damage
o
membrane
pds
•
and
acvy
o
Caseous
necross
necons
•
suc
caracersc
as
o
sopasmoss.
ubercuoss
e
dead
and
ssue
some
unga
breaks
down,
Leakage of ysosoma enzymes a dges e ce creang
•
s
pospopases
L oca
nlammaton
n
response
o
e
reeased
conens
o
a
ceesy
S ome
specc
componens
o
ese
conens
ave
been
moecuar
paerns
(DAMPs).
ese
ncude
ATP
(rom
damaged
mocondra),
examnaon
(Fg.
e
necroc
ocus
s
a
coecon
o
1.5).
ragmened
ysed
ces
w
an
amorpous
granuar
pnk
(eosnopc)
reeased appearance.
acors
gross
caed or
damage-assocaed
on
dead Mcroscopcay,
ces.
conssency
urc
acd
Ceuar
ounes
canno
be
dscerned,
and
ere
s
(a oten a perpera coecon o macropages ormng a granuoma.
breakdown
produc
o
DNA),
and
numerous
oer
moecues
a
•
are
normay
conaned
wn
eay
ces
and
wose
Fat
necross
resung
ndcaes
severe
ce
njur y.
ese
moecues
are
recognzed
rom
expressed
by
macropages
and
mos
oer
ce
rgger
pagoc yoss
o
e
debrs,
as
we
as
e
o
c yoknes
acue
a
nduce
nlammaon
(see
Caper
2).
produce
more
proeoyc
enzymes
a
o
w
exacerbae
and
e
subsequen
reacon,
un
e
e
o
a
desrucon,
pancreac
ypcay
pases
pancreas
and
e
peronea
cavy.
no
s
e
occurs
(Caper
cacum
o
13).
produce
Fay
acds
grossy
are
vsbe
reeased
caky
and
we
(a
saponcaon),
necroc
ssue
o
deny
wc
e
enabe
esons
e
surgeon
(Suppemena
eFg.
and
e
1.1).
On
as examnaon,
e
oc
o
necross
conan
sadowy
ceared.
man
causes
o
necross
ncude
scema,
exposure
o
oxns,
burns
and
oer
orms
o
cemca
and
pysca
ounes
o
necroc
deposs
and
an
a
ces
surrounded
nlammaor y
by
basopc
cacum
reacon
mcro-
• ba
areas
acvaed
e
soogc
been
e
pancreas
paoogs
damage
o
Inlammaareas
ces
oca
producon combne
or y
o
reease
ypes, n
and
e
by subsance
recepors
reers
reease
njury,
Fbrnod
necross
s
a
caracersc
mcroscopc
ndng
seen
and
mos
commony
n
mmune
reacons
n
wc
compexes
o
unusua suaons n wc enzymes eak ou o ces and njure adjacen
angens
and
anbodes
and
exravasaed
pasma
proens
are
ssues (as n pancreas). A ese nang rggers ead o rreparabe
deposed damage
o
numerous
ceuar
componens,
wc
cumnae
n
pnk, brane
damage,
e
Morphology.
bass
or
Necroc
e
ces
subsequen
sow
more
seps
n
dfuse
noss)
o
sequena
canges,
ragmenaon
dssouon
o
rom
cyopasmc
condensaon
nuce
o
(karyorrexs)
croman
o
er
rom
e
eosno-
(pyk-
compee
was
o
bood
appearance
vesses,
were
remnscen
o
ey
brn
ave
a
(Fg.
brg
1.6).
aboraory
ncrease
necroc
n
serum
ces
dagnoss
eves
because
o
o
o
necross
nraceuar
membrane
may
be
proens,
damage.
s
made
by
wc
s
e
deecng
eak
bass
ou
o
o
an
e
measur-
ng serum roponn or dagnoss o myocarda narcon, ransamnases
or ver dsease, and pancreac enzymes suc as amyase or pancreas.
(karyoyss).
Necross
e
amorpous
necross.
pa compared w a seen n reversbe njur y (Fg. 1.2). Nuce
undergo
n
mem-
dferen
causes
s
manesed
by
dferen
mor-
Apoptosis pooges, and recognon o ese paerns s epu or deermn-
ng
•
e
In
underyng
coaguatve
preser ved,
a
Apoptosis
eoog y :
necross,
eas
or
e
some
underyng
me,
even
ssue
oug
arcecure
e
s
consuen
no
a
longer
is
a
form
needed
potentially
of
or
cellular
are
harmful
suicide
damaged
that
beyond
inammatory
eliminates
repair,
response.
cells
without
that
are
eliciting
CHAPTER
Supplemental
deposits
eFig.
represent
1.1
foci
of
Fat
fat
necrosis.
necrosis
The
with
areas
of
calcium
white
soap
chalky
formation
(saponification) at sites of lipid breakdown in the mesentery. (Courtesy of
Dr.
James
cine
at
Crawford,
Department
Hofstra/Northwell.)
of
Pathology,
Zucker
School
of
Medi-
1
Cell
Injury
and
Cell
Death
3.e1
4
CHAPTER
Cell
1
Injury
and
A
Cell
Death
B
Fig.
1.2
with
of
Morphologic
viable
epithelial
cytoplasm,
of
nuclei
and
katachalam,
and
changes
cells.
(B)
swelling
of
fragmentation
University
of
in
reversible
Early
occasional
of
cells
Texas
and
(reversible)
and
Health
irreversible
ischemic
cells.
(C)
leakage
of
Sciences
cell
injury
Necrotic
contents.
Center,
San
injury
(necrosis).
showing
surface
(irreversible)
(Courtesy
injury
of
Drs.
(A)
Normal
blebs,
of
epithelial
Neal
kidney
increased
cells,
Pinckard
tubules
eosinophilia
and
with
M.A.
loss
Ven-
Antonio.)
I
N
A
B
Fig.
of
1.3
the
outlines
is
In
s
dsmane
paway
e
o
ce
nuceus
Causes
Apoptosis
nae
poenay
uness
(Tabe
damaged,
ens;
rapdy
occurs
n
us,
e
many
I
especay
rreparaby
•
•
o
o
ces
o
o endng
•
by
A
and
wedge-shaped
(N)
an
and
necrotic
inflammatory
kidney
cells
infiltrate
in
infarct
the
(dark
(yellow).
infarct
nuclei
(I).
(B)
The
Microscopic
necrotic
interspersed
cells
between
view
of
show
the
edge
preserved
necrotic
tubules)
and
e
and
suaons
ces
as
a
a
by
specc
ragmens
afecs
ce
s
sgnas
a
are
are
even
e
o
repaced
( neu rop s
mmune
ser ves
ouved
ce’s
o
em-
er
wen
DNA
use-
ces
or
are
pro-
emnaed.
deveopmen
a
and
ave
paoogc
damage
ssues
acvaed
generang
pagocyes.
damaged
eu ko c yes
n ammaor y
e
durng
prmorda
D e a
(A)
kidney
nuclei,
enzymes
occurs
wen
Pysoogc apoptoss
ces
of
pysoogc
ces
aso
•
D ea
necrosis.
normal
cyopasm,
ceared
armu
1.2).
loss
dea,
and
and
of
with
with
present.
recognzed
Apoposs
Coagulative
infarct,
and
organsms,
by
maure
suc
y mpo c yes )
resp ons es
ave
as
ssues
a er
em nae d
agens
E mnaon
o
dysuncona
or
auoreacve
ympocyes
or
ympocye precursors, parcuary n e bone marrow and e
ymus
Fig.
tion
1.4
of
Liquefactive
the
tissue.
necrosis.
An
infarct
in
the
brain
showing
dissolu-
CHAPTER
Table
Cell
1
1.2
Injury
Physiologic
Associated
With
and
and
Cell
Death
Pathologic
5
Conditions
Apoptosis
Condition
Mechanism
of
apoptosis
Physiologic
During
embryogenesis
Loss
of
growth
(presumed
Turnover
sues
of
proliferative
(e.g.,
bone
marrow
Involution
of
tis-
lymphocytes
and
Absence
in
survival
of
signaling
signals
death-inducing
or
acti-
signals
thymus)
hormone-
dependent
of
vation
factor
mechanism)
tissues
Decreased
(e.g.,
hormone
reduced
survival
levels
lead
to
signals
endometrium)
Decline
of
leukocyte
numbers
immune
at
the
and
Loss
end
of
for
inflammatory
of
survival
leukocyte
signals
as
activation
stimulus
is
elim-
inated
responses
Elimination
harmful
Fig.
1.5
Caseous
caseous
necrosis
necrosis.
Tuberculosis
containing
of
yellow-white
the
lung,
(cheesy)
with
a
large
area
of
of
potentially
Strong
self-reactive
recognition
induces
lymphocytes
mitochondrial
debris.
of
apoptosis
and
self
by
antigens
both
death
the
receptor
pathways
Pathologic
DNA
damage
Accumulation
of
misfolded
Activation
of
proapoptotic
proteins
Activation
of
proapoptotic
proteins,
proteins
possibly
direct
activation
of
caspases
Infections,
viral
especially
certain
Activation
infections
of
pathway
Killing
T
of
the
by
mitochondrial
viral
infected
proteins
cells
lymphocytes,
by
which
cytotoxic
activate
caspases
proens
dea
•
s
e
ater
e
sensors
1.6
Fibrinoid
necrosis
in
an
artery
in
a
patient
with
n
The
wall
of
the
artery
shows
a
circumferential
bright
pink
necrosis
with
protein
deposition
and
e
(ntrnsc)
end
by
patway
pysoogc
cyopasm
e
bodes
and
deec
resu
seems
o
paoogc
e
o
apopoc
ce
pagocyes.
ack
o
be
responsbe
suaons.
sur vva
or
Moecuar
or
e
accumuaon
o
msoded
proens.
sgnas,
ese
DNA
acvaed
area
sensors of
mos
resdues.
apopoc
polyarteritis
damage, nodosa.
n
acd
o
mtocondra
apoposs
Fig.
asparc
cearance
nduce
e
dmerzaon
o
wo
proens
(caed
BAX
and
inflammation.
BAK)
a
nser
no
e
mocondra
membrane
and
orm
can-
nes, eadng o ncreased mocondra permeaby. e cannes
aow proapopoc acors (.e., cyocrome c and oer proens) o
•
Ce oss a aernaes w ce proeraon n ormone-responeak
no
e
cyoso,
were
ey
acvae
e
enzyme
caspase-9.
A
sve ssues suc as e endomerum cascade
•
•
Patoogc apoptoss o
•
addona
caspases
s
acvaed,
cumnang
n
e
enzy-
Emnaon o ympocyes a recognze se angens mac
o
breakdown
nuce
and
o
oer
nuce
and
organees
cyopasmc
suc
as
srucures.
mocondra
Fragmens
are
exruded
S evere DNA damage, ater exposure o radaon or cyooxc drugs no
•
Accumuaon o msoded proens, gvng rse o ER sress
•
C eran
ragmens
pagocyosed.
necous
agens,
parcuary
some
vruses
suc
B
and
C,
wc
rgger
mmune
responses
a
Because
apopoc
ceuar
bodes)
membranes
a
are
reman
subsequeny
nac,
enzymes
as and
epas
(caed
oer
ce
conens
do
no
eak
ou
(as
ey
do
n
necross),
and
desroy ere s no nlammaon. e dmerzaon o e efecor moecues
neced
ces. BAX
o
Mechanisms
of
sic)
are
two
pathway
differ
in
e
dea-
pathways
and
their
the
and
of
apoptosis,
death
initiation
bocemca
enzymes
receptor
and
caspases.
the
(or
molecular
paways
sur vva-nducng
caed
BAK
BCL
s
normay
amy,
noaby
prevened
BCL-2
by
and
anapopoc
BCL-x.
ese
moecues
are
acvaed
Apoptosis by
There
and
e
o
extrinsic)
signals
apoposs
sgnas
Caspases
mitochondrial
and
are
pathway,
(Fig.
conro
umaey
cysene
(or
intrin-
ce
which
o
1.7).
e
e
baance
a
o
o
ceave
•
acors,
sur vva
BCL-2
sands
acvaon
proeases
grow
or
by
B
and
dscovered
e
deat
one
as
an
way
aberraons
oncogene
(extrnsc)
membrane
a
grow
proeraon.
ympoma-2,
receptor
pasma
s
subsequen
genec
ce
was
are
wc
so
s
seen
(see
o
Consuve
umors;
or
Caper
patway
recepors
n
named
e
of
acors
e
n
promoe
acvaon
ac,
umor
n
BCL-2
wc
5).
apoptoss.
umor
Dea
necross
recepors
acor
(TNF)
6
CHAPTER
Cell
1
MITOCHONDRIAL
Injury
and
Cell
Death
(INTRINSIC)
DEATH
RECEPTOR
P ATHWA Y
(EXTRINSIC)
P ATHWA Y
Receptor-ligand
Cell
•
injury
•
FAS
•
TNF
interactions
receptor
Mitochondria
Growth
factor Adaptor
proteins
withdrawal
•
DNA
damage
Phagocyte (by
radiation,
Cytochrome BCL-2
toxins,
and effectors
(BAX,
activation
proapoptotic
Protein
proteins
misfolding
(ER
Caspase
other
BAK)
radicals)
•
c
family
free
Regulators
BH3
stress)
(BCL-2,
BCL-x
) L
sensors
Endonuclease
Breakdown
activation
of
cytoskeleton
Nuclear
fragmentation
Ligands
for
phagocytic
cell
Apoptotic
Fig.
and
1.7
Mechanisms
both
related
culminate
to
members
BH3-only
proteins
ciency
BCL-2
and
of
various
induce
from
the
complex,”
recepor
ser ved
amy
ound
cyopasmc
activation
the
activate
and
as
of
two
pathways
caspases.
sense
molecules
that
receptors
in
cell
lead
caspases,
to
and
that
c,
the
lack
a
e
ype
I
membrane
Wen
cues
ese
are
dea
urn,
TNF
enter
and
on
many
ces.
doman”
T
recognze
doman.
kng
o
n
and
expressed
acvaes
nvoved
recepor
proen
cross-nked
ese
by
ese
a
en
e
recepors
medaes
by
and
o
on
ave
a
neracon
FAS
and
of
survival
the
is
ey
by
of
begn
recepors
ragmens
undergo
cyoss
e
o
express
on
apopoc
a
pyknoc,
rom
o
appearng
ces,
ces
race,
T
s
and
e
o
In
Wen
o
oten
FAS
recepor
the
protein
In
caspases.
into
concert
which
with
a
reticulum;
defi-
leaky
caspases
pathway,
“death-inducing
Endoplasmic
are
These
become
Activated
receptor
a
regulation,
damage.
mitochondria
death
proteins
and
proteins,
signals
signaling
TNF,
tumor
ces are removed so qucky and eiceny a ey are oten no den-
w
ed
va
e
wc,
and
a
n
n
dyng
so
wn
eicen
o
a
s
o
n
s
e
Other
dea,
er
bu
•
express
Pathways
severa
dead
ces
vruay
ces
s
1.8).
ces
nuce
and
•
e
and
ces
are
apopoc
e
n
ssues
n
wc
many
ces
are
consdered
e
s
a
oca
are
by
o
ead
o
o
ave
orm
ce
by
ce
o
and
o
s
n
response
produced
rrans.
njur y,
moecues,
ce
eaures.
knases
wc
o
receny.
nvesgaon,
unque
oer
membrane
paways
descrbed
opc
specc
as
ke
n
as
Sgnas
necross,
apoposs,
so
bo.
nduced
cyoknes,
and
a
and
(TNF),
specc
dea
reeases
nlammaon
o
mcrobes
pasma
been
remans
acor
eaures
o
bes-dened
aso
names
acvaon
reguaed
o
er
necross
response
s
e
ave
dseases
aware
umor
dyng
Death
apoposs
uman
be
knases
process
P yroptoss
Cell
nduced
os
ese
nduce
•
appear
o
e
s
s
cyokne
wc
dsappear
absen.
However,
bu
pago-
dsncve
e
croman,
e
e
even
mecansms
n
soud
Necroptoss
e
of
and
oer
mporance
rom
e
necross
sudens
o
apoposs,
desroy
specmens,
apoposs.
Aoug
recognzed
beore
conens.
secons,
(Fg.
are
and
mnues,
apopoc
vacuoes
undergo
a
nges
er
nlammaon
H&E-saned
n
ces
soogc
by
s
moe-
paway
ympocyes
moecues
reease
condensaon
e
or
permeability.
the
ER,
induction
BH3-only
DNA
activate
In
body
their
con-
(FASL)
proens
ympocyes
Pagocyes
and
appearance
necross.
because
srunken,
number
damage
apopoc
eavng
morpoogc
dferen
fragments.
a
pagocyes.
membrane
o
wou
apoptotc
o
and
same.
par
Cearance
or
permeability,
adaptor
the
FASL
•
mitochondrial
cytosol
of
in
pathway,
signals
fragmentation.
result
ympocyes.
caspase-8,
dea
se-reacve
cyooxc
T
arges,
adapor
acvae
e
gand
acvaed
bnd
caspases.
some
(CD95).
FAS-expressng
recru
emnaon
ces
FAS
many
FASL
downsream
arge
mitochondrial
assembly
end
differ
factor.
“dea
ces
apoptosis
increase
oer proens nvoved n ce dea. e prooypc dea recepors
are
the
of
mitochondrial
death
the
In
a
maintain
cytochrome
culminate
activates
The
family,
proteins
such
that
membrane
BCL-2
effector
other
substances,
which
apoptosis.
the
of
changes
plasma
necrosis
in
of
receptors
ever
by
suc
(ence
bacera
as
oxns
nereukn-1,
pyro
n
e
n
a
name).
Autopagy s a orm o “se-eang” (Greek, paga = o ea) n wc
ces
sar ved
maera
o
o
nurens
provde
and
porons
use
w
o
dges
energy
e
ysosomes,
or
cyoso
and
e
er
own
sur vva.
are
organees
In
encosed
conens
are
s
and
process,
wn
recyce
vacuoes,
desroyed
by
e
organees
wc
ysosoma
CHAPTER
aer)
Cell
1
and
Injury
decreased
moecues,
suc
as
ATP
and
Cell
producon.
cyocrome
c,
Death
7
Mocondra
wose
reease
no
aso
e
sequeser
cyoso
s
an
ndcaor o damage and, as descrbed earer, a rgger or apoposs.
•
C euar
and
and
organees
suc
as
lud
branes,
dges
by
resu
by
(some
indicated
shown.
(The
apoptosis
cells
in
in
this
chromatin
by
arrows)
preparative
epithelial
normal
and
the
in
a
crypt
regimen
cells,
tissue.)
which
Note
shrunken
for
the
cell
in
the
cells.
colonic
colonoscopy
explains
the
fragmented
bodies,
some
Apoptotic
abundance
nuclei
with
with
pieces
dead
condensed
falling
off
ron
n
(Courtesy
of
Dr.
Sanjay
Kakar,
Department
of
Pathology,
ecues
rom
of
California
San
as
e
ces
o
ROS
to
of
type
of
OF
injury
the
o
necross.
ceuar
genec
mem-
enzymes
Damage
consuens,
maera.
ceuar
proeraon.
ncude
e
ER
processng)
to
a
are
o
be
a
o
e
Nucear
uncons
Irreparabe
(one
and
e
end
damage
(.e.,
damage
proen
o
DNA
e
se
o
proen
cyoskeeon
syness
(e
sruc-
ces).
damaged
rom
durng
cellular
group
gy
orb.
proens,
ree
e
ousde,
nlammaor y
abnormalities
of
molecules
reacve
ey
reac
pds,
or
exampe,
reacons.
that
called
and
moecues
w
a
nucec
converng
radcas
produced
connues
because
e
nuren
decency
are
free
induced
by
radicals.
em
w
an
norganc
acds)
no
and
ree
unpared
and
eec-
organc
remove
radcas.
mo-
eecrons
Boogcay
ncude
ROS
normay
n
and
sma
nrc
oxde
amounts
n
(Fg.
a
1.10).
ces
respraon
CELL
INJURY
AND
from
any
offending
injurious
agent,
its
and
reactons
energ y
a
generaon.
occur
durng
In
s
durng
te
mocon-
process,
moecuar
a
addon
sma
are
o
our
amouns
eecrons.
o
generaed
gy
wen
s
reacon
reacve
oxygen
bu
s
s
mperec,
sor-ved
ony
paray
owever,
oxc
nerme-
reduced.
ese
DEATH
stimulus
severity,
(redox)
oxygen s reduced n mocondra o generae waer by e sequen-
s
nermedaes
degree
ce
may
moecues,
are
daes
the
ce’s
eukocyes
refers
belong
ouer
(e.g.,
and
on
ysosoma
of
no correced, can rgger apoposs by e mocondra paway.
The
o
o
o
reease
ces
Francisco.)
process
MECHANISMS
oss
o
o
uncons
Stress
stress
oer
dra
I
e
“moor”
reducton–oxdaton
enzymes.
amark
n
ranspor
Damage
eads
proen
Univer-
• sity
o
agens
and
radcas
an
mporan
them.
we
producs
which
Free
are
induces
of
resus
crca
conan
srucure
cells
epithelium
frequently
as
srucures,
e
ROS, apoptotic
mos
scafod
Oxidative
of
e
and
e
apoposs.
Oxidative
appearance
ce,
agens,
pds
In addon o ce njur y resung rom mparmen o ese nrn-
sc
Morphologic
omeosass.
oer
pos-ransaon
ura
1.8
numerous
ranscrpon-dependen
njurous
and
Fig.
o
manan
Oter ceuar components a sufer damage upon exposure o var-
ous
•
ey
necross.
syness),
rggers
composed
ser ve
on
or
njured
sore
dsrups
•
and
membrane
o
Nuce
are
moecues.
and
ROS
e
pasma
•
membranes
carboydrae
varies
and
its
gen peroxde (H
depending
duration,
ncude
2
superoxde
as
O
2
superoxde
O
,
2
wc
s
convered
o
ydro-
) sponaneousy and by e acon o e enzyme
dsmuase.
H
2
O
s
2
more
sabe
an
O
and
2
can
cross
2+
well
as
the
Sma
adaptive
amouns
ability
o
a
and
oxn
genetic
or
bre
makeup
perods
o
of
the
target
scema
boogc
cell.
may
s
cause
3
cause
ours,
ater
may
n
20
One
wereas
o
aso
genes
rae
o
o
necross.
30
Sraed
cardac
mnues
deermne
encodng
meabosm
e
goas
ndvduas
w
o
o
musce
musce,
reacon
members
o
many
precson
reac
o
o
e
w
scema.
e
n
e
o
e
s
survves
ger
genec
medcne
ypes
s
o
o
meaboc
agens.
cyocrome
and
scema
makeup
njurous
cemcas
dferen
eg
P450
ence
use
e
o
2
needs,
e
o
des
afec
efecs
o
o
e
injury
results
from
abnormalities
in
•
or
ROS
are
durng
ow
owng
more
components,
mainly
mitochondria,
membranes,
and
urn
(Fig.
reacve
o
ree
o
meas,
ydroxy
radcas
s
suc
radca
ncreased
as
Fe
by
by
,
e
H
2
O
2
Fenon
exposure
o
mpar
ROS
mocondra
producon
uncons.
because
o
Oxygen
ncompee
deprvaon
reducon
o
produced
o
n
pagocytc
desroy
nlammaon.
ngeson
e
o
a
In
e
o
O
2
,
a
many
mcrobes
“respraor y”
mcrobe,
generaon
eukocytes,
ngesed
and
or
s
burs,
membrane
convered
o
H
2
and
subsances
“oxdave”
pagosome
wc
neutrops
oer
O
2
o-
enzyme
convered
o
a
gy
reacve
compound,
.
H
2
O
ypocore
2
s
(e
the major
nucleus
presence
essential n
cellular
o
macropages,
smu.
one
gy
generaon
may
eads
caayzes
Cell
e
e
e
oxygen.
oxns.
predc
wc
aso
ndvdua
amy
o
In
UV g, radaon and oxns, and durng norma ceuar agng, a
o
Poymorpsms
genecs
njurous
or
convered
reacon.
reversbe njury bu arger doses o e oxn or more proonged scema
may
membranes.
componen
o
ouseod
beac),
by
e
enzyme
myeoper-
1.9). oxdase,
wc
s
presen
n
eukocye
granues.
s
s
one
reason
e consequences o mparmen o eac o ese ceuar organees wy
are
dsnc
bu
nlammaon
o
k
necous
paogens
s
oten
overappng. assocaed
•
nended
w
njur y
o
norma
ssues.
Mtocondra are e ses were ATP , e prmary carrer o energy n •
Ntrc
oxde
s
anoer
reacve
ree
radca
produced
n
macro-
ces, s produced by oxdave posporyaon. Injury due o ypoxa, pages
scema,
radaon,
or
oer
nsus
mpars
oxdave
and
eadng
o
e
ormaon
o
reacve
oxygen
eukocyes
durng
nlammaor y
reacons.
I
can
posporyacombne
on,
oer
speces
(ROS)
w
O
2
o
orm
a
gy
reacve
(see re,
wc
aso
parcpaes
n
ce
njur y.
compound,
peroxyn-
8
CHAPTER
Cell
1
Injury
and
Cell
Death
Hypoxia/ischemia
Radiation
Radiation
Other
injurious
ROS
agents
Other
MITOCHONDRIA
ATP
injurious
CELLULAR
Damage
ROS
to
Mutations
agents
MEMBRANES
lysosomal
Damage
membranes
Damage
Energy-
NUCLEUS
to
plasma
membrane
to DNA
lipids,
dependent
proteins,
nucleic
functions
Leakage
acids
of
Impaired
enzymes
Leakage
transport
of
damage
functions
cellular
contents
Reduced
Activation
protein Cell
of
caspases
injury synthesis
NECROSIS
Fig.
1.9
branes,
NECROSIS
Principal
or
triphosphate;
ROS
can
damage
cross-nkng),
dues),
s
and
us
conroed
ase,
ree
wc
and
by
afec
a
down
durng
(by
(by
enzymes
break
radcas
pds
DNA
cellular
nuclear
DNA.
ROS,
reactive
ceuar
as
ydrogen
paoogc
breaks
stimuli.
structures
(many
er
injurious
progress
Increased
by
res-
accumuaon
peroxdase
over wems
Most
may
and
caa-
generaon
ese
Hypoxa
bood
Oxygen
eres
w
reduced
of
leads
energy-dependent
reduced
cellular
generation
systems
(Fig.
of
ATP
e
apoptosis.
cellular
ATP,
coronar y
or
cerebra
n
bood
and
failure
1.11).
low,
arer y
arer y
probems
s
may
and
s
on
mem-
Adenosine
n
o
esmaed
e
major
ese
ces
are
o
a
o
n
arera
o
o
some
n
oxygen
s
pds,
o
seen
suaons
(wc
emogobn).
cause
cause
mocondra
and
o
s
posonng
Iscema,
obsrucon
myocarda
sroke)
o
e
or
a
mos
o
ner-
or
(as
narcon,
severe
drop
requen
and
medcne.
pospae
proens
a
capacy
major
reducon
g-energ y
syness
oxygen)
monoxde
consequence
e
cnca
e
a
e
(sock).
produced
depends
be
dsease,
n
o
carbon
dsease,
pressure
a
avaaby
and
oxygen-carr yng
bood
n
ATP
to
anema,
o
Ischemia
deciency
mitochondria,
or
(reduced
oss,
serous
and
affect
necrosis
scavengng
mecansms.
Hypoxia
stimuli
to
species.
deoxyymdne
componens.
peroxde.
injurious
these
proens
a
guaone
njur y
of
to
oxygen
peroxdaon),
creang
suc
targets
Injury
APOPTOSIS
an
requred
and
eay
eecrocemca
(oxdave
or
urnover
ndvdua
membrane
o
reacon
pospor yaon)
ranspor,
pospopds.
burn
50
o
75
kg
I
o
s
ATP
Ischemia
ever y
ATP
day.
ereore,
damages
many
oxygen
ceuar
deprvaon
and
componens,
as
e
resung
depeon
+
•
Reduced
acvy
o
e
pasma
o
oows:
membrane
ATP-dependen
Na
+
-K
+
pump
resus
eadng
e
o
n
ce
eares
e
nlux
sweng
o
and
manesaons
Na
and
daon
o
ce
o
njur y
waer,
e
as
ER,
(see
dscussed
wc
Fg.
are
earer,
some
o
1.1).
Mitochondrion
•
Anaerobc
absence
Oxidative
decreased
phosphorylation
many
gycoyss
o
oxygen,
ncreases
resung
nraceuar
nraceuar
pH,
n
n
an
aemp
ncreased
and,
o
generae
producon
consequeny,
ATP
o
n
acc
reduced
e
acd,
acvy
o
enzymes.
•
Rbosomes deac rom e ER, eadng o reduced proen syness.
•
Hypoxa
ATP
may
damagng
+
Na
pump
Anaerobic
glycolysis
Detachment
of
•
ribosomes
of
e
generaon
o
ROS,
wc
ave
many
Umaey, ysosoma and mocondra membranes are damaged,
ysosoma
begns
2+
Influx
ncrease
efecs.
o
acd
dges
ydroases
se,
are
acvaed
cumnang
n
by
ow
pH,
and
e
ce
necross.
Ca
+
H
O,
2
and
Na
Glycogen
Lactic
pH
Protein
acid
synthesis
Ischemia–Reperfusion
Injury
+
Efflux
of
K
Restoration
ER
swelling
Cellular
Loss
doxically
of
of
blood
exacerbates
ow
to
tissue
an
ischemic
tissue
sometimes
para
injury.
e ce njur y a may oow reperuson s key due o ncreased
swelling
microvilli
producon
o
ROS
by
njured
ces
w
damaged
mocondra
and
Blebs
by
Fig.
1.10
The
functional
and
morphologic
consequences
of
hypoxia
eukocyes,
ATP,
Adenosine
triphosphate.
ER,
endoplasmic
are
recrued
o
ge
rd
o
e
necroc
ces.
and
ese ischemia.
wc
nlammaor y
ces
may
reease
enzymes
a
cause
ye
more
s-
ener
e
reticulum.
sue
damage
(see
Caper
2).
Compemen
proens,
wc
CHAPTER
Cell
1
Injury
Pathologic
and
Cell
Death
9
effects
Radiation
Toxins
Production
of
ROS:
Lipid
peroxidation
Membrane
damage
Reperfusion
O
H
O
2
2
Superoxide
OH
2
Hydrogen
Hydroxyl
peroxide
radical
Protein
DNA
Conversion
to
H
by
O
2
Decomposition
H
2
1.11
ROS
is
The
radicals
in
maor y
ssue,
may
aso
free
by
to
removal,
and
injurious
may
role
of
stimuli.
Excessive
damage
lipids
reactive
These
production
(by
oxygen
free
or
by
directly
cytochrome
A
cassc,
njury
s
ver
conrbue
moecue
s
njury,
e
ER
and
in
o
used
e
njur y,
convered
many
e
n
by
membrane
toxins
conversion
as
n
oer
nlam-
sae;
dry
exampe
naaon
ceanng
ver
no
membrane
causes
reactive
cellular
com-
metabolites,
often
a
o
o
carbon
ndusry
a
ree
n
bu
radca
pospopd
decne
oxn-medaed
e
eracorde,
now
a
banned.
s
e
cause
peroxdaon.
syness
o
o
ansm
o
acon.
enzymes,
serous
and
ver
I
e
s
acue
anagesc
meabozed
overdose
damage
n
e
o
aceamnopen
o
a
s
Uned
ree
drug
Saes
radca
s
e
and
as
by
smar
and
mec-
cyocrome
mos
oer
a
requen
deveoped
Reticulum
(ER)
as
Tabe
accumulation
of
misfolded
mechanisms
and
trigger
n
Wen
mpropery
proecve
oded
proen
ransaon
s
a
manan
mechanisms
s
ncreased
(Fg.
(see
of
injury.
free
SOD,
proen-secreng
mupe
and
myeoma.
ceuar
Caper
ypoxa,
Dseases
Damage
P450
cause
o
counres.
o
erapeuc
Damaged
ce
age,
abnormay
17).
by
n
Deprvaon
aso
caused
ces,
may
parcuary
Proen
o
ncrease
msoded
msodng
severa
neu-
gucose
e
and
burden
proens
are
o
sed
o
poena
o
e
n
p53
apoposs
I
a
be
p53,
ese
upon
and
corrected
o
exposure
ROS
wc
and
arress
be
an
e
nerere
a
w
s
w
n
and
o
by
DNA
e
aby
o
o
G1
aso
correc
repair
pase
e
a
ce.
arres
cancers
o
ce
e
DNA
DNA
us,
DNA
e
cemo-
muaons.
acvaes
paway.
o
numerous
radaon,
resu
abnorma
ransormaon
w
o
a
ces
mocondra
survve
assocaed
as
repared
mecansms
by
magnan
are
to
occurs
damage
raer
nduce
great
drugs,
apoposs
de
o
muaons
DNA
acvaes
aow
rggers
“cooses”
too
apoptosis.
nucear
mecansms.
p53
is
to
(ancancer)
DNA
cyce
repar
that
leads
in
the
ER
can
stress
dam-
e
ce
as
e
Predcaby,
cycng
or
(see Caper
o
5).
Aging
adapage
because
of
accumulation
of
mutations,
progressively
apoptosis.
caed
accumuae
e
unfoded
n
e
ER,
proten
ey
reduced
and
e
producon
newy
syneszed
proens
n
1.12).
I
e
oad
o
msoded
and
defective
protein
homeostasis.
rs
response,
o
replication,
age
because
er
ces
age.
Aoug
muc
o
e
pubc’s
n on
agng
s
ocused
on
s
cosmec
and
pysca
conse-
caperones
er
e
greaes
danger
o
ceuar
agng
s
a
promoes
e
proper deveopmen
sape)
o
as
undamena
scema
Damage
quences, (moecues
suc
dseases
damage
aenon wc
cell
by
Stress
proteins
proens
reacon
e
DNA
Peope a
in
of
and
accumulation
neopasms
proens.
decreased
acvae
be
DNA
Cells tive
production
decay
1.3
Cellular The
to
resulting
neopasms
o
msoded
nduce
Endoplasmic
ceran
ce
oug
Damage
enzymes
deec resus n e accumuaon o pds n epaocyes and oer ces
aer).
The
a
s
orm compexes w rgycerdes, acang rgycerde secreon; s
see
leads
DNA,
injury.
spontaneous
ce
pasma proens, as we as apoproens, wc are ranspor proens a
(seaoss;
and
oxygen,
n
sorca,
e
to
damage
cells.
oowng
n
and
cell
by
removal
rodegenerave
microbial
liver
many
in
dismutase.
Injury
after
damage
once
o
or
P450
now
cemca
ce
Cell
(ROS)
removed
proteins,
pasma
environmental
ponents
are
inadequate
s
Many
species
radicals
peroxidation),
reacons.
Toxin-Mediated
Mutations
catalase
systems.
which
damage
radicals
many
enzymatic
misfolding
glutathione
generation,
cells,
superoxide
reperused
of
increased
specialized
by
peroxidase,
SOD
Removal
Fig.
O
2
Breakdown,
modifications
proens
s
o
many
degenerave,
meaboc,
and
neopasc
dsor-
oo ders. Numerous nrnsc moecuar abnormaes are beeved o cause
grea,
e
ce
des
by
e
mocondra
paway
o
apoposs;
n
s e
way,
ces
a
can
no
onger
uncon
are
• Inraceuar
accumuaon
o
agng
msoded
proens
may
be
abnormaes
reduce
e
a
aby
ncrease
o
e
emnae
producon
em.
o
ese
msoded
may
resu
be
suc
as
ose
responsbe
or
c ysc
bross,
producon
w
o
a
proens
a
decreased
canno
capacy
o
od
propery :
correc
a
agng,
msodng;
D ecreased
ead
vra
necons,
wen
arge
amouns
o
syneszed
wn
ces,
exceedng
e
mcroba
ce’s
wc
ncreased
nsun-ressan
demand
saes;
or
secreor y
canges
n
e
proens
wc
occurs
nauray
and
muagens.
repcaton
eomerase,
of
ces
wc
because
manans
o
progressve
e
norma
oss
o
e
eng
o
eomeres.
ese
sor
DNA
sequences
a
e
e
ends
o
cro-
proec
w
e
ever y
ends
rom
repcaon
uson
bu
can
and
be
degradaon.
mananed
by
Teomeres
e
acvy
proens e
enzyme
eomerase.
Because
mos
ces
(excep
germ
ces)
proen-odng
suc
as
nraceuar
pH
e
or
no
eomerase,
eomere
sorenng
s
nevabe
nsun n
n
DNA,
envronmena
s
conan capacy ;
n
and
necons,
o are
ROS
o
soren especay
by
gene
mosomes assocaed
1.13).
mutatons
proens
rom
enzyme e
o
enanced
enzyme muaons,
(Fg.
caused
• or
ces
Accumuaon
may by
o
emnaed.
and
redox
dvdng
ces.
W
compee
oss
o
eomeres
durng
ceuar
10
CHAPTER
Cell
1
Injury
Mild
Misfolded
ER
lumen
ER
membrane
ER
and
Cell
Death
Stress
Severe
ER
Stress
proteins
P
P
P
P
P P P
P
Sensor
of
P
P
misfolded
Signaling
proteins
Signaling
Cytosol Increased
Reduced
Increased
protein
protein
Activation synthesis
of
BH3 chaperones
synthesis
Reduced
load
of
Fig.
1.12
proteins
trigger
the
an
1.3
Diseases
ER
adaptive
pathway
unfolded
unfolded
the
misfolded
drial
Table
The
in
is
misfolded
Caused
by
Mutant
by
Proteins
hypercholesterolemia
Tay-Sachs
and
sensors
in
amount
and
of
endoplasmic
ER
which
reticulum
membrane
can
misfolded
the
disease
protect
proteins
irreparably
Retinitis
by
stress.
the
is
cell
too
damaged
from
great
cell
The
proteins,
the
to
dies;
this
presence
also
misfolded
earlier)
that
consequences
corrected,
is
of
mentioned
harmful
be
PROTEIN
APOPTOSIS
the
called
of
mitochon-
the
terminal
Proteins
protein
That
are
Pathogenesis
Degraded,
Leading
to
Their
Misfolded
Loss
of
CFTR
LDL
Loss
of
LDL
Lack
of
the
receptor
Proteins
pigmentosa
Deficiency
CFTR
Hexosaminidase
Caused
(er)
(BH3-only
α
subunit
sides
Diseases
UNFOLDED
RESPONSE:
the
response,
induced
Misfolded
fibrosis
Familial
response
by
the
Affected
Diseases
TERMINAL
response.
Disease
Cystic
is
of
caspases
proteins
RESPONSE
protein
When
apoptosis
protein
Caused
protein
unfolded
proteins.
of
PROTEIN
detected
Activation
degradation
ADAPTIVE
UNFOLDED
of
proteins
That
Result
in
ER
in
Stress–Induced
Rhodopsin
Abnormal
death,
leads
to
receptor
defects
leads
lysosomal
to
in
chloride
transport
hypercholesterolemia
enzyme
leads
to
storage
of
GM
2
ganglio-
neurons
Cell
Loss
folding
of
resulting
rhodopsin
in
causes
photoreceptor
loss
and
cell
blindness
sc
Creutzfeldt-Jakob
disease
Prions
Abnormal
folding
and
folding
of
aggregation
of
PrP
causes
neuronal
cell
death
Alzheimer
disease
Aβ
peptide
Abnormal
rons
Diseases
the
Caused
by
Misfolded
Proteins
That
Result
From
Both
ER
and
peptide
causes
aggregation
within
neu-
Stress–Induced
Cell
Loss
and
Functional
Deficiency
of
Protein
Alpha-1-antitrypsin
deficiency
α-1
antitrypsin
Storage
of
absence
elastic
Selected
CFTR,
Aβ
apoptosis
illustrative
Cystic
examples
fibrosis
of
diseases
transmembrane
are
shown
conductance
in
which
regulator;
protein
LDL,
misfolding
low-density
is
thought
lipoprotein.
to
be
the
nonfunctional
of
enzymatic
tissue,
major
giving
protein
activity
rise
mechanism
of
to
in
in
hepatocytes
lungs
causes
causes
apoptosis;
destruction
of
emphysema
functional
derangement
or
cell
or
tissue
injury.
CHAPTER
Environmental
metabolic
and
Telomere
insults
Cell
1
Injury
and
Abnormal
shortening
protein
Cell
Death
11
Calorie
homeostasis
restriction
ROS?
Insulin/IGF
Accumulation
mutations
in
of
Cellular
DNA
TOR
Proteins,
replication
signaling
misfolded
proteins
Defective
Altered DNA
repair
transcription
DECREASED
CELL
CELL
DECREASED
FUNCTIONS,
CELL
LOSS
CELL
LOSS
FUNCTIONS
DNA
CELLULAR
repair
AGING
Protein COUNTERACTS
Fig.
1.13
proteins
calorie
Mechanisms
are
restriction,
Insulin-like
agng,
e
response,
•
“naked”
causng
D efectve
muaon
•
Atered
ors.
par
ere
nang
ewer
In
as
e
One
DNA
a
o
o
o
mechanisms
by
activating
reactive
acvae
e
ncreased
oxygen
DNA
repcave
proens,
damage,
of
replicative
cellular
various
species;
TOR,
damage
urnover
w
possby
afec
n
denng
obser vaon
s
grow
a
caore
acor,
nrnsc
responses
so
o
ese
a
caore
cyce
ess
and
dyng
e
bo
and
some
ypes
o
as
aerosceross,
ype
2
such
factors.
no
reeved.
scema
as
IGF,
For
due
exampe,
o
dabees,
cancer.
a
an
Grow
survvng
ces
are
e
can
be
reave
cardac
ack
exampe
due
o
are
dea
ess-dferenaed
by
o
capabe
and
a
s
o
yper-
oxygen
o
varey
responsbe
remova
repcaon
oten
ncreased
n
or
paoogc
by
ce
ypes.
o
e
e
and,
n
and
Posparum
o
ducuar
nduced
smuang
may
o
ormones
proeraon
some
occurs
and
response
yperpasa
or
o
o
progenor
Hyperpasa
smuaed
pysoogc
or
ces.
pysoogc
proeraon
produced
acors
o
yperropy
breas
ater
eer
dferenaed
popuaons
w
ceuar
o
s
ce
Hyperpasa
acors
mones.
suc
s
nsances,
conans
enargemen
dsposes
dseases,
sress
proeraon,
suaons,
epeum
many
transcription
myocarda
some
smu.
ces nduce ow-eve nlammaton, and cronc nlammaon pre-
o
e
concurreny
grow
damaged
n
ssue
same
errors.
abnormaes,
cause
ncreased
or,
occur
sg-
sufer
and
misfolded
stresses,
Hyperpasa s an ncrease n e number o ces n an organ a sems
ces
n
and
homeostasis
and
rapamycin.
njury
can
decreased
devery, and evenuay gve rse o cardac aure.
•
resrcon
reduces
of
and
environmental
pathways
ropy
ac-
paways,
resrcon
ces
grow
Some
target
organ
and
accu-
aging.
signaling
senescence.
ogeer
senescence,
rom
neres
nrgung
ese
ROS,
sae
due
may
repcaon–reaed
addon
a
aging
DNA
proens.
grea
nsun-ke
ends
ener
aging.
best-described
factor;
nraceuar
patways
been
o
e.
by
o
msoded
because
proongs
•
o
o
omeostass,
syness
sgnang
growth
ces
the
cellular
counteract
cromosome
e
proten
decreased
among
of
AGING
by
or-
proeraon
ces
n
an
o
organ
(e.g., grow o resdua ver oowng para epaecomy, caed com-
pensatory
CELLULAR
ADAPTATIONS
TO
yperpasa).
napproprae
Adaptations
metabolic
their
are reversible changes in
activity,
or
functions
of
the
cells
number,
in
size,
response
phenotype,
to
changes
progeserone
environment.
o
be
paoogc.
androgens
ces
o
medaors
uerus
e
norma
(e.g.,
durng
case
o
Pysoogc
smuaon
e
by
and
or
o
musces).
usuay
ormones
ormone-nduced
pregnancy),
bones
adaptatons
e
or
represen
enargemen
demands
Patoogc
o
o
e
mecanca
adaptatons
are
njur y,
bu
paopysoogc
•
Hypertropy
men
s
o
e
caused
a
e
expense
adapaons
s
an
organ
eer
ncrease
(Fg.
by
an
o
can
n
1.14).
norma
ake
e
I
sze
can
ncreased
uncon.
severa
be
o
dsnc
sress
ces
uncona
or
demand
or
n
by
e
o
and
organ
o
enarge-
py
oowng
sress.
an
weg
Cardac
exampe
o
tng
yperropy
paoogc
s
n
an
e
esrogen
adapaon
yperenson
yperropy
eves.
workoad
ormona
o
or
Musce
ncreased
aorc
resung
rom
dsuse
yperro-
mecanca
vave
dsease
ncreased
s
work
and
resu
grow
o
ac-
Bengn
cause
prosac
obsrucon
o
yperpasa
e
low
o
s
nduced
urne
and
by
preds-
suc
sgnas
as
a
abae.
In
afecng
some
e
cases,
perssen
endomerum,
ses
paoogc
e
sage
or
I
s
caused
acvy)
by
and
decreased
ncreased
proen
proen
syness
(due
breakdown
o
med-
aed by e ubqun–proeasome paway. Causes ncude a decreased
and
(as
n
aropy),
ces
ncreased
grow
srnk.
ormone
by
can
meaboc
pregnancy
caused
ypcay
Atropy s a decrease n e number o ces and, ence, may cause an
smuaon. For exampe, pysoogc enargemen o e uerus durng
s
s
ormones
muaons and oncogenc ransormaon.
•
reduced
paoogc
by
e deveopmen o cancer because proerang ces are suscepbe o
orms.
resung
pysoogc
baance.
and
yperpasa,
(n
responses
Pysoogc
wen
and
sress a aow ces o moduae er srucure and uncon and us
escape
yperpasa
smuaon
sa rom neopasa: Unke neopasc grows, yperpasa s reversbe
cemca
breas
excessve
pose o urnary rac necons. I s mporan o dsngus yperpa-
responses
endogenous
and
ors, as n endomera yperpasa resung rom a dsurbed esrogen–
in
Ceuar adapaons may be par o pysoogc ceuar responses or
may
Paoogc
STRESS
mmobzaon
progressve
smuaon
undergo
aropy
(as
or
denervaon
scema,
n
raer
reduced
menopause).
an
dea
as
o
Faced
an
musce,
nuron,
w
eadng
and
o
reduced
manuron,
adapaon
o
reduced
energy suppy. I s oten assocaed w ncreased auopagy.
•
Metapasa
response
o
s
a
cange
sress
n
o
one
wc
a
adu
ce
ce
a
s
ype
o
sensve
anoer.
o
a
I
s
sress
a
s
oad. In a orms, ormones and mecanca sensors acvae sgnang
repaced by anoer ce ype a s beer abe o sur vve e adverse
paways a ead o ncreased proen syness and assemby o more
envronmen.
organees,
ssue
o
sress,
and
us
enargemen
yperropy
can
o
progress
e
o
ce.
Aoug
unconay
an
adapaon
sgncan
ce
or
sem
e
ces
mecansm
o
s
dferenae
oug
aong
a
o
be
new
reprogrammng
paway.
o
Exampes
ncude squamous meapasa o e bronca coumnar epeum
12
CHAPTER
Cell
1
Injury
and
A
Cell
Death
C
B
Adapted Adaptation: Normal
myocyte response
to
myocyte
(hypertrophy) increased
load
D
E
Fig.
1.14
nancy.
partum
plump,
tion.)
1
n
cronc
squamous
1.15).
er
broncus
e
ar ways
smu,
and
ng
upper
n
rom
e
as
n
uncon;
n
o
bronc
o
Barre
w
o
e
uterus
cells
a
o
e
sur vve,
ce
smooth
gravid
with
left
oten
epeum
o
a
Physiologic
and
a
uterus;
severe
com-
n
acon,
a
o
proec
rggerng
neopasc
carcnoma
o
rans-
e
wall
e
e
is
•
ces
man
Some
ACCUMULATIONS
IN
exampes
may
which
accumulate
may
mediastinal
degrees
of
be
abnormal
harmless
lymph
injury.
nodes
(e.g.,
of
amounts
carbon
city
and
uterus.
C,
preg-
for
(C)
post-
Large,
same
magnifica-
myocardium
(thickness
cm.
be
or
ocaed
n
may
e
be
o
and
are
during
removed
n
e
produced
abnorma
deposon
descrbed
n
and
may
wn
be
organees
syneszed
by
esewere.
nraceuar
degradaon
or
cyopasm,
nuceus,
or
o
an
e
accumuaons
excessve
producon
abnorma
exogenous
are
o
an
mae-
oowng.
eFg.
1.2),
mos
ay
and
w
or
ver
n
n
obese
dsease
coeser y
pd
oten
(see
esers.
e
ver
oowng
ndvduas
Caper
as
proonged
componen
o
13).
Pagocyc
(rgycerdes,
a
ces
coesero,
may
and
become
coeser y
CELLS
of
various
particles
dwellers)
(B
consumpon
Coestero
esers)
Cells
may
subsance,
overoaded
PATHOLOGIC
2
paways
nonacooc
•
(B).
uterus
was
Fatty cange (steatoss). Seaoss s e accumuaon o pds (Sup-
acoo
esopagus).
the
non-gravid
than
or
of
that
Normal
remova
pemena
ars-
(D)
ysosomes),
endogenous
ra.
a
with
subsance
afeced
e
(left)
from
thicker
nadequae
ung)
adenocarcnoma
cells
compare
(ypcay
e
wo
hypertrophy
uterus
hypertension.
ventricular
(Fg.
gravid
muscle
esopagea
car y
perssence
(esopagea
The
relux
epeum
se
from
(A-C)
(right)
uterine
patient
gasrc
provde
e
be
in
hypertrophy.
squamous
(squamous
rac
muscle
cronc
ces
hypertrophy.
normal
spindle-shaped
meapasa
and
can
a
hypertrophy
bronca
Aso,
epeum
of
smooth
nsance,
mucus
norma
gasronesna
seng
Small
w
aows
or
pathologic
Myocardial
coumnar
necon.
e
(E)
paens
produce
meapasc
ormaon,
cm).
and
uncons
(B)
Myocardial
meapasa
canno
mporan
E)
and
appearance
hypertrophied
1.5
smokers
Gross
bleeding.
(D,
epeum
Aoug
promses
to
Physiologic
(A)
or
in
may
substances,
the
lungs
cause
and
varying
1.3),
n
severa
mosy
osm
o
Caper
pds.
8).
dferen
paoogc
caracerzed
O
ese,
by
processes
ncreased
aerosceross
nake
s
e
(Suppemena
or
decreased
mos
eFg.
caab-
mporan
(see
CHAPTER
Cell
1
mmunogobuns
some
oc
•
pasma
yane”
(see
browns,
a
a
s
Squamous
membrane
columnar
metaplasia
n
o
eFg.
aropc
by
and
ssues.
Death
accumuae
anges
ypes
Is
so
may
maera
ree
1.5).
njur y,
Cell
n
n
13
e
roug
neurons;
and
ER
o
“aco-
13).
severa
granuar
produced
radca–medaed
msod
Caper
fuscn
s
and
neurobrar y
Pgmens
(Suppemena
Normal
a
ces;
Pgments.
ens
Basement
Injury
accumuae
composed
radca–medaed
accumuaon
s
oten
Hemosdern
s
seen
a
n
n
o
n
pd
ces
oder
ces.
pds
s
Lpo-
and
pro-
peroxdaon
a
sgn
o
ree
ndvduas
emogobn-derved
and
brown
epithelium
A
pgmen
•
(Suppemena
and
oer
ces
ron
overoad
n
eFg.
1.6)
condons
(see
Caper
o
a
accumuaes
ncreased
red
ce
n
pagocyes
breakdown
or
9).
Gycogen. Excessve nraceuar deposs o gycogen are assocaed
w
abnormaes
n
e
meabosm
o
eer
gucose
or
gycogen.
Gycogen may accumuae n poory conroed dabees or n gyco-
gen
•
sorage
dseases
(see
Caper
13).
Cacum. Cacum sa deposs are seen n a varey o dsease saes.
Dystropc
cum
n
and
areas
ropc
caccaton
s
o
e
caseous
necross
caccaon
cc
senoss
due
o
o
occurs
deposon
e
can
aorc
n
o
e
seng
cacum
and
ave
n
sas
advanced
uncona
vave
o
n
causng
norma
njured
serum
(e.g.,
aerosceross).
Dys-
consequences,
et
ca-
ssue
venrcuar
as
n
ca-
yperropy
B
Fig.
1.15
(right)
in
Metaplasia
a
bronchus,
of
normal
shown
columnar
(left)
schematically
(A)
to
squamous
and
histologically
pressure
ccaton
epithelium
(B).
saes
o
occurs
Protens.
Morpoogcay
common
an
up
are
or
synesze
vsbe
excessve
n
11)
bodes,
proen
accumuaons;
excessve
rena
amouns
gomeruar
er
pd
vsbe
ubuar
o
damage
For
epea
ces
eadng
eosnopc
may
amouns.
proens
(Suppemena
ey
eFg.
o
rom
e
1.4).
ncusons
e
accumuaons
exampe,
wen
urne,
neproc
Oer
occur
ces
ake
wc
newy
resorb
occurs
(see
ncude
on
w
Cap-
Russe
syneszed
occurs
nersa
mucosa.
dropets
ubues
syndrome
o
ess
proten
e
exampes
comprsed
wen
are
•
ar
o
a
reaed
o
n
e
(Suppemena
seng
cancers
usuay
Amyod
brar
ssues,
organs
as
wdey
ssues
I
Amyod.
assume
n
yperparayrodsm
desrucon,
•
overoad
were
o
e
does
e
e
no
cause
o
may
processes
o
are
1.8).
s
or
s
ncreased
Measac
ungs,
ca-
seen
n
bone
cacca-
afecs
and
e
gasrc
dysuncon.
many
and
Metastatc
wc
prncpay
kdneys,
nerere
and
bu
cnca
one
eFg.
1.7).
16),
bone.
body
vascuaure,
conormaon
ey
Caper
nvovng
consss
eFg.
ypercacema,
(see
rougou
(Suppemena
mmune
o
dferen
deposed
w
e
Amyod
dscussed
proens
n
norma
uncons
deposon
n
a
exraceu-
Caper
4
s
oten
CHAPTER
1
Supplemental
tubular
of
the
the
liver.
James
at
In
displaced
most
rim
Crawford,
1.2
Fatty
cells,
of
the
liver.
High-power
well-preserved
cytoplasm
Department
of
about
the
nucleus
fat
Pathology,
detail
of
is
vacuole.
Zucker
fatty
change
squeezed
(Courtesy
School
of
into
Dr.
Medicine
Hofstra/Northwell.)
Supplemental
phages
by
eFig.
(foam
eFig.
cells,
cholesterolosis.
ogy,
University
of
1.3
arrow)
Cholesterolosis.
in
(Courtesy
the
Dr.
Washington,
lamina
Matthew
Seattle.)
Cholesterol-laden
propria
Y eh,
of
gallbladder
Department
macro-
affected
of
Pathol-
Injury
eFig.
1.4
epithelium
Rennke,
Supplemental
Cell
Boston.)
in
Department
a
Protein
patient
of
and
Cell
reabsorption
with
Pathology,
13.e1
Death
albuminuria.
Brigham
droplets
in
(Courtesy
and
the
Dr.
Women‘s
renal
Helmut
Hospital,
13.e2
CHAPTER
Cell
1
Injury
and
Cell
Death
A
B
Supplemental
indicated
by
eFig.
arrow)
1.5
and
Lipofuscin
(B)
electron
granules
in
microscopy
a
cardiac
(note
the
myocyte
shown
perinuclear,
by
(A)
light
intralysosomal
microscopy
(deposit
location).
B
A
Supplemental
golden-brown,
sian
blue
eFig.
finely
1.6
Hemosiderin
granular
granules
pigment.
(B)
Iron
in
liver
cells.
deposits
(A)
shown
Hematoxylin-eosin–stained
by
a
special
staining
section
process
called
showing
the
Prus-
reaction.
Supplemental
eFig.
1.7
Dystrophic
aortic
heart
with
calcific
valve
thickened
in
and
a
fibrotic,
and
calcification
aortic
behind
each
stenosis.
cusp
are
of
It
is
the
aortic
markedly
irregular
valve.
View
narrowed
masses
of
looking
down
(stenosis).
piled-up
The
dystrophic
onto
the
semilunar
unopened
cusps
calcification.
are
CHAPTER
A
Cell
1
Injury
and
Cell
Death
B
C
Supplemental
deposits
of
the
of
deposits
almost
Hinton,
eFig.
amyloid
totally
in
when
1.8
walls
of
observed
obliterated
Department
Amyloidosis.
the
of
by
the
blood
by
a
(A)
section
polarizing
massive
Pathology,
A
vessels
and
of
of
Texas
of
liver
stained
sinusoids.
microscope.
accumulation
University
the
along
(C)
In
amyloid.
(B)
the
(B,
Southwestern
with
Note
kidney,
red
reveals
yellow-green
the
Courtesy
Medical
Congo
the
glomerular
Dr.
Trace
School,
architecture
Worrell
Dallas.)
pink-red
birefringence
and
is
Sandy
13.e3
2
Inflammation
and
Repair
O U T L I N E
Overview of Inflammation, 14
Causes
of
Sequence
Features
Cells
Acute
of
Inflammation,
of
of
Events
Acute
in
and
Vascular
Chronic
Cellular
Reactions,
Resolution
of
OF
Inammation
is
Outcomes
Inflammation,
15
Chronic
15
to
brings
Clinicopathologic
Tissue
17
Repair,
20
consequences
e
anbodes,
n
e
o
e
were
In
as
and
bood,
ssues,
sue
such
bu
ey
be
ces
nvoved
n
ey
uncon
on
s
nlammaor y
se
be
as
(e.g.,
response
s
ts
•
(e.g.,
noe
crca
ater
an
aso
or
on
pan,
a
par
o
organ
e
the
Some
ssues,
reas.
s
and
response
uncona
appropraey
denoes
ea
regu-
and
s-
nlammaon
menngs).
[as
n
(e.g.,
26
Chronic
Inflammation,
Features
of
Chronic
Features
of
Tissue
26
Inflammation,
27
Repair,
28
be
e
n amma on.
n ammaor y
or
no
a a ,
o
v ra ,
mos
D eren
resp ons es ,
as ng
p aras c)
and
m d
o
cron c
and
me d c a y
n e c ous
rom
d amage,
proonge d
u nga ,
common
p a ogens
ac ue
s e vere
e c
n am ma on
s ysem c
re ac ons
m crob a
mp or an
a
a
range
a
re ac ons
c aus e
ox -
c aus es
o
c aus es
a
exens ve
c an
ssue
njur y.
Immune
em
reactons occur wen e normay proecve mmune sys-
damages
gens
ndvdua’s
ese
n
Caper
assocaed
o
end
w
Necross
oss
s
4).
be
cronc
rom
bood
necroc
o
any
a
ssues
reacng
major
and
eer
o
aergc
by
o
ssue
smu
or
dseases
and
aackng
envronmena
cause
e
perssen
njur y
e
canno
dcu
o
se
an-
subsances
n
ese
nlammaor y
be
cure
emnaed,
and
are
oten
nlammaon.
cause,
suppy,
or
Because
auommune
reacons
own
dseases)
Inlammaon
(see
responses
by
e
(auommune
dseases
n
Inlammaon
(b ac er a ,
among
even
ecs
sere
njur y
nlammaon
as
due
n
o
narcon
moecues
caused
reeased
ces.
or
normay
armess
commensa
envronmena
mcrobes,
or
agans
se
dseases])
and
even
some
nlammaon
as
n
gou
and
endogenous
arge
substances
amouns
coesero
are
smuae
deposed
cr ysas
n
n
poenay
ssues
(e.g.,
armu
urae
cr ys-
aerosceross).
he smuus s persstent and canno ready be emnaed (e.g., e
Too
e
a
causes
nlammaon,
Sequence
ubercuoss)
wc
s
ypcay
manesed
by
ncreased
suscepby o necons, s aso probemac and s mos oten caused
quanave
rom
or
repacemen
eukocyes
by
quaave
o
cancer
e
deecs
marrow
erapes,
or
by
use
n
eukocyes,
cancers,
o
wc
desrucon
may
o
mmunosuppressve
nlammaor y
resores
ssue
reacon
ses
n
moon
e
process
o
drugs.
repar,
The
wc
negry.
he
Events
hese
reactions
major
remova,
seps
a
Recog nton
or
and
seps
are
in
n
o
e
and
be
e
nl amma on.
consists
recruitment
by
(e
e
descrbed
noxous
he
of
of
response
repar
medaed
w
Inflammation
response
reguaon,
medaors
1.
of
inammatory
vascular
resu
norma
Ater e noxous smu and e damage ey cause are emnaed,
e
23
Foregn bodes (e.g., spners, dr, suures) may ec nlammaon,
agans
aerges]
auommune
mycobacerum
by
are
(aerges).
useu
norma
o
norma
body.
n
ns
e
ces),
crcuae
o
resde
ever,
an
bood
normay
n
needed
and
tissues).
damage
se
ookou
empass
o
and
ese
are
toxins)
(we
preven
any
they
or
damage
rom
msdrected
n
a
o
o
tissue
:
I
[as
o
conjuncvs,
•
ssues
e
e
cells
responses
consequences
I s nadequatey controed
s
on
mporan
•
subsances
Mos
recrued
o
where
eukocyes
sequesered
muc
sux
sites
and
microbes
necrotic
proens.
are
appendcs,
damagng
(e.g.,
sennes
s
he
the
(e.g.,
nlammaor y
armu
bu
of
Inflammation,
25
28
Clinicopathologic
infections
ncude
rapdy
medcne,
manenance.
can
injury
to
to
injury
compemen
ey
cnca
of
deense
can
been
a
o
were
mparmens),
aed
of
response
molecules
cause
medaors
Acute
Inflammation,
27
Angiogenesis,
Inflammation,
host
and
the
Acute
20
of
INFLAMMATION
a
cells
eliminate
of
Features
Reactions
Infec tons
that
Inflammation,
Inflammation,
Cellular
16
Acute
OVERVIEW
14
16
Reactions,
of
Clinicopathologic
Inflammation,
Inflammation,
Inflammation,
Mediators
14
sequential
are
5
events
involving
leukocytes.
Rs),
recognon,
descrbed
coordnaed
recrumen,
nex
acons
(Fg.
o
2.1).
cemca
aer.
agen
ce s
a
a
s
r g ger
e
n a ng
s mu us
nl amma on
( ssue-
resden s en ne ce s, pago c yes, and o ers, des cr b e d aer) are
Causes
of
e qupp e d
Inflammation
w
subs ances The
major
causes
of
inammation
are
infections,
14
tissue
necrosis,
and
environmental
a
rom
re cog nze
d amage d
mcrob a
ce s.
pro duc s
C e u ar
re cepors
and
or
immunologic
mcrob es reactions,
re cepors
ree as e d
substances.
c an
be
o c ae d
n
p asma
membranes
(or
ex race u ar
CHAPTER
and
STIMULUS
(microbes,
necrotic
tissue)
BY
TISSUE
compemen
(ops onze d)
2.
RECOGNITION
or
Inflammation
2
w
Recr utment
CELLS
B e c aus e
o
proens,
an b o des
eu ko c yes
bo o d
p er us es
and
w c
and
and
re cog nze
15
mcrob es
co ae d
compemen.
p as ma
e ver y
Repair
proens
ssue,
no
eu ko c y es
e
and
ssues .
proens
(”sentinels”)
suc
o
PRODUCTION
OF
as
compemen
mcrob a
be
d evere d
Wen
o
any
p a ogen c
vas c u ar z e d
mcrob es
se
nvad e
e
MEDIATORS
ssues,
aer,
or
ssue
ce s
mono c yes
rapd y
Blood
c an
nvas on .
d e,
and
re cr ue d
eu ko c yes
( rs ,
y mpo c y es)
rom
e
and
crc u a on
man y
neu rop s;
p as ma
o
e
proe ns
are
ex ravas c u ar
se
vessel
w ere
e
p asma
bo o d
Exudation
and
of
plasma
vess es
de a
fluid
proteins
3.
o endng
proens
agen
rom
and
e
s
o c ae d.
bo o d
Te
re qures
s e cre on
o
exo dus
o
co ord nae d
me d aors ,
c e s
and
canges
d es c r b e d
n
n
more
aer.
Remova o e smuus or nlammaon s accompsed many by
pagocyc
DILATION;
ces,
wc
nges
and
desroy
mcrobes
and
dead
ces.
Pagocyoss, descrbed aer, nvoves ree sequena seps: (1) rec-
INCREASED
ognon and aacmen o e parce o be ngesed by e eukocye; PERMEABILITY
(2) engumen, w subsequen ormaon o a pagocyc vacuoe;
and
4.
(3)
desrucon
Reg uaton
o
e
o
e
ngesed
resp ons e
s
maera.
mp or an
or
er mna ng
e
re ac -
on w en as accompse d s pur p os e. In arge p ar , er m na -
on
s
a er
b e c aus e
e
o
e
s mu us
s
d e c ay
o
me d aors
e mnae d.
I
s
and
key
d e a
a,
o
n
eu ko c yes
conc er
w
LEUKOCYTE
e ADHESION
n ammaor y
resp ons e,
ac ve
regu aor y
me can sms
a s o
TO
are
r g gere d
a
s er ve
o
ur n
o
e
resp ons e.
ENDOTHELIUM
5.
Repar
eas
Features
The
two
differ
of
e
damage,
Acute
principal
in
kinetics
and
and
dscussed
Chronic
patterns
and
s
many
of
a
e
o
e
caper.
Inflammation
inammation,
other
end
acute
and
chronic,
features
LEUKOCYTE
Acute
nammaton
s
a
rapd,
oten
se-med,
response
o
nec-
or
ours
TRANSMIGRATION
ons
and
and
s
zed
o
by
ssue
sor
e
emgraon
LEUKOCYTE
ACTIVATION
ELIMNINATION
OF
AND
ng
2.1
Sequence
tory
reactions,
of
events
recognition
of
in
inflammation.
an
smuus
offending
In
agent
most
(the
inflamma-
stimulus
repared.
reacon
leads
to
the
production
of
chemical
mediators,
Bu
the
vascular
and
cellular
o
lud
deveops
ours
and
o
e
a
reacon
wn
ew
pasma
predomnany
emnaed,
reactions
that
serve
to
e
progresses
mnues
days).
proens
I
caracer-
(edema)
neurops.
subsdes
s
and
I
and
e
e
ofend-
o
na
a
response
proraced
as
ype
o
o
cear
resdua
e
njur y
smuus,
nlammaon
a
s
e
caed
nlammaon.
which
Chronc elicit
(severa
eukocyes,
s
ypcay
for
cronc
inflammation)
duraon
exudaon
o
I
STIMULUS
s
Fig.
damage
eliminate
nammaton
may
oow
acue
nlammaon
or
arse
the
de
novo
(and
acue
nlammaon
may
be
supermposed
on
a
back-
offenders.
ground
o
duraon
p a ogens),
(or
e
ce
c yos o
njur y
re cepors
ke
a
by
k nes,
o
w os e
L eu ko c yes
re cepors,
and
o
o
a
pro duc s
aer.
e ver-nducng
re cepors
e
a
c yos o
pres en
resu
e y
are
c a e d
e
A
c a e d
and
are
p a ogen-
(PAMPs
e ads
c yo-
subs e
o
o
c yos oc
c a e d
e
c yok ne
nereu k n-1
or
p or on
Fc
To -
re cepors
compex
o
o
e
pron-
(IL-1).
an b o des
s
ympoc yes
and
rom
ncudng
pro duc on
e
n
es e
ncudng
p aer ns
nl amma on,
mu proen
e
are
re cog nze
moe c u ar
des cr b e d
s mu aes
express
o ers.
e y
o
or
bre a kdow n).
am es,
Engagemen
ac vaes
w c
and
a s o
are
DNA
and
ce
d amage
moe c u es
o
b e c aus e
de ad
me d aors
unc ons
mcrob es),
ce
moe c u ar
d amage-ass o c ae d
re cepors
l ammaor y
pro duc
re cepors
resp e c vey).
nammas ome,
o
re cog nze
a
s e vera
mcrob a
pro duc on
NOD- ke
ngese d
S ens ors
e y
acd,
NOD- ke
and
DAMPs,
e
ce s:
ur c
b eong
ass o c ae d
(or
agens).
re cog n on
ac vae d
o
o
(e.g .,
re cepors,
p aer n
and
endos omes
n race u ar
cronc
and
was
know
s
as
and
w
Cronc
more
macropages,
ssue
e
nlammaon
desrucon,
proeraon
o
s
o
e
onger
presence
bood
vesses,
ibross.
Aoug
on
nlammaon).
assocaed
a
e
ey
response
many
dsncon
s
a
based
dfer
o
n
and
response
bacera
and
beween
on
e
severa
ofendng
bacera
necon
some
e
orgnay
vra
o
oer
acue
duraon
ways
agens
(Tabe
a
necons
agens
a
paogens,
are
Acue
dead
as
we
emnaed,
and
suc
cronc
eradcae,
and
now
nlammaon
ces,
o
se
nlamma-
reacon,
ready
dcu
we
cronc
e
2.1).
and
are
as
and
o
suc
as
envronmena
angens.
Cells
The
of
cells)
in
he
a
Inflammation
principal
the
major
deec
cells
of
circulation
ces
o
paogenc
inammation
and
are
leukocytes
(white
blood
tissues.
nlammaon
mcrobes,
are
oxns,
(1)
and
ssue-resden
producs
o
ce
sennes
damage,
16
CHAPTER
Table
2.1
Acute
and
Inflammation
2
Chronic
and
Repair
Inflammation
Acute
Inflammation
Chronic
Onset
Rapid:
minutes
Slower:
Duration
Typically
Cellular
Mainly
infiltrate
brief
to
hours
(days)
Inflammation
days
Prolonged
neutrophils
Macrophages
(derived
from
blood
monocytes),
lymphocytes
Tissue
injury
Usually
self-limited
Scarring
Uncommon
Major
Histamine,
mediators
prostaglandins
cytokines,
Local
and
Common
systemic
signs
complement
and
leukotrienes,
Pyogenic
death
Immune
reactions
Trauma
(e.g.,
necrosis
Antibody
deposition
fungi,
some
Intracellular
sis),
tissues
in
burns,
Not
tissues
(in
autoimmune
immediate
dis-
T
human
deposition
Infections,
acute
ces
many
a
o
e
emnae
he major sentne ces are:
•
D endrtc
ces,
so
medaors
e
•
Sometimes,
in
tissues
(e.g.,
named
noxous
syndrome
because
o
nlammaon,
and
(2)
•
recognze
dspay
proen
mcrobes
angens
and
o
o
T
dead
er
ces,
o
ces
w
dendre-ke
and
nae
aso
Mast ces are ocaed adjacen o bood vesses.
•
Tssue-resdent
macropages
are
presen
n
a
(e.g.,
Kuper
sysem,
mos
ces
aveoar
n
e
ver,
macrophages
macropages
are
mcroga
n
e
derved
n
ung).
responses.
rom
connecve
e
bood
Acute
cenra
rom
emaopoec
sem
ces
nervous
nlammaon,
cells,
Acue
ssues
monocyes,
n
e
bone
progenors
deveopmen
and
are
n
e
yok
sac
and
ea
ver
eary
durng
dever
were
bood
eukocyes,
no
e
monocyes
or
se
PMNs)
o
monocytes,
nlammaon.
maure
no
are
Foowng
macropages.
recrued
er
rom
enry
Neurops
The
e
respond
macropages
ved.
more
become
Aoug
pagocyoss,
ey
rapdy
n
cemoacc
progressvey
bo
dfer
o
ce
e
ypes
are
span
and
medaors,
domnan
sare
e
because
common
specazed
no
bu
ey
moe
•
acves
o
(T abe
Oer ces pay dverse roes n varous nlammaor y reacons:
•
Lymphocytes, especay T ymphocytes, are promnen wen e
adapve
mmune
response.
hs
s
oten e case w vra necons and auommune and aergc
reacons.
aso
Anbody-producng
be
promnen
n
B
ymphocytes
reacons
o
and
parcuar
atherosclerosis,
asthma,
fibrosis
seen
n
aergc
reacons
and
necons
parases.
is
a
rapid
antibody
and
and
tissue
response
to
microbes,
toxins,
deposition.
consss
pasma
o
vascuar
proens
proens
ge
and
rom
rd
o
e
e
ceuar
bood
noxous
reacons
no
e
a
ssues,
subsances
a
pasma
smu.
ces
changes
in
blood
increased
o
ces
aeraons
and
n
vessels
during
acute
inammation
are
permeability.
pasma
bood
proens
vesses.
he
rom
e
na
bood
canges
no
are
ssues
daon
e
ex
o
Vasodaton
eukocyes.
s
nduced
by
e
acon
o
severa
medaors,
noaby
samne, on vascuar smoo musce. I irs nvoves e areroes
and
en
eads
o
e
openng
o
new
capar y
beds
n
e
area.
he
resu s ncreased bood low, wc s e cause o ea and redness
are
uncon
an
exposure
and ncreased permeaby o e vesses, oowed by canges a pro-
w
•
ecs
radiation
beryllium)
Reactions
ex
•
(er yema)
a
Increase
vascuar
n
conracon
racon
agen
ces
and
requres
more
2.2).
ofendng
silica,
response.
major
dilation
abundan eary n e reacon because ey are more numerous n e
and
low-dose
(e.g.,
arthritis,
oten
nlammaon
ese
he
and
and
eukocyes
eced
ong-ved.
he wo major casses o crcuang pagocyes, neutrophs (poymor-
may
repeated
wc
Phagocytes are ces specazed or eang and kng ofendng agens.
ponucear
diseases
marrow.
Many o e ssue-resden macropages are derved rom ema-
opoec
cause
inflammatory
INFLAMMATION
Vascular orgnae
are
emnc
inammation
necrotic
Durng
tuberculo-
fungi
and
and mos organs. hey are gven speca names n dferen organs
onger
inflam-
projec-
capure
mmune
•
me
acute
Mycobacterium
hepatitis),
underlying
particles
Rheumatoid
Eosnophs
subsances.
bood
in
gout)
distress
ACUTE ons,
ssues,
involved
hypersensitivity
radiation
respiratory
(e.g.,
(e.g.,
frequent
pulmonary
produce
pagocyc
a
bacteria
viruses
cell–mediated
diseases
e
mediators
milder
Inhaled
Crystal
of
of
IgE-mediated
injury,
staphylococci),
toxins
Others
Examples
(e.g.,
influenza).
Ischemic
Physical
Environmental
•
other
mation
Usually
bacteria
eases),
aso
extensive
Cytokines,
proteins
Prominent
viruses
and
be
causes:
Infections
Cell
May
Prominent
o
s
e
s
eced
ca
mos
o
sows,
o
common
by
o
e
nlammaon.
permeabty
endoea
a
e
w
cause
openng
o
(wn
e
eakage.
eukorenes,
o
a
ssue.
wo
30
njur y.
and
medae
hs
and
occurs
mnues).
Drec
mecansms:
nerendoea
vascuar
15
by
endoea
o
vasodaon,
proens
no
occur
drec
bradyknn,
medaor
pasma
can
and
mecansm
aso
vesses
ces
ces
samne,
aowng
roug
se
endoea
medaors
exposure
e
os
response
oer
cem-
rapdy
he
bood
deense
endoea
Con-
spaces
o
njur y
ater
low
pass
s
e
CHAPTER
Table
2.2
Origin
HSCs
in
bone
marrow
HSCs
in
Many
tissue-resident
in
tissues
1–2
days
bone
liver
marrow
(early
Inflammatory
Responses
to
activat-
Rapid,
stimuli
Reactive
oxygen
Rapidly
species
Nitric
short-lived,
mostly
degranulation
and
enzymatic
More
activity
induced
(respiratory
oxide
Low
levels
Degranulation
Major
Cytokine
Low
or
by
assembly
of
phagocyte
oxidase
Less
inflammatory
17
reactions)
stem
cells
in
yolk
sac
or
development)
days
macrophages:
prolonged,
gene
in
(in
macrophages:
macrophages:
Tissue-resident
ing
Repair
Macrophages
fetal
span
and
Phagocytes
Neutrophils
Life
Inflammation
2
slower,
or
weeks
years
often
dependent
on
new
transcription
prominent
burst)
none
response;
Induced
induced
by
cytoskeletal
rearrange-
Not
following
transcriptional
activation
of
iNOS
prominent
ment
production
levels
or
none
Major
functional
activation
NET
formation
Secretion
somal
This
table
many
(the
of
lists
the
features,
of
e
canges
ng
red
e
n
resu
a
nvoved
n
er
o
o
o
As
o
nitric
proens
of
nuclear
contents
Less
bood
ermed
sass
ou
aso
low,
o
stass,
as
synthase;
venues,
njur y
o
e
e
e
(e.g.,
ssue
oss
o
NET,
reactions
into
and
o
vesses
wc
bood
vascuar
n
s
and
resus
ncreased
concenraon
e
w
seen
bood.
sowy
mov-
soogcay
redness
(er y tema)
eukoc yes,
o
hese
prncpay
endoeum,
e
and
and
ender
irs
nlammaor y
ses
o
reacons
acue
and
nlamma-
(ympadens).
Te
p a s e s ,
a
other
inammation
e
and
thelium
into
the
and
o
e
stimulate
tissue.
e
text.
a
Note
typical
orgna
that
blood
n
smuus
end
recru
and
neurops
o
the
two
cell
neutrophil
and
nay
ympocyes,
some
cases
predomnae
apoposs
a d e s on
ea
o
(n
24
a ge n .
o
a
types
and
aergc
durng
48
e
share
monocyte
duraon
recru
mxed
e
reacons
irs
o
o
e
neurops,
nirae.
ours),
a ow ng
an d
o
2.3).
m ove m e n
nvo ve s
e x pre s s e d
o
a c
pr n c p a
s e e c ns
Te
c an
6
o
be
be
e u ko c y e s
r ans m g r a on
sep
a e r
Te
o
n a y
e u ko c y e s
pro e ns ,
Tab e
en
an d
e
e m g r a on
a d e s on
E ac
v a s c u au re .
am e s
2.2
o
wa ,
m o e c u e s ,
ce s,
e
e u ko c y e
rs
n am m a on ,
ve s s e
o e n d ng
activate
endothelial
cells
at
the
In
24
ave
acue
ours,
repaced
by
seps
s ou b e
on
on
o
n
e
e
e u ko c y e s
ce s
an d
m o e c u e s
e u ko c y e
ow ard
m e d a or s
e n d o e a
n e g r ns ,
n o
e n d o e u m
e u ko c y e s
a d e s on
an d
o
o
d v d e d
o
an d
an d
endo-
ce s
an d
b e ong
er
re c r u m e n
o
g an d s
are
e
L eukoc y te
the
binding
migration
of
of
leukocytes
cells
through
marg naton .
As
e
bo o d
ow
sow s,
eu ko c ye s ,
site
to
endo-
the
endo-
arger
e
eum. the
the
o ow ng :
mediators
subsequent
o
necons
undergo
s e
ne ar thelium
in
show
necons
eosnops,
pro c e s s
b eng of
naure
c ons s ng
rou g
• and
vra
en
(Fg.
Reactions
Cytokines
images
monocyes.
as
o
e
nlammaon,
wo
swoen
described
The
Bacera
ncreased
ymp
are
are
trap.
on
wereas
e
dranng
above
chemotaxis.
he ype o eukocye a emgraes no a se o necon or njur y
depends
e ave
nodes
and
extracellular
capares,
vesses.
Vesses
summarized
tissues,
neutrophil
burns)
(exudate)
lud
ncreased
vscosy
ocazed
parcpae
exudae.
oxide
escape
sma
deveops,
o
The
vessels
response.
ncreased
exernay
adere
blood
oxns.
he
and
macrophages.
through
on are oten engorged and congesed (ympangs), and e dranng
Cellular
transcriptional
reactions).
necrozng
no
sower
and
migrate
inflammatory
escapes
and
vesses
e
and
severe
a
to
inducible
engorgemen
mgraon
remove
in
neutrophils
ability
nlammaon.
condon
ssue.
Lympac
ep
lud
e
begn
o
mcroba
vesses,
congeston
neurops,
sep
ead
n
the
iNOS,
ces
cases
se
sma
ces,
vascuar
e
a
cells;
wc
n
some
dameer
ces
extrusion
requires
genes
Less
between
macrophages
proen-rc
edema
vesse
o
differences
phagocytosis,
stem
by
areroes
exposure
red
as
tissue
mecansm
n
by
Prominent
major
such
Hematopoietic
and
induced,
activity,
cytokine
enzymes
precursor
HSC,
Rapidly
lyso-
of
an
vess e
re d
wa ,
ce s,
sow
a ow ng
e
d ow n
e
mos
eu ko c yes
o
and
bnd
acc umu ae
o
e
end o-
18
CHAPTER
Inflammation
2
and
Repair
ROLLING
INTEGRIN
BY
Selectin
ACTIVATION
CHEMOKINES
ligand
Leukocyte STABLE
ADHESION
Integrin
(low-affinity
state)
MIGRATION
THROUGH
ENDOTHELIUM
Integrin
(high-affinity
state)
P-selectin
E-selectin
PECAM-1 Proteoglycan
(CD31)
Integrin
ligand
(ICAM-1)
Cytokines
(TNF,
Chemokines
IL-1)
Fibrin
Macrophage Microbes with
Fig.
2.2
blood
to
Leukocyte
vessels
the
migrate
toward
roles
different
in
on
adhesion;
1;
2.3
and
Adhesion
Selectin
L-selectin
and
for
then
steps
of
CD31
this
in
platelet
process:
Major
in
in
Cell
tissues.
The
from
The
the
the
in
cell
rolling;
Leukocyte
to
of
process
roll;
injury.
pierce
leukocyte
become
the
Different
the
Intercellular
molecule-1;
of
then
chemokines
increase
ICAM-1,
adhesion
first
endothelium,
source
neutrophils
transmigration.
multistep
leukocytes
across
selectins
the
endothelial
Molecules
Molecule
to
emanating
activating
(PECAM-1)
(CD31),
blood
neutrophils.
transmigrate
chemoattractants
Adhesion
Family
from
here
endothelium)
PECAM-1
Selected
migration
shown
endothelium;
glycans
Table
is
and
fibronectin
(extracellular
microbes
molecules
tumor
molecule
necrosis
adhere
to
integrins
1;
and
predominant
bound
integrins;
through
and
membrane,
play
displayed
of
adhesion
TNF,
basement
(usually
avidity
migration
activated
matrix)
IL-1,
proteo-
in
firm
interleukin
factor.
Migration
Type
Principal
Lymphocytes
Ligands
Sialyl-Lewis
X
on
various
glycoproteins
expressed
on
endo-
X
on
glycoproteins
expressed
on
neutrophils,
glycoproteins
expressed
on
neutrophils,
thelium
E-selectin
Activated
endothelium
Sialyl-Lewis
monocytes,
T
P-selectin
Activated
endothelium
lymphocytes
Sialyl-Lewis
X
monocytes,
Integrin
LFA-1
T
MAC-1
Monocytes,
lymphocytes,
VLA-4
T
lymphocytes
α4β7
T
lymphocytes,
neutrophils
dendritic
cells
of
the
integrins,
ICAM,
integrins
and
their
intercellular
are
expressed
ligands
are
adhesion
also
on
many
named
molecule;
Ig,
leukocytes;
according
to
only
the
immunoglobulin;
CD
the
cell
types
nomenclature,
IL-1,
interleukin-1;
that
but
expressed
on
activated
endothelium
expressed
on
activated
endothelium
expressed
MAdCAM-1;
are
most
their
TNF,
CD
tumor
lymphocytes
ICAM-1
ated
Most
T
ICAM-1
VCAM-1
monocytes
on
necrosis
are
on
a
not
factor;
activated
expressed
lymphoid
dependent
numbers
on
endothelium
endothelium
in
gut
and
gut-associ-
tissues
particular
shown
VCAM,
on
for
integrin
for
adhesion
are
listed.
simplicity.
vascular
cell
adhesion
molecule.
All
the
selectins,
CHAPTER
•
Endotea actvaton. Two o e cyoknes secreed n response o
mcrobes
ac
on
ns
and
oer
nearby
and
smu,
endoea
gands
or
umor
ces
negrns.
o
necross
ncrease
Cyoknes
acor
e
aso
(TNF)
and
expresson
conver
e
o
•
bnd
seec-
endoe-
•
L eukoc y te
pro duc s,
rong.
o
bnd
e
a
eukocyes
aong
e
Seecn
seecns
s
on
easy
bnd,
gands
e
on
dsruped
deac,
e
ps
endoeum.
and
by
e
bnd
o
neurop
s
lowng
agan,
s
a
and
mcro-
us
on
and
ro
e
nzed
a
surace
by
The
cange
1.
acvaed
o
e
recepors
ow-any
A
by
e
o
on
endoea
endoeum.
e
rong
conormaon
a
g-any
RECOGNITION
AND
Microbes
phagocyte
o
ces
bnd
hese
and
are
cemoknes
eukocyes,
negrns
o
on
wc
e
by
dspayed
are
•
rom
e
wc
arres
are
and
nduced
irm
on
endoea
aacmen
o
ces
eukocyes
s mu ae
cemc a
Ts
C emok nes
compemen
eu ko c y e
g rad en).
sp aces,
roug
pro cess
noxious
o
substances
through
and
pro duc s ,
cemo axs
Te
e
w a ,
o er
and
o
dead
by
following
bnd
ces,
membranes
o
mcrob a
movemen
mg rae
e
ex ravas a on
se
as
b e we en
o
n am -
b e en
triggered
inammation
intracellular
steps
(Fig.
are
destruction,
cleared
mcrobes
cr ysas,
around
and
and
e
oer
oregn
parces,
parces
maera),
and
(suc
wrap
nernaze
e
as
ragmens
er
pasma
parces
Lysosome
with
enzymes
Fusion
of
phagosome
Microbe
in
with
ingested
lysosome
phagosome
Degradation
2.
by
ENGULFMENT
Phagocyte
zips
membrane
up
in
Phagolysosome
of
lysosomal
microbes
enzymes
phagolysosome
around Phagosome
with
microbe
3. ingested
KILLING
AND
DEGRADATION
microbe
Cytoplasmic Primary oxidase granule
MPO
MPO
+ O
NADPH
Active
Cl
2
oxidase
+
iNOS
NADP
•
O
•
H
2
O
2
OCl
Arginine
2
++
Fe
Membrane
NO oxidase
•
OH
ROS
Membrane
Phagocyte
oxidase O
B
PHAGOCYTIC
Fig.
2.3
rium)
Phagocytosis
involves
vacuoles
with
lysosomal
binding
to
of
the
and
intracellular
receptors
lysosomes.
enzymes
components
and
This
by
is
on
phagocyte
destruction
the
followed
reactive
2
C
VACUOLE
by
oxygen
oxidase
of
leukocyte
microbes.
enzyme
(A)
membrane,
destruction
and
of
nitrogen
assemble
Phagocytosis
engulfment,
ingested
species.
in
the
particles
(B)
In
of
and
within
activated
membrane
of
a
particle
fusion
the
of
(e.g.,
the
bacte-
phagolysosomes
phagocytes,
the
a
phagocytic
by
cytoplasmic
phagosome
to
form
the
– .
active
enzyme,
which
catalyzes
the
conversion
of
oxygen
into
superoxide
(O
2
)
and
H
O
2
.
2
Myeloperoxidase,
. present
in
the
granules
of
neutrophils,
converts
H
O
2
2
to
hypochlorite
(OCl ).
In
the
presence
of
metals
such
. ++
as
Fe
gen
be
,
H
O
2
species
released
NADPH,
2
can
(ROS)
into
also
and
be
converted
nitric
oxide
extracellular
nicotinamide
adenine
to
(NO)
tissues
highly
kill
(not
dinucleotide
reactive
ingested
shown).
hydroxyl
microbes.
iNOS,
phosphate;
pro
2.3)
to
receptors
receptor
c a e d
which
ATTACHMENT
Phagocytic
o
me d aors,
s ome
(dre c e d
eu ko c yes
vess e
eu ko c ye
that
followed
the
macropages
a
sae.
bind
by
Recognton, attacment, and engufment. Acvaed neurops and
sgnas
eukocyes
gands,
o
transmg raton .
phagocytosis
ceeds
recog-
dever
19
dapedes s.
endoeum.
aso
a
ma on.
Integrn actvaton. Cemoknes secreed by senne ces n e s-
sue
er
eu ko r enes ,
endo e a
hereore,
sowy
as
a ong
ow-any
bood.
Repair
e endoeum.
oxns.
v
o
eadng
suc
neracon
•
gy
cyoknes,
sae. Loca romboss may preven dssemnaon o mcrobes and
Leukocyte
and
Stabe adeson o eukocyes. he acvaed negrns on e eukocyes
IL-1,
a surace rom s norma anromboc sae o a proromboc
•
Inflammation
2
radicals
During
Inducible
ROS,
).
(C)
Microbicidal
phagocytosis,
NO
reactive
(OH
synthase;
oxygen
granule
MPO,
species.
reactive
contents
oxy-
may
myeloperoxidase;
no
20
CHAPTER
vesces
o
caed
recepors
bnd
e
o
IgG
•
w
Kng
and
e y
a
(e.g .,
by
as
so
(or
n
C3b
a
varey
a
gycoproens.
e
ave
Fc
use
recepors
wa
and
a
parces
recepors,
recepors
C4b
subs anc es
and
ave
are
suc
on
(wc
e
bnd
a
( e. g . ,
sp e ces
o
d amag ng
o
g ranu es ,
gone
and
ved.
a
In
because
o
n
sop
e
lammaory
and
e
medaors
addon,
varey
swc
as
sgnas
ype
o
o
e
a
o
oowng)
deveops,
acvey
aracdonc
eukorenes
beraon
(see
nlammaon
and
e
ermnae
acd
e
meaboe
annlammaory
annlammaory
neurops
process
reacon,
produced,
poxns
cyoknes,
are
se
ncudng
rom
a
pron-
(descrbed
ncudng
sor
rggers
aer),
ransormng
grow acor-β (TGF-β) and IL-10, rom macropages and oer ces.
e
o er
more
d es r uc ve
sub-
ma r x
enzy mes
mye op erox d as e,
w c
re e
r ad-
nex) .
ey
by
no
producs
cause
suc
(IFN-γ)
and
as
eukocyes
njur y
o
are
n
ssues.
a
quescen
Ater
acvaon
popoysaccardes,
cemoknes,
and
cyoknes
pagocyc
suc
recepors
of
reactions
duced
or
hese
o
a
e
and
the
at
medaors
may
o
a
described
mediators
the
reacon
se
moecues
ucs
inammation
called
activated
nlammaor y
vaed
Inflammation
of
chemicals,
site
be
or
of
the
are
nlammaon.
by
ces
recrued
hey
are
rom
(Table
a
e
ces.
induced
are
e
se
bood
ony
ncudng
necroc
are
that
pro-
2.4).
resdng
rom
produced
nlammaon,
reeased
previously
inammation,
reaction
produced
a
smuae
subsances
of
o
and
n
response
mcroba
One
e
ac-
prod-
medaor
can
smuae e reease o oer medaors. For nsance, producs o com-
pemen
Crcuang
do
Mediators
The
g ran -
ngese d
ce aves
and
and
ves ces
s e c ond ar y)
d es roy
proe as es)
me can sms
es e
yp es
(or
a
ys os omes,
o
w ou
wo
sp e c c
proe as e
o er
w
con nes
en zy mes
s er ne
oxy gen
us e
e
ngese d
many
actvaton.
neeron-γ
pagocyes
IgG-specic
Pagos omes
con an
and
re ac ve
mcroba
ce
o
pr mar y)
k ng
a
mannose
ncreased
producs
Repair
Pagocyes
e
Neu rop s
e as as e,
des cr b e d
sae
as
mcroba
bnd
e
s e ) .
e as n,
Leukocyte
suc
greay
ac vae d
g ranu es
ac vae
c a s,
are
azurop
conver s
wc
(wc
des roy
pago c ye
proen
or
s
compemen
(w ere
s ances
on
process
destr uc ton .
Tes e
pagosomes.
and
recepors).
enzy mes
u es.
or
mcrobes,
mannose
ags
s e vera
c a e d
o
s
and
compemen
e
•
o
anbodes
pagocyes)
o
bnd
ermna
ecency
opsonzed
as
endosomes
o
Inflammation
2
TNF
acvaon
acs
on
cyokne,
vaed
us
a
IL-1,
by
smuae
endoea
and
many
enzymes,
sysem
o
or
reease
o
o
oer wse
and
samne,
smuae
cemoknes.
are
cecks
e
ces
baances
e
hey
qucky
scavenged
a
and
e
producon
or
reguaes
cyokne
o
decay,
anoer
are
nbed.
medaor
nac-
here
s
acons.
suc as mannose recepors or recepors or opsonns, e eukocyes
acqure
•
he
major
ncude
and
•
e
aby
kng
reacve
ysosoma
process
o
and
neurops
(ROS)
(see
dead
and
Caper
Cell-Derived
ces.
macropages
1),
nrc
oxde,
enzymes.
hese
gens
ese
o
ydrogen
peroxde
or,
superoxde,
under
e
pagocye
wc
acon
can
o
be
con-
neurop
gens
and
Fc
damage
pysca
proens,
by
and
ssues
e
DNA,
ad
n
are
acon
and
e
normay
o
pd
ceanup
membranes
o
debrs
proeced
anoxdan
rom
enzymes
and
rom
us
desroy
necroc
ces.
ROS-medaed
dam-
a
degrade
ROS,
suc
oer
recepors,
acd.
In
many
pospopase
pospopds.
cycooxygenase
scavenge e ree radcas.
renes.
(NO)
s
made
mosy
n
macropages
oowng
ran-
hese
kocyes,
as
scrpona acvaon o e enzyme nducbe nrc oxde synase
cncay
(NOS). NO s convered o ree radcas a ac muc ke ROS.
nb
Lysosoma enzymes, ncudng easase and oer proeases, gan
•
access
o
e
E xtraceuar
ngesed
destructon.
parces
Some
o
and
dges
ese
em.
moecues,
especay
yso-
n
desroy
maon
er
mcrobes
nucear
neurop
s
mes
reeased
Some
ve
os
deveop
se
suc
as
cear
desroyed
e
coaera
responses,
wen
e
or
poen
raps
by
a
ssues.
mes
Neurops
o
(NETs).
aso
sones
and
Mcrobes
are
anmcroba
subsances
exrude
DNA
caed
rapped
a
are
n
aso
NETs.
damage
bu
s
s
s
an
oer
nevabe
usuay
usuay
s
consequence
se-med.
argeed
armess
o
Paoogc
abnormay
(e.g.,
envronmena
proec-
esons
agans
subsances
aergens).
eukocye
wc
n
rops
and
urn
and
e
ces
o
e
reease
Acute
Inflammation
acd
n
Tabe
o
acvy
PGE,
ce
o
I
by
acng
capares
s
sored
acvaon
aergens
o
producs
,
derved
s
PGD
2
en
and
IgE
C5a
n
by
on
o
on
and
mas
pao-
mas
and
2.4.
,
he
C3a,
ce
and
2a
,
on
by
bood
enzyme
membrane
e
enzyme
no
vesses
acon
on
srucura
and
e
mporan
PGF
rom
er
euko-
and
o
eu-
many
aby
o
medaors.
PGG,
ndcaes
aracdonc
e
poxygenase
depends
ese
on
acd
erapeuc
drugs
o
rom
nduce
convered
by
acons
based
mos
smu
aracdonc
PGF ,
wc
he
nvoved
e
gves
e
o
are
dverse
n
recrumen.
o
pao-
casses
PGI
eaures
PGH)
number
and
o
by
subscrp
doube
prosagandns
(prosacycn),
2
coded
a
n
bonds
nlam-
and
TXA
2
).
some
acvaor
4
of
2
seps,
and LTE
Resolution
2
A
Leukotrenes are
and
beraes
named
2),
PGE
(romboxane
•
are
1,
major
areroes
ces.
mas
nlammaor y
ave
or
PGD,
(e.g.,
are
bndng
annlammaor y
compound.
mupe
nlammaon
agans
and
dead
ormng
exraceuar
and
no
angens
and
conens,
e
daes
upon
prosagandns
producon
numera
soma enzymes, are reeased no e exraceuar space, were ey
wc
cemcas
(e.g.,
recognze
he
permeaby
endoea
eukotrenes
summarzed
eer
a
ea.
no
Prostagandns
a
e
compemen
Aracdonc
useu
e
as
e
ypes,
A2,
o
rapdy
suc
o
and
ce
wc deoxies ydrogen peroxde, as we as serum proens a
oxde
and
ces
eukocyes.
a
ncreases
reracon
sgnas,
senne
moecue
and
exposure
rauma
e
recrued
oowng.
reeased
Prostagandns
by
by
sma
ces
and
as superoxde dsmuase, wc degrades superoxde, and caaase,
Ntrc
a
and
e
causng
granues
myeoperoxdase, o gy reacve ades. A o ese subsances
are
s
by
ROS
e
Hstamne
ce
e
o
medaors
venues
o
assemby
ocay
ces,
ayzes
generaon
rapd
produced
dead
enzyme n e membrane o e pagoysosome. hs enzyme ca-
e
by
are
and
Mediators
musce
age
•
speces
mcrobes
smoo
Heay
•
mecansms
oxygen
naed
mcrobes
ngesed
oxdase
vered
•
desroy
ROS are produced many n neurops by e respraory burs,
a
o
irs
o
rse
o
vascuar
he
wc
LTB
4
venuar
ysosoma
smoo
o
generaes
or
macropages,
neurops,
and
syness
LTC
4
and
s
causng
endoeum,
enzymes.
.
a
eukorene
LTB
4
s
LTC
4
poen
s
A
4
nvoves
(LTA
4
by
cemoacc
and
generaon
and
reacons
produced
aggregaon
e
musce
eukorenes
agen
adeson
o
ROS,
meaboes,
),
neu-
o
and
LTD
4
, are produced many n mas ces and cause nense vaso-
consrcon,
broncospasm
(mporan
n
asma),
and
ncreased
Normay, oowng cearance o e ofendng agen, e acue nlamma-
permeaby o venues. In genera, eukorenes are ar more poen
ory
an
response
sponaneousy
subsdes,
because
e
acvang
smuus
s
samne.
CHAPTER
Table
2.4
Mediators
of
Inflammation
2
and
Repair
21
Inflammation
Pharmacologic
Mediator
Production
Cell-Derived
Role
in
Inflammation
Antagonists
Mediators
Histamine
Stored
as
cells
a
preformed
and
ulation
in
trauma,
molecule
basophils;
response
released
to
complement
IgE
in
granules
rapidly
of
upon
cross-linking
mast
Dilation
degran-
of
blood
increased
vessels,
vascular
Antihistamines
permeability
bind
(allergy),
to
receptors
products
itively
for
allergy;
histamine
and
inhibit
compet-
histamine
binding
Arachidonic
acid
PLA
derived
2
production
complement
releases
Produced
and
→
in
prod u c ts ,
cells
cells,
by
in
ma n y
c ell
c y to kines ,
a c id
converted
mast
other
trauma,
indu c e d
arachido n ic
pholipids
Prostaglandins
is
to
fro m
o the r
activ e
→
pho s -
m e diators
endothelial
cyclooxygenase;
products,
by
s t i m ul i
me mb r a ne
leukocytes,
complement
t y pes
activated
cytokines,
cells,
Vasodilation
by
microbial
(PGI
products
Produced
and
Table
or
in
mast
other
cells
cells,
by
leukocytes,
lipoxygenase;
products,
endothelial
activated
cytokines,
by
microbial
cells,
stimulate
pain,
vascular
PGE
(TXA
);
)
(PGD
nonsteroidal
antiinflammatory
platelet
2
fever
Many
inhibit
2
(NSAIDs)
,
inhibit
drugs
cycloo-
xygenase
2
)
muscle
products
,
2
2
Neutrophil
trauma,
increased
(PGD
aggregation;
complement
Cytokines:
)
2
PGE
Leukotrienes
and
permeability
(LTC
,
chemotaxis
(e.g.,
LTD
4
),
4
(LTB
bronchial)
involved
);
4
smooth
Leukotriene
contraction
in
receptor
antagonists
for
asthma
asthma
see
2.5
Platelet-activating
factor
Produced
(PAF)
and
in
mast
platelets
cells,
by
leukocytes,
action
of
PLA
2
endothelial
on
cells,
Vasodilation,
membrane
meability,
phospholipids
platelet
increased
vascular
constriction
aggregation
of
per-
bronchi,
(promotes
thrombosis)
Plasma
Protein–Derived
Complement
proteins
Produced
(see
Chapter
Mediators
tial
at
site
enzymatic
of
complement
(protease)
activation
by
sequen-
C5a,
activity
C3a
cytes
4)
are
chemotactic
(especially
for
leuko-
neutrophils),
Anti-C5
dilate
vessels
C3b
Synthesized
in
the
liver
in
response
to
cytokines
diseases
by
excessive
complement
coats
their
Pentraxins
for
caused
microbes
and
promotes
(in
activation
trials)
phagocytosis
Markers
of
inflammation
(acute-phase
proteins)
C-reactive
protein
(CRP)
CRP:
opsonizes
microbes
for
phago-
cytosis
Serum
Kinins
amyloid
Bradykinin:
cells
by
protein
peptide
the
(SAP)
produced
kinin–kallikrein
SAP:
in
activated
endothelial
unknown
Vasodilation,
system
increased
permeability,
vascular
bronchial
constriction,
pain
•
Lpoxns
ase
are
aso
paway,
suppress
bu
generaed
unke
rom
aracdonc
prosagandns
nlammaon
by
nbng
and
e
acd
by
e
eukorenes,
recrumen
poxygen-
e
o
poxns
cysene
cemoaxs,
Cytoknes
kocyes
and
moecues
subse
o
are
cemoknes,
o
e
se
o
o
sgnang
knes.
no
ces
and
uncon
by
oer
paways
cyoknes
major
groups
o
communcaon
ave
e
dsnc
descrbed
accordng
o
e
earer,
or
e
eads
and
2.5).
o
o
o
e
roes
arrangemen
o
known
and
sennes,
acvaon
n
are
e
hes e
n
e
on.
or
Protein–Derived
o
cyo-
acue
and
cassied
conser ved
medaors
ver
he
oowng
he
eukocyes
secreon
Cemoknes
One
mcrobes
recepors
overappng
aer.
o
eu-
messenger
(Tabe
movemen
syness
among
e
cyoknes,
Recognon
recognon
menoned
nduce
consdered
nlammaon
drec
Eac
group
acs
preerenay
on
neurops,
are
syn eszed
ympocyes.
Mediators
endoeum.
cemoaracan
paern
ces,
as
and
e
s
e
ereore
(cemoaxs).
e
a
nlammaon,
our
o
o
drec
are
mmuny
consss
wose
dead
Varous
cronc
reguae
adeson
a
and
nlammaon
macropages,
o
ces,
cyoknes
as
producs
proens
oer
a
and
resdues.
eosnops,
eukocyes,
Plasma neurop
(C)
monocyes,
are
and
mos
(s ee
are
Tabe
by
o
ssues
mp or an
compement
acvaed
pro duc s
o er
o
pasma
and
proens
ac vaed
es e
a
a
e
me daors
are
se
o
nlamma-
des cr b ed
n
e
2.4).
system
mcrobes
consss
and
by
o
severa
anbodes
crcuang
or
pasma
proens
ecns
a
bound
o
mcrobes and oer angenc subsances. Compemen acvaon eads
o
sequena
e
oer
ces
mcrobes.
er
enzymac
deposon
4,
n
or
o
a
pagocyoss;
Compemen
e
modicaon
producs
conex
o
o
varousy
recru
acvaon
s
e
coa
proens,
eukocyes;
descrbed
ypersensvy
cumnang
(opsonze)
n
reacons.
and
mcrobes
yse
more
n
and
n-waed
dea
n
Cap-
22
CHAPTER
Table
2.5
Major
Inflammation
2
Cytokines
of
Acute
and
and
Repair
Chronic
Inflammation
Principal
Functions
and
Role
in
a
Cytokine
Principal
Cytokines
Tumor
in
Acute
necrosis
factor
Cell
Sources
Use
of
Therapeutic
Antagonists
Inflammation
Macrophages,
(TNF)
Inflammation
cells,
T
dendritic
Endothelial
cells
cells:
adhesion
reduced
activation
molecules,
→
expression
secretion
anticoagulant
of
of
Rheumatoid
chemokines,
properties
bowel
arthritis,
disease,
inflammatory
psoriasis
(inflammation,
coagulation)
Neutrophils:
activation
Hypothalamus:
Muscle,
Interleukin-1
(IL-1)
Macrophages,
cells,
lial
dendritic
fibroblasts,
cells,
Endothelial
endothe-
keratinocytes
Macrophages,
cells,
T
dendritic
B
(many)
Virtually
all
cell
types
Th17
cells:
(inflammation,
Rheumatoid
TNF
matory
of
Th17
acute-phase
of
in
Chronic
(IL-2)
T
of
protein
Rheumatoid
antibody-producing
cells
arthritis
(juvenile
and
adult)
from
the
circulation
into
Inflammatory
(in
of
lymphoid
of
T
and
tissue
B
cells
clinical
bowel
disease
trials)
architecture
in
secondary
organs)
Inflammation
cells
T
genetic
proteins
acute-phase
leukocytes
(segregation
Interleukin-2
(rare
differentiation
of
Maintenance
Cytokines
autoinflam-
diseases)
tissues
lymphoid
arthritis,
syndromes
differentiation
proliferation
Recruitment
to
fever
synthesis
cells:
(cachexia)
activation
similar
synthesis
cells:
Liver:
cells
T
Chemokines
cells:
Hypothalamus:
T
(IL-6)
fever
catabolism
coagulation),
Liver:
Interleukin-6
fat:
(mainly
CD4+
helper
T
cells:
cells)
and
proliferation
memory
and
cells;
development,
differentiation
promotes
survival,
and
into
regulatory
effector
Anti-IL-2
T-cell
acute
receptor
organ
used
to
transplant
prevent
rejection
function
+
Interleukin-4
(IL-4)
CD4
T
cells
(Th2),
mast
B
cells
T
cells:
cells:
isotype
Th2
in
to
differentiation,
Macrophages:
Role
switching
alternative
allergic
IgE
Asthma,
atopic
dermatitis
proliferation
activation
inflammation
+
Interleukin-5
(IL-5)
CD4
T
cells
(Th2)
Eosinophils:
Role
Interleukin-12
Macrophages,
dendritic
cells
(IL-12)
T
in
cells:
NK
activation,
allergic
Th1
cells
increased
generation
Asthma
inflammation
differentiation
and
T
cells:
IFN-γ
synthesis
+
Interleukin-17
CD4
T
cells
(Th17)
Epithelial
cells,
increased
GM-CSF
macrophages,
chemokine
and
activation
of
G-CSF
and
and
other
cytokine
production
→
cell
types:
Psoriasis;
production;
recruitment
some
effect
in
multiple
sclerosis
and
neutrophils
+
Interferon-γ
(IFN-γ)
T
cells
NK
(Th1,
CD8
T
cells),
Macrophages:
cells
microbicidal
T
Interleukin-10
Macrophages,
(IL-10)
(mainly
Transforming
growth
T
factor-β
cells,
cell
T
cells
regulatory
cells:
Th1
cells)
Role
macrophages,
other
T
in
cells:
types
inhibition
(increased
Hemophagocytic
syndromes
cells:
inhibition
inflammation
proliferation
inhibition
angiogenic
Fibroblasts:
of
of
differentiation
Macrophages:
of
dendritic
termination
functions;
(TGF-β)
activation
differentiation
Macrophages,
T
classical
functions)
of
of
and
Th17
effector
and
activation;
Treg
stimulation
factors
increased
collagen
synthesis
a
Specific
for
the
Pentraxns
(CRP)
and
popds
cytokine
are
serum
or
its
pasma
amyod
expressed
on
receptor.
proens
proen
bacera
a
(see
ncude
beow).
membranes
C-reacve
ey
(and
proen
recognze
apopoc
pos-
ces)
crcuang
pan
and
1s
e
caor
emnaon
nes
proens
o
ese
ncrease
nlammaor y
mcrobes
durng
reacons,
e
and
dead
ces.
acue-pase
dscussed
aer.
e
pasma
response
Knns
are
a
eves
o
accompa-
produced
rom
e
he
promoe pagocyoss or acvae e compemen sysem, us causng
ese
a
by
precursor
se
our
cenur y
o
major
AD
(warm),
e
acons
uncon,
was
proens
by
eaures
e
tumor
o
and
conrbue
o
vascuar
daon
and
nlammaon.
nlammaon
aer.
(nay
encycopeds
(sweng),
parcuar
added
o
Roman
and
medaors
door
(Tabe
descrbed
Cesus),
(pan),
2.6).
A
rubor
can
be
it
n
e
(redness),
expaned
sgn,
oss
o
CHAPTER
B ecause
a
Tabes
on
2.4
o
wdey
e
o
nb
er
and
2.5).
ndvdua
used
o
syness
o
are
s
as
),
as
aso
that
clinical
typically
e
drugs
An
nlammaor y
pyscan’s
bock
excepon
e
n
are
o
oug
medaors
(see
a
o
are
nb
(by
nbng
c yoknes.
corcoserod-nduced
apoposs,
varous
o
auommune
Features
reactions
associated
manifestations
dsorders
as
of
with
(Table
Acute
show
Inflammation
distinct
different
morphologic
inciting
patterns
conditions
and
Fig.
2.4
skin
blister
Serous
Speca
inflammation.
Low-power
view
of
a
cross
section
of
a
2.7)
collection
Morphology.
23
unc-
mupe
producon
reang
or
corcoserods
wc
acd–derved
as
producon
Repair
drugs
armamenarum
e
s
process,
and
magnances.
inammatory
are
n
e
nlammaon,
sensve
useu
ympoc yc
o
ese
we
Clinicopathologic
Acute
o
medaors.
2
an
we
Mos
roe
par
aracdonc
A
Lympoc yes
a
are
suppress
pospopase
efec
essena
medaors
Inflammation
2
morpoogc
paerns
are
oten
showing
of
pale
the
epidermis
pink-staining
or
separated
clear
from
serous
the
dermis
by
a
focal
effusion.
supermposed
on e genera eaures o acue nlammaon (vasodaon, eukocye Table
2.6
Role
of
Mediators
in
Cardinal
Features
of
recrumen, and edema), dependng on e severy o e reacon, s Acute
specic
ance
cause,
o
and
e
recognzng
parcuar
e
gross
ssue
and
and
se
nvoved.
mcroscopc
he
paerns
s
Inflammation
mpor-
a
ey
Feature
Mechanism
oten provde vauabe cues abou e underyng cause. Redness
•
In
serous
nammaton
(Fg.
2.4),
exuded
lud
s
ce
poor
and
(rubor)
Vasodilation
dins)
accumuaes
n
body
caves
suc
as
e
peura
or
(caused
by
histamine,
prostaglan-
percardum
and
stasis
congestion
in
of
blood
(erythema
parenchymal
in
the
skin,
organs)
(ormng an efuson) or under epea suc as e skn (ormng Warmth
bsers
or
vesces).
hs
reacon
s
ypca
o
md
njury
Swelling
erma
burns
o
skn),
necons
a
damage
e
(calor)
Increased
blood
Exudation
of
adjacen
(tumor)
fluid
(suc
as
peurs
accompanyng
pneumona)
or
resorbed
•
wen
Fbrnous
necons
e
(suc
as
nlammaon
nammaton,
ke
vra
percards).
he
lud
s
fibrin
subsdes.
serous
sible
nlammaon,
occurs
on
Pain
(dolor)
Action
cuar eaks are arge and ence, e exudae conans arge-moec-
paway
pasma
acors,
proens
wc
suc
become
as
ibrnogen
acvaed
and
and
nsoube
organ
(Fg.
ibrn
2.5),
co.
and
Fbrn
may
s
deposed
eer
be
removed
e
by
can
resouton)
cause
ibrnous
or,
sgnican
exudae
by
exensve,
be
uncona
scar
ssue
s
repaced
o
enzymac
by
mparmen.
Puruent
(suppuratve)
by
histamine,
deposits
for
in
fibrinogen
and
extravascular
induration
in
chronic
tissue
of
prostaglandins
and
kinins
o
dead
eadng
ssues
sensory
scar
2.7
Patterns
of
Acute
Inflammation
ssue
of
a
Repacemen
Inflammation
Morphology
Serous
Accumulation
Examples
of
Diseases
o
of
cell-poor
Pleuritis,
pericarditis,
caed organzaton.
nammaton
nlammaon
coecon
on
endings
e
s
caracerzed
exudate
mild
burns,
o
and
e
ormaon
neurops.
I
o
s
pus,
a
mos
skin
dis-
by (pemphigus)
qFibrinous
ueied
of
(respon-
inflammatory
eases
desrucve
prostaglan-
formation
yss
fluid
•
of
ibrnogen
surace
Type
(caed
organ
vascular
coaguaon
conver
on
(caused
leakage
nerve
Table o
affected
increased
reactions)
e
surace o organs suc as e ung or ear, bu n s case e vas-
uar-weg
the
to
reavey dins);
nondesrucve
in
due
spermeability
sue
flow
(e.g.,
Deposition
of
fibrin
Pericarditis,
meningitis,
oten pleuritis
caused
by
necons
by
pyogenc
(pus-producng)
bacera
a
Suppurative
ec
a
neurop
Necrosis
(purulent)
•
An
abscess
s
a
with
ocazed
coecon
o
puruen
tion
of
leukocytes
2.6)
w
cenra
necross
and
acue
and
Bacterial
nias,
pneumo-
appendicitis,
nlammaon formation
(Fg.
accumula-
exudae.
nlammaon
of
pus
(con-
abscesses
oten taining
dead
leukocytes
surrounded by nlammaory ces and scar ssue ( s cronc). and
tissue
cells)
Abscesses may orm n any organ as a resu o seedng by bacera Ulcer
or
odgng
o
sepc
embo.
Because
ey
are
poory
Epithelial
defect
underlying
ey
•
may
ave
o
be
draned
surgcay
or
eang
o
e
as
a
somac
necon
resu
or
and
o
necross
duodenum
exacerbaed
and
(oten
by
oss
o
caused
gasrc
e
by
acd),
epeum,
Hecobacter
or
n
e
as
sores
seen
n
n
dabecs
edery
pressure).
Mos
because
ndvduas
ucers
o
reduced
because
sow
eaures
o
o
bood
acue
and
ulcer,
dia-
betic
ulcer,
venous
chronic
and
arterial
inflammation
(typically
in
ulcers
lower
extremities)
pyor
or
as
mmoby
cronc
Manifestations
bed
and
nlam-
maon. Heang o ucers requres reamen o e underyng con-
don.
Gastric
exremes
suppy,
proonged
and
n
Systemic (oten
acute
occur.
An ucer (Fg. 2.7) s a ocazed deec n e surace o a ssue,
usuay
with
vascuarzed,
Acute
inammation
festations
diagnostic
that
may
clues
is
(Table
Inlammaon,
cyokne-nduced
usually
cause
even
accompanied
clinical
problems
by
and
systemic
provide
mani
valuable
2.8)
sysemc
s
ocazed,
reacons
a
may
are
be
assocaed
coecvey
w
caed
e
24
CHAPTER
Inflammation
2
and
Repair
F
P
B
A
Fig.
2.5
overlies
Fibrinous
the
pericarditis.
pericardial
surface
(A)
Deposits
of
fibrin
on
the
pericardium.
(B)
A
pink
the
lung
meshwork
of
fibrin
(F)
(P)
A
B
Fig.
2.6
monia.
Purulent
(B)
The
surrounded
intensely
by
inflammation.
abscess
congested
congested
(A)
contains
blood
alveolar
Multiple
bacterial
neutrophils
vessels.
walls
and
and
Alveolar
abscesses
cellular
destruction
intra-alveolar
(arrows)
debris
is
in
resulting
seen
in
the
from
lower
in
a
case
destruction
right
corner.
of
of
bronchopneu-
alveoli,
Above
left
and
is
shows
exudate.
A
B
Fig.
2.7
The
Low-power
in
the
base.
morphology
of
cross-sectional
an
ulcer.
view
of
a
(A)
A
chronic
duodenal
duodenal
ulcer
crater
ulcer
with
seen
an
as
acute
a
defect
and
in
the
chronic
mucosa
(arrow).
inflammatory
(B)
exudate
CHAPTER
Table
2.8
Systemic
Manifestations
of
Cytokines
the
Clinical
(IL-1,
TNF)
stimulate
hypothalamus,
Initially,
TNF
act
on
prostaglandin
body
production
temperature
control
in
In
severe
center
cause
stimulates
release
of
leukocytes
from
the
bone
Marker
marrow.
Later,
by
colony-stimulating
stem
cells
in
neutrophils
Increased
of
plasma
acute-phase
levels
Increased
proteins
factors
macrophages
bone
and
liver
(GM-CSF ,
and
marrow
T
and
cells
G-CSF)
act
stimulate
on
cases,
mental
with
for
clinical
activated
inated
intravascular
coagulation,
alized
of
increased
can
coma
not
by
itself
a
cause
of
production
of
monocytes
synthesis
in
response
to
cytokines
(IL-6,
IL-1,
C-reactive
TNF
and
other
procoagulant
cytokines
activity
of
→
vasodilation,
protein:
endothelium
amyloid
tions
tion
marker
increases
chronic
and
inflammation
may
lead
causes
acute
sedimentation
to
rate
amyloidosis
in
inflammation
complication
other
(burns,
of
erythrocyte
protein:
Life-threatening
gener-
edema,
temperature
and
problems
Fibrinogen:
levels
body
NSAIDs
inflammation;
prolonged,
High
increased
disturbances
produced
TNF)
dissem-
25
hemopoietic
Serum
Hypotension,
Repair
Features
Treated
Leukocytosis
and
Inflammation
Mechanism
Fever
Inflammation
2
of
of
disseminated
severe
acute
infec-
inflamma-
pancreatitis)
organ
failure
G-CSF,
TNF,
Granulocyte
tumor
acue-pase
ncreased
Fever
pon.
or y
s
a
s
(caed
c yoknes
ncrease
acd
suc
presen.
as
IL-1
rese
e
2
,
s
nbng
assocaed
maor y
muaons
mcrobes
n
oten
Cyoknes
o
ours)
margna
e
an
nduced
o
aned
eukoc yoss
n
bone
e
es
and
e
ser ve
o
o
ncrease
ous
o
orgn
promnen
can
reac
Pasma
aed
by
un
e
ces
are
e
a
reease
a
aracdonc
prosagandns,
Nonseroda
asprn,
reduce
producon
resu
o
o
pyrogens)
eve.
aso
amy
s
neuroransmers
ger
caed
o
ever
o
IL-1
reease
days
a
We
n
o
o
gan-o-uncon
o
by
durng
ces
bood
ce
a
acng
sense
In
s
n
a
rom
more
hese
avaabe
are
o
wdey
o
wc,
n
ces
acv-
and
may
as
and
IL-1,
interleukin
1;
NSAID,
nonsteroidal
antiinflammatory
drug;
o
n
o
cyoknes
opsonns
causes
IL-6)
protens
o
rse
ncrease
wen
er
e
ver
syness.
s
o
and
ix
orm
proen
and
(CRP),
SAA
bnd
compemen.
sacks
rae
producon
serum
o
amyod
mcroba
Fbrnogen
(roueaux)
a
ce
bnds
sedmen
A
(SAA)
was
o
red
more
and
ces
rapdy
wose
(ESR)
as
an
s
ndcaor
ncreased
n
o
nlammaon.
e
acue-pase
Anoer
response
s
e ron-reguang pepde epcdn. Croncay eevaed pasma con-
cenraons
e
o
epcdn
be
or
9).
Acue-pase
maon,
n
anema
bu
saes
o
Severe
response
proens
proonged
(see
cassc
cnca
nravascuar
eadng
on
cyoknes,
o
Caper
by
ese
coaguaon,
bances
o
organ
ron
efecs
n
and
are
durng
proens
some
respons-
(see
Caper
acue
nlam-
(especay
cases,
cause
SAA)
secondar y
4).
(see
n
o
nlammaon
ese
can,
3),
s
and
condons
generazed
s
n
e
suc
caused
as
caused
and
by
by
suc
as
severe
he
dssemnaed
meaboc
e
ds-
nammatory
pancreas.
ypoenson,
edema,
a
sepss,
systemc
condons
reacons
dysuncon,
prncpay
seen
n
nonnecous
nlammaor y
rad
o
nlammaon
caused
and
cronc
producon
acue
syndrome,
rauma,
avaaby
beneica
nlammaon
necons
burns,
e
w
ave
Caper
sysemc
semnaed
reduce
assocaed
cronc
amyodoss
Outcomes
Mos
•
acue
R esouton.
and
e
cases,
ree
•
he
massve
dsur-
produc-
TNF .
o
Inflammation
be
n
acve,
ence
e
perssen
to
and
ends
are
e
o
descrbed
chronc
canno
are
srucure
n
B ecause
s
oucomes.
ved
more
and
are
no
mnma
s
may
In
naed
o
need
e
smua-
onger
ssue
ces
presen
desruc-
reaned.
dea
emnaed.
a
mos
nlammaon
nammaton
be
ree
smu
agens
ere
acue
o
e
sor
ofendng
ssue
ypes
one
emnaed.
Typcay,
norma
Some
ave
because
nlammaon
once
(scarrng),
Progresson
ces)
subsdes.
Organzaton.
responses
response
necroc
reacon
on,
•
Acute
moecues
on
mos
smu-
of
nlammaor y
(mcrobes,
e
so-caed
he
em
CRP
pepde
ibross
acute-pase
(many
C-reacve
sedmenaon
nec-
e
ac
are
ibrnogen.
an ndvdua red ces. hs s e bass or measurng e er yrocye
emnae
severe
(e
e
proens
proen,
reacon).
eves
factor;
sus-
reacon
used
be
nlammaon,
eukemas
s
mnues
progenor
presumed
acue
ose
on
a
eukoc yes.
(n
nlammaor y
are
couns
ces
eukoc yes
produce
producon.
neurops,
approxmang
acvaed
aso
e
a
wc
oer wse.
bood
may
weeks)
bood
eukoc yoss
preormed
and
eukoc ye
de
by
o
man
auonlam-
proens
we
produced
marrow,
numbers
s
e
o
popoysacca-
conver
Excessve
appearance
ncrease
proved
ncrease
a
crcuang
nlammaon,
numbers
eukemod
o
agen.
dagnose
rapd
(over
e
n
c yoknes
bone
repace
ofendng
cnc
by
marrow
a
ncudng
recepor
as
bu
nlamma-
eukoc yes
endogenous
syndromes,
wc
ncrease
e
e
a
syness.
ever
o
suc
producon
pon
uncear,
se
ces.
enancng
poo
colony-stimulating
and
emperaure
underyng
ypoaamus,
e
se
Nod-ke
s
(caed
e
an
smuae
(NSAIDs),
some
smuae
by
In
eukocyoss,
body
remans
(c ycooxygenases)
perodc
necroc
Leukocy toss
mos
TNF
ever,
e
producs,
prosagandn
and
ever
pyrogens),
drugs
syndromes,
o
aers
Bacera
emperaure
w
a
by
weer
smuae
an-nlammaor y
by
granulocyte-macrophage
proens.
assessng
and
enzymes
PGE
GM-CSF,
manesed
uncon
n
prosagandns.
especay
a
sgn
are
acue-pase
response
exogenous
e
no
o
pysoogc
process
rde
and
eves
c yokne
cnca
factor;
factor.
response
pasma
e
vauabe
colony-stimulating
necrosis
are
repaced
by
aer.
occur
mos
e
smuus
nsances,
s
owever,
26
CHAPTER
Inflammation
2
and
Repair
Antigen+
CD4 presenting Th1
cell
cell
Presents
antigen
IL-17,
T
TNF
to
Granuloma
cells
Epithelioid
Giant
Cytokines
IFN-
Leukocyte
cell
cell
γ (e.g.,
IL-12,
IL-6,
IL-23)
Monocyte
Activated
recruitment,
macrophage
inflammation
Fibroblast
Activated
Blood
Fig.
2.8
that
recruit
Macrophage–lymphocyte
activate
ing
of
Lymphocyte
vessel
macrophages
macrophages
antigens
and
via
(tumor
(interferon
cytokines
interactions
necrosis
gamma
such
as
in
factor
[IFN-γ]).
IL-12.
chronic
[TNF],
inflammation.
interleukin
Activated
Prolonged
17
macrophages
activation
of
Te
oow
pro ducng
acue
in
T
cells
produce
chemokines)
turn
stimulate
macrophages
may
T
and
cells
lead
to
cytokines
others
by
the
that
present-
formation
granulomas.
cronc nlammaon s a dsnc reacon a does no necessary
an
Activated
[IL-17],
macrophage
pase.
macropages
NO,
r y
o
d es roy
ys os oma
or
en zy mes,
wa
and
o
e
o end ng
c yok nes
a
agen
by
re c r u
more
angens,
env-
eu ko c yes.
T
CHRONIC
ympocyes
ronmena
Chronic
in
inammation
which
a
be
coesero
adapve
ces,
oer
o
mmuny,
and
many
e
especay
nlammaon
and
e
seng
ere
acvaon
perssen
summarzed
usually
s
or
a
o
coexist.
nec-
reumaod
o
oxc
agens
endogenous
srong
(e.g.,
componen
o
c yokne-producng
T
promnen
he
n
stimuli
perssen
(e.g.,
exposure
and
macropages.
are
persistent
o
dseases
parces)
cases,
to
scarring
proonged
sca
especay
o
n
reaction
auommune
(e.g.,
In
conrbue
eukoc yes,
cronc
injury,
deveops
sceross),
exogenous
cr ysas).
wc
prolonged
tissue
ubercuoss),
mupe
may
a
nlammaon
(e.g.,
arrs,
is
inammation,
Cronc
ons
mos
Tabe
acvaon
requen
o
ens),
rom
a
Reactions
of
inammatory
Chronic
reactions
e
ces
T
proen
oer
ces.
ese
Subses
o
o
auommune
angens
o
acvaed
T
and
dseases).
T
ces
ces
and
mody
se
pro-
Macropages
respond
produce
many
o
and
sgnas
cyoknes
nlammaon:
IL-5 acvaes eosnops.
IL-17 smuaes e producon o cemoknes a recru neuro-
•
TNF acvaes endoea ces and promoes recrumen o euko-
ps.
causes
cyes
2.1
(as
Oer
ere
n
ces
are
acue
n
nlammaon).
cronc
nlammaor y
supermposed
epsodes
o
reacons
acue
ncude
pasma
nlammaon,
ces.
neurops
Inflammation
are
reacons
neracons
mmune
Macropages
ac vae d
dspay
(n
o
•
dominated
by
inltration
may
be
promnen.
of
deveop
as
a
consequence
o
inammation
beween
macropages,
T
by
are
e
ces
(Fg.
cen ra
c yok nes
at
the
same
is
accompanied
by
tissue
injury
and
repair
time.
pro-
Tssue
are
angens
bnd
cells.
nlammaor y
bdrecona
and
mcroba
IFN-γ acvaes macropages.
njur y
s
caused
by
e
numerous
medaors
a
macro-
ympo-
pages cyes,
by
somemes
•
occurring
onged
se
conrbue
Chronic mononuclear
Cronc
acvaed
(wc
•
aso
Chronic
cemcas
and
dendrc
I
Cellular
are
INFLAMMATION
produce
n
e
aemp
o
emnae
e
ofendng
agen.
Wen
2.8).
ce s
o
pro duce d
cron c
by
T
n am ma on .
ce s,
mos y
e
response
age
o
s
srong
and
proonged,
ere
s
oten
consderabe
dam-
Te y
IFN-γ,
oer wse
eay
ssues
a
e
se
o
nlammaon.
and
Repar o njured ssues oten accompanes cronc nlammaon. o er
sg na s
prov d e d
by
T
ce s.
Pers sen
n nae
m mune
s m-
Proeraon u a on
by
To - ke
re cepors
and
o er
re c epors
may
a s o
Tes e
macropages
ave
b e en
c a e d
c ass c a y
grow
macropages
(n
con ras
o
a er na vey
ac vae d
w c
are
nvove d
n
ssu e
rep ar,
and
vesses
(angogeness)
c yoknes,
noaby
and
ibross
vascuar
are
nduced
endoea
d s c uss e d
(VEGF)
and
TGF-β,
produced
by
e
acvaed
grow
macropages.
[M2]
hs macropages,
bood
acors
ac vae d
acor (M1)
o
con-
by r bue.
aer) .
process
s
dscussed
aer
n
e
conex
o
ssue
repar.
CHAPTER
Inflammation
2
and
Repair
27
*
A
B
Fig.
2.9
logic
are
Chronic
features:
replaced
(fibrosis,
tiple
Clinicopathologic
inflammation.
(1)
by
collection
spaces
arrows).
(B)
Langhans-type
Features
of
lined
inflammation
inflammatory
cuboidal
epithelium,
tuberculous
cells,
Chronic
Chronic
chronic
by
Typical
giant
(A)
of
granuloma
epithelioid
cells,
and
in
cells
the
(*),
lung,
(2)
arrowheads),
showing
an
inammation
underlies
many
o
e
mos
vexng
dseases
o
umans,
suc
as
aeroscleroc
renal
caused
a
dsease,
coronar y
leas
advances
n
n
and
varous
arer y
dsease,
par
by
auommune
lver
cronc
mmunoerapy
or
and
crross,
allergc
nlammaon.
In
w
weg
cnca
caenges
some
and
o
major
ese
causes
Despe
dseases,
o
hese
dsorders
are
dscussed
n
capers
connective
surrounded
tissue
by
mul-
severe
appee
and
and
proonged
ncrease
cases,
e
g
eves
caabosm
o
o
TNF
pds,
may
resung
oss
e
(caed
s
aso
cacexa
assocaed
wen
w
severe).
Inrequeny,
deposon
o
amyod
cronc
proen
because
e
precursor
serum
amyod
proen
s
an
n
acue-pase
proen
wose
cases
cronc
producon
ncreases
durng
nlammaon.
In
some
mpressve
ey
morbdy
on
histo-
alveoli
are
o
nlammaon,
suc
as
cronc
vra
epas,
obvous
reman
and
dferen
sgns
are
absen,
and
e
dagnoss
requres
aboraor y
assess-
mormen
ay.
by
necrosis
(normal
end-
dseases,
pysca mporan
replacement
central
characteristic
pumonar y
ssues, sage
three
parenchyma
diseases.
nlammaon ibross,
all
of
lymphocytes.
n Some
(3)
of
ubercuoss.
Inflammation
important
and
area
nerere Chronic
showing
destruction
and
ssue
bopsy.
organ
sysems.
TISSUE
Morphology.
Mos
cronc
nlammaor y
dseases
sow
After cear
ce
(ympoc ye
and
macropage)
niraon
REPAIR
mononu-
w
the
offending
damaged and
ssue
njur y
(Fg.
2.9A).
Under
some
crcumsances,
agent
is
eliminated
and
inammation
subsides,
ibross
suc
tissue
is
repaired
by
two
processes,
regeneration
and
as scarring.
necon
w
uberce
bac,
e
reacon
may
deveop
a
parcuhe
erms
repar,
eang,
and
resouton
are
oten
used
ner-
ar morpoog y reerred o as granuomaous nlammaon. Grancangeaby, uomas
are
crcumscrbed
coecons
o
acvaed
abundan
ave
a
c yopasm,
caed
epteod
ces
because
epeum-ke
sape
Acvaed
may
use
o
orm
munuceae
gant
ces
(Fg.
2.9B).
ormaon
s
a
cassc
exampe
o
a
speca
n
wc
macropages
are
ype
srongy
o
T
mas
ces
are
ence
or
by
seen
as
recognon
n
ony
mporan
a
ew
o
perssen
condons,
erapeuc
oregn
and
acvaed
bodes.
recognzng
mpcaons.
endemc,
may
Fg.
In
be
e
e
mos
wesern
requen
word,
Were
cause
o
granuomas
o
resoraon
o
norma
ssue
arcecure
and
w-
Under
by
dferen
regeneraon
or
condons
scarrng
o
ssue
(descrbed
njur y,
beow
e
and
repar
sown
2.10).
a
B o
are
processes
produced
are
many
rggered
by
by
c yoknes
macropages.
In
and
some
grow
suaons,
macropages
a
nae
repar
beong
o
e
aernavey
ac-
Granuo-
er
vaed
(M2)
knes
(o
subse,
wc
produces
varous
annlammaor y
c yo-
presermnae
nlammaon)
and
grow
acors
(o
promoe
ubercuoss One
secreed
c yokne
a
can
bo
suppress
nlammaon
granuomaous and
nlammaon.
wounds
eer
repar). s
skn
cronc
e by
reers
scarrng.
many
acors nlammaon
o
Grann
uoma
reers
macropages s
aso
generay
ey ou
laened,
eang
macropages resouon
w
aoug
are
more
smuae
ibross
(scarrng)
s
TGF-β
oten Regeneraon s e proeraon o resdua ces o resore e dam-
seen
n
Cron
dsease,
a
ype
o
nlammaor y
bowe
dsease,
n aged
sarcodoss,
a
rare
bu
proean
dsease
o
unknown
eoog y,
or n
some
unga
dseases
suc
as
ssue.
conans
e
scafod
seen
he
n
Manifestations
sysemc
cay
ess
ac,
reacons
severe
an
recurren
o
cronc
ose
ever
and
o
nlammaon
acue
ng
occurs
sem
wen
ces
e
a
njured
can
ssue
dferenae
s
capabe
no
o
proeraon
uncona
ces,
and
sopasmoss. wen
Systemic
I
and
are
nlammaon.
sweas
are
a
smar
Fever
cassc
o
s
bu
yp-
common;
manesaon
o
n
connecve
or
e
epea
o
e
capacy
proeraon
s
o
oer
ces.
proeraon
sroma
arcecura
proerave
and
ssue
skn,
and
smuaed
By
by
and
suceny
resoraon.
nesnes,
conan
conras,
s
regeneraon.
Regeneraon
and
ver,
abundan
grow
cardac
nac
acors
musce
s
wc
ssue
sem
secreed
and
o
by
neurons
provde
mos
ave
a
ces.
a
oten
g
her
macropages
are
ncapabe
28
CHAPTER
Inflammation
2
and
Repair
Platelet
Eschar
Fibroblast
Epithelial
cells
Granulation
Macrophage
Collagen
scar
tissue Neutrophil New
blood
vessels
Capillary
A
B
Fig.
2.10
Tissue
resolution
by
scar
(A)
occurs
Fbrous
scar
srucura
acks
e
ura
Inflammation
as
uncons
e
ropages,
called
a
o
njur y
ibroblass
o
e
s
a
cesses
ssue
ad
ibers
o
n
by
a
and
e
hs
by
and
se
o
newly
o
e
ssue
skn)
organ
are
e
n
s
o
nuron
ssue
e
o
caed
a
arge
by
e
e
during
by
not
the
underlying
connective
wound
vessel
tissue,
healing
growth
and
in
tissue,
repair
the
is
skin.
proliferating
nduced
Separaton
e
o
by
vascuar
percytes
basemen
endoea
rom
membrane
e
o
grow
abumna
aow
acor
surace
ormaon
o
(VEGF)
and
a
breakdown
vesse
sprou
Mgraton o endothea ces oward e area o ssue njur y
•
Proeraton o endothea ces jus bend e eadng ron (p) o
•
Remodeng no capar y ubes
•
R ecr utment
mgrang
ar es
and
maure
•
ces
per e ndothea
mus ce
ce s
ce s
(p er c yes
or
arger
or
sma
vess es )
o
c ap -
or m
e
vess e
Suppresson
men
o
smo o
o
endothea
proeraton
and
deposon
o
e
base-
membrane
Grad-
wc
roug
cross-nkng
Clinicopathologic
The
eads
depos-
bu
amouns
wen
pro-
same.
extent
Wen
on,
pes
s
of
e
gu.
No
Heang
son
o
ay
of
e
njur y
s
by
md,
ce
scar
by
ssue
irst
by
macropages
of
tissue
Tissue
varies
s
e
Repair
according
to
the
nature
e
and
ver
n
so
a
ssue
e
and
capabe
edges
e
are
o
proera-
cosed.
epeum
o
Exam-
e
skn
ormed.
cosed
bood
and
o
ntenton occurs
a
a
s
acue,
regeneraon,
regeneraon
skn
seaed
Features
repaired
injury.
repared
ncude
and
(ver,
underyng
appearance
and
resapng
scar,
the
•
o
marx,
C oagen
to
but
Vasodaton n response o nrc oxde (NO) and ncreased perme-
o
mac-
Remodeng
coagen.
tissue
aby
•
syn-
days
scar,
subsequen
•
depends
marx
e
leads
capllares,
orm
nvoves
e
5
nlammaon.
o
n
damage
specifically
granulation
acors
collagen
o
of
epithelium
with
shown,
scar
produced
3
are
injury
the
scar.
sruc-
macropages,
nal
or
a
ibroblass
undamena
essenay
fibrous
exracellular
abnormay
he
are
ormed
usuay
Formation
the
damages
severe
formation
Grow
provde
and
(B)
more
adequae
exraceuar
process
scar
and
meaoproeases.
ibross.
reacons
on
by
loose
after
which
regenerae
granuaon
we-compaced
(mb,
as
a
nensy
e
marx
ac
injury,
Aoug
(FGF)
ibrobass
n
o
uncon.
and
n
by
provdes
Durng
w
enzymes
parencyma
ese
vessels
srengen
srong
reerred
a
by
but
produce
unabe
produced
amoun
deec
to
proleraon
embedded
e
down
resorpon
n
s
also
mild
formation.
acor
cells,
er
illed
repair
damaged.
ssue
below).
remodeng.
perpera
occurs
ung),
tssue.
modied
caed
para
n
s
s
s
ssue,
grow
blood
in
clot
ssue
oer
(see
and
srucuray
ed
new
and
some
VEGF ,
o
coagen
and
me
process
o
o
Steps
Remodeling
eay
and
area
sze
e
C
Following
regeneration,
rreversby
smulae
ibroblass
coagen
(C)
ibroblas
o
granuaton
e
over
and
ormaon
repar,
uay,
e
C oncomanly,
e
s
manan
ssue
prolerang
on
o
macropages
connecve
o
o
TGF-β
acvaed
ess.
ormed
ramework
negry
suc
s
by
formation.
fibroblasts.
e
repair.
co,
w
n
oowed
ormaon
o
a
cean,
surgca
a
by
e
sma
unneced
suures.
arrva
amoun
he
o
surgca
nc-
s
n-
neurops
and
o
wound
granuaon
s-
Angiogenesis sue a s repaced by a n scar. Concomany, e surace epea
Ang ogeness
exs ng
a s o
n
and
n
o
e
(Fg .
e
I
s
pro cess
no
de veopmen
a ow ng
er
ne w
s
vess es.
or g na
vess es
2.11):
o
umors
bo o d
rom
o
on y
ne w
co aera
o
ncre as e
suppy.
exs ng
bo o d
cr c a
ones
n
vess e
e a ng
crc u a ons
n
sz e
ses
a
conss s
e
nvoves
o
o
ses
b e yond
Ang ogenes s
and
d e veopmen
a
e
rom
njur y
o
s cem a
c ons ra n s
sprou ng
o ow ng
ces
bu
o
seps
regenerae
Heang
res
o
evens
e
s
on
a
sss
or
e
a
by
and
skn,
amoun
onger
ibrous
o
scar
e
e
o
perod,
s
e
ncsona
ntenton
wen
denca
e
brdge
second
occurs
edges
one
canno
descrbed
granuaon
and,
cker.
gap.
n
ence,
By
abou
more
be
ssue
o
s
6
weeks,
deep
e
arger
s
ad
e
nju-
sequence
w
muc
coagen
and
he
prevousy,
more
4
severe
cosed.
and
down
skn
o
excep-
per-
and
wound
CHAPTER
Quiescent
Vasodilation
vessel
(VEGF)
Leading
(“tip”)
Inflammation
2
and
Repair
29
cell
(VEGF) Angiogenic
factors
Pericyte
Pericyte
detachment
(angiopoietin)
Basement
membrane Basement
Endothelium
membrane
degradation
(MMPs)
Pericyte
A recruitment
ECM
Elongation
of
Formation
vascular
of
new
stalk
vessel
B
Fig.
2.12
vessels,
Tissue
inflammatory Fig.
2.11
Angiogenesis.
In
tissue
r e p a i r,
angiogenesis
occurs
the
sprouting
of
new
vessels.
The
steps
in
the
process,
and
signals
involved,
are
illustrated.
The
newly
formed
cells.
a
(A)
Granulation
loose
tissue
extracellular
Collagen
is
stained
showing
matrix
blue
numerous
containing
by
the
blood
occasional
mature
collagen
can
be
seen
at
this
point.
trichrome
(B)
Trichrome
stain;
stain
the
of major
and
mainly minimal
by
repair.
edema,
mature
scar,
showing
dense
collagen,
with
only
scattered
vascular
vessel
channels. joins
up
bed.
ECM,
VEGF,
with
vascular
conracs
ssue,
other
vessels
extracellular
endothelial
because
srnkng
o
e
(not
matrix;
e
growth
acon
area
shown)
MMP,
o
o
njur y
to
form
matrix
the
new
vascular
metalloproteinases;
f a c t o r.
myoibroblass
(Fg.
n
e
connecve
cyokne
2.12).
ea
• Repair
can
be
impaired
by
numerous
producon
normay
and
Compromsed
by
macropages.
conan
bood
exensve
suppy,
wc
Dabec
skn
granuaon
can
cause
ucers
do
no
ssue.
ucers
n
e
ower
factors. exremes.
ese
ncude: In
•
ons
•
Infecton,
wc
proongs
e
nlammaon
and
causes
ssue
n
wc
o
ese
e
suaons
repar
process
o
deecve
becomes
repar,
excessve.
ere
hs
are
can
cond-
gve
rse
progressve o
yperropc
scars
oowng
njur y,
wc
usuay
regress
sowy,
njur y and
•
conras
Mecanca factors suc as excessve movemen or pressure
Dabetes,
a
underyng
dsease
n
meaboc
wc
eang
abnormay
and
s
rearded
vascuar
because
narrowng,
o
scar
ssue
a
grows
beyond
e
margns
o
e
njur y
and
as
e o
regress,
n
organs
caed
keod
(Suppemena
eFg.
2.1).
Excessve
scarrng
eadng resus
n
uncona
compromse
and
s
e
bass
o
serous
o a reduced bood suppy. Furermore, dabecs are suscepbe o dsorders necons
because
o
decreased
neurop
uncon
and
suc
as
pumonar y
mpared e
ver
(Caper
13).
ibross
(Caper
10)
and
crross
o
CHAPTER
Supplemental
eFig.
scar
Keloid.
a
Atlas
Dermatopathology.
of
raised
2.1
forming
known
as
Excess
keloid.
collagen
(From
Philadelphia,
WB
deposition
Murphy
GF ,
Saunders,
in
the
Herzberg
1996,
p
skin
AJ:
219.)
2
Inflammation
and
Repair
29.e1
3
Hemodynamic
Disorders,
Thromboembolism,
and
Shock
O U T L I N E
Hyperemia,
Edema,
Congestion,
and
Edema,
30
Embolism,
30
Hemostasis and Hemorrhage, 31
Platelets,
Coagulation
Control,
ea
devers
aboc
mens
and
34
Shock,
depends
nurens
producs.
made
Infarction,
n
e
Bood
marrow
on
adequae
and
removes
as
wo
(we
bood
major
ces,
crcuaon,
carbon
doxde
consuens:
red
ces,
and
wc
and
lud
pase
(pasma),
conssng
o
waer,
ceuar
paees)
norganc
sas,
and
Imporan
numerous
pasma
proens,
proens
mos
ncude
o
wc
abumn,
are
e
In
nor ma
o
waer
n
pasma;
mmunogobuns
and
componens
o
sysem
(dscussed
n
Caper
4);
and
coaguaon
and
n ravas c u ar
by
no
o er
junc ons
sma
n
c ap ar es
mo e c u es ,
bu
are
no
p er me abe
o
yd ros a c
pressure
ends
o
pus
proens .
waer
e
ssues ,
bu
s
s
ne ary
b a anc e d
by
o s mo c
and
pressure,
e s
generae d
by
p as ma
proe ns
and
pu s
waer
b ack
no
e
abundan
e
(Fg .
3.1).
Te
sma
amoun
o
ud
a
do es
acc umu ae
n
compenor ma
men
end o e a
s a s
and
vess es proen
ssues,
and
organc
made
mos
39
ee-
w c ver.
Shock,
Edema
s a s meaboes,
37
37
me-
Hg a
Emboli,
37
37
38
Septic
ssues
oxygen
wase
33
35
o
Thromboembolism,
Thromboembolism,
Nonthrombotic
Cascade,
e
Systemic
32
Coagulation
Thrombosis,
36
Pulmonary
acors,
ssues
s
a ken
up
by
y mpa c
vess es
and
reur ne d
o
e
wc crc u a on
roug
e
orac c
duc .
upon acvaon caayze a seres o reacons a cause e bood o co. Edema
and
efusons
may
occur
w
ncreased
ydrosac
pres-
Dsorders a dsurb norma lud baances beween e bood and sure, ssues
or
a
compromse
e
negry
or
paency
o
bood
decreased
ver y
common,
and
may
cause
dysuncon
or
necross
o
In
s
caper,
we
w
rs
dscuss
dsorders
o
lud
e
accumuaon
o
excessve
lud
wn
ssues
or
and
e
oss
o
bood,
and
en
urn
o
dsorders
are
sed
or
excessve
cong,
ncudng
paoogc
n
roug
Common
Tabe
3.1.
severa
Noe
drec
a
or
some
ndrec
acors
cause
lud
accu-
efecs.
Inammaton (dscussed n Caper 2) promoes edema by ncreas-
o
bo
bood
nravascuar
low
and
vascuar
permeaby
o
proens.
he
pro-
nadeen-rc
quae
obsrucon.
body ng
caves
ympac
baance,
• ncudng
or
afeced muaons
ssues.
pressure,
vesses causes
are
osmoc
lud
o
nlammaon
s
reerred
o
as
an
exudate,
wereas
cong proen-poor
nonnlammaor y
edema
lud
s
reerred
o
as
a
tran-
(romboss) and e seddng o cos no e crcuaon (embosm), sudate. and
er
sock,
a
downsream
dsorder
sysemc
aure
w
o
consequences.
severa
ssue
We
dferen
w
causes
ns
a
by
ave
dscussng
n
common
•
Cardac aure, wc akes wo orms:
•
a
Rght-sded
cardac
e
sysemc
crcuaon,
mcrocrcuaon,
HYPEREMIA,
CONGESTION,
AND
lud
EDEMA
Swelling
of
tissues
may
stem
from
increased
blood
volume
due
•
n
or congestion,
or from
increased
uid
within
the
a
condition
s
called
dened
generay
due
o
o
e
ncreased
low
o
arera
bood
no
a
areroar
envronmena
skeea
musce,
or
congeson
daon.
caenges
cod
cardac
n
urn
causes
resung
aure
s
a
n
egress
pressure
o
subcuaneous
common
cause
n
n
e
proen-poor
edema.
o
peura
efuson
and
aso
dmnses
pumonar y
e
kdney,
wc
responds
by
ncreasng
bood
renn
sup-
produc-
Renn
I
s
a
norma
n
(e.g.,
exposed
ncreased
skn).
By
adapaon
workoad
conras,
n
acvaes
angoensn,
ereby
ncreasng
ar eroar
smusce
one
and
smuang
e
producon
o
ado-
o by
e
adrena
corex,
wc
promoes
reabsorpon
exercso
ng
venous
ydrosac
edema.
by
serone ceran
wc
nersum,
and
smoo sue,
passve
e
inter
on. Hyperema
causes
rasng
to
py stitium,
e
L et-sded
edema hyeperemia
aure
peruson.
congeson
sodum
and
waer
by
e
kdney.
he
reenon
o
sodum
s and
waer
ncreases
e
ydrosac
pressure,
oten
worsenng
an abnorma process caused by decreased venous oulow rom a ssue. edema Congesed
on
and
ssues
even
ave
necross.
poor
bood
Edema
dever y
reers
o
an
and
are
prone
abnorma
o
rougou
e
body.
dysunc-
accumuaon
o
Morphology.
Edema
s
easy
recognzed.
Tssues
(parcuary
e
lud n ssues. hroug smar mecansms as ose a cause edema
subcuaneous (descrbed
n
e
oowng),
abnorma
lud
accumuaons
suc
as
caed
ssue,
ungs,
and
bran)
are
swoen
and
eavy.
Sub-
efu-
cuaneous edema s accenuaed n dependen pars o e body (e.g., sons
may
aso
gaer
n
body
caves
e
peura,
percarda,
e and
30
peronea
spaces.
sacrum
n
recumben
paens
and
e
ee
oowng
proonged
CHAPTER
Hemodynamic
3
Disorders,
he sng
or
sandng).
Pumonar y
edema
s
marked
by
eavy
Thromboembolism,
erms
sed
descrbe
and
beeds
Shock
accordng
31
o
er
may
range
sze
and
ungs, appearance:
wc
reease
roy,
bood-nged
lud
wen
cu.
Bran
edema,
• generazed,
eads
o
e
narrowng
o
suc
because
o
Hematoma
bruses o
e
swoen
g yr
agans
e
sku.
Anasarca
(generazed
seen
n
panes
(e.g.,
cronc
rena
e
ear
aure
eyeds).
congeson
ear
as
aure,
aure.
somemes
Varous
we
By
as
congeson
e
preerenay
orms
edema.
conras,
o
In
ear
afecs
aure
paens
produces
edema
are
w
necross
o
a
e
aa
a
beed
nracerebra
no
ssues
and
emorrages
(Fg.
Petecae
are
pnpon,
1-
membranes,
or
serosa
o
2-mm
suraces
beeds
paens
nadequae
(see
Fg.
no
e
3.3),
skn,
usuay
ssues
assocaed
w
paee
uncon.
w
rg-sded
epac
obues Table
3.1
Causes
of
Edema
and
Effusions
(centrlobular necross). he gross appearance s known as numeg
ver
(Fg.
produces
3.2).
In
et-sded
bood-engorged
ear
aure,
capares,
pumonar y
nersa
congeson
edema,
and
Increased
alure
o
emosdern-aden
cells),
e
aer
nraaveoar
semmng
rom
macropages
sma
Hydrostatic
Venous
Congestive
Liver
wdey
Features.
he
dependng
cnca
on
er
efecs
sze
and
o
lud
heart
ocaon.
accumuaons
sgna
an
mporan
underyng
dsorder
Subcuaneous
(e.g.,
ear
and
ance
necons.
o
ay
aso
e
severe
exacerbang
ncreases
bran
e
canno
may
nerere
Pumonar y
underyng
rsk
o
expand
w
edema
wound
mpars
condons
necons.
wn
e
gas
suc
Bran
eang
obstruction
Venous
thrombosis
edema
encosed
ear
may
sku.
extremity
may
compromse
e
bood
suppy
o
e
or
(e.g.,
by
a
mass)
(e.g.,
with
renal
prolonged
failure,
dependency
left-sided
heart
failure)
cear-
Sodium
(poen-
aure)
aa
Increases
bran
inactivity
retention
and
Renal
snce
n
Retention
failure
Left-sided
heart
failure
CNS Arteriolar
pressure
compression
kdney
and
be
or
edema
or
excange
as
(ascites)
Venous
var y
Sodium
aure)
failure
pericarditis
cirrhosis
Lower
may
Return
(heart
beeds.
Constrictive
Clncal
Pressure
e
Impaired
presence
cause
Dilation
er-
Inflammation
naon
a
roug
conro
e
oramen
respraon
(see
magnum,
Caper
njurng
meduar y
ceners
17). Reduced
Osmotic
Protein-losing
HEMOSTASIS
AND
HEMORRHAGE
Liver
Pressure
glomerulopathies
(nephrotic
syndrome)
failure
Malnutrition
Hemorrhage
allowing
is
blood
caused
to
by
injuries
extravasate
into
that
tissues
disrupt
or
blood
outside
of
the
vessels,
body.
Protein-losing
he
ders
failure
negry
a
o
desroy
of
gastroenteropathy
It
Lymphatic represents
Obstruction
hemostasis.
bood
vesse
vesses
was
may
(e.g.,
be
dsruped
vascus,
by
eroson
rauma
by
or
Inflammatory
dsor-
cancers).
Neoplastic
Ds-
Postsurgical
orders
a
mpar
bood
cong
exacerbae
beedng
endences,
even
Postirradiation
n
e
absence
o
obvous
rauma.
LYMPHATICS
To
thoracic
duct
to
left
and
eventually
subclavian
vein
Obstruction
Increased Hydrostatic
interstitial
pressure fluid
pressure
Malnutrition
Liver
Heart
Renal
failure
failure
Nephrotic
failure
syndrome
Inflammation
Sepsis
Plasma
osmotic
Arterial
Fig.
are
3.1
lates
or
Factors
normally
is
cleared
heart
CAPILLARY
influencing
by
failure),
meability
end
balanced,
so
fiuid
there
lymphatic
osmotic
increases
(as
movement
is
little
drainage.
pressures
with
rom
skn
3.3).
fall
net
across
(as
in
or
may
pressure
Venous
capillary
of
result
or
walls.
fluid
into
when
malnutrition,
sepsis),
colloid
BED
movement
Edema
inflammation
mucous
accom-
oose
severe
o
edema)
• s
descrbes
compresson
liver
Capillary
the
lymphatic
hydrostatic
interstitium.
hydrostatic
failure,
end
or
vessels
pressures
nephrotic
are
and
What
osmotic
little
rise
(as
fluid
in
syndrome),
obstructed.
forces
accumu-
renal
failure
vascular
per-
seen
n
32
CHAPTER
Hemodynamic
3
Disorders,
Thromboembolism,
and
Shock
A
A
B
Fig.
(A)
3.2
In
Liver
this
compared
liver”
(so
with
autopsy
with
chronic
the
called
passive
specimen,
surrounding
because
it
congestion
central
tan
areas
viable
resembles
and
are
hemorrhagic
red
and
slightly
parenchyma,
the
cut
creating
surface
of
a
necrosis.
depressed
“nutmeg
nutmeg).
B
(B)
Fig. Microscopic
preparation
shows
centrilobular
hepatic
necrosis
with
3.3
(A)
Punctate
and
scattered
Hofstra/Northwell
•
School
of
cells.
Medicine,
(Courtesy
of
Hempstead,
Dr.
James
hemorrhages
thrombocytopenia.
(B)
Fatal
of
the
colonic
intracerebral
mucosa,
a
hemorrhage.
NY .)
are
3-
o
5-mm
unc on,
be e ds
rauma,
a
vas c u ar
may
sem
rom
n am ma on ,
d ee c s
or
n
vas c u ar
Platelets
rag y.
that
Eccymoses are 1-2 cm n sze and correspond o “bruses”; ey are
lant
usuay
of
Crawford,
Platelets
P ur pura
p aee
•
inflammatory
petechial
hemor-
consequence rhage
caused
by
Paee
rauma.
the
essential
life.
clotting
of
blood
following
blood
vessel
trauma,
fragments
primary
that
promotes
uncon
and
plug
secondary
depends
cyoskeeon,
derived
hemostatic
on
surace
cyopasmc
from
and
megakaryocytes
provide
a
procoagu-
hemostasis.
gycoproen
granues
a
recepors,
conan
a
a
con-
number
is o
for
anucleate
the
surface
race Hemostasis,
are
form
procoaguan
undergo
a
subsances.
seres
o
In
sereoypc
e
seng
o
vascuar
njur y,
paees
evens:
Under norma crcumsances, bood cong occurs a ses were e
• was
o
bood
vesses
ave
been
pyscay
dsruped.
he
na
seps
Adeson. Paee adeson s medaed argey by neracons w
n vWF ,
co
ormaon
are
wo
muuay
renorcng
processes
(Fg.
gen
•
Prmary
emostass
s
naed
by
e
exposure
o
and
von
Webrand
acor
(vWF)
and
wn
njured
hese
Actvaton.
orm
acors
a
ead
o
paee-rc
e
adeson
and
S econdary
emostass
s
acvaon
o
e
rggered
by
e
exposure
o
ssue
subendoeum
w
acor
VII
and
ssues.
(descrbed
aer)
Tssue
o
acor
nae
acs
e
as
wc
uses
n
e
paees
coacors
and
cange
e
coacors
growng
subendoea
1b
coa-
(Gp1b).
sape
conens
o
rom
smoo
er
granues,
dscs
o
wc
spky
ncude
(cacum,
a
are
presen
on
e
eads
o
e
deposon
o
brn.
dpospae
acor
(ADP),
V)
and
wc
paee
recru
acvaors
oer
paee
paees
acvaon
exposes
pug.
con-
Aggregaton.
he
sape
cange
assocaed
w
coaguaon
suraces
carged
Fbrn
pospopds,
wc
are
requred
by
ceran
o coaguaon
acvaed
reease
adenosne
negavey cascade,
exposed
gycoproen
acor
• juncon
beween
recepor
paees,
o wn
brdge
pug. suc
•
a
Paees
and
coaguaon wc
as
surace
vesse speres
was.
acs
paee
subendoea
• coagen
wc
3.4):
acors
(descrbed
aer),
and
aso
aers
e
conorma-
renon o surace gycoproen IIb/IIIa (GpIIb/IIIa), converng GpIIa/
orces
and
sabzes
e
paee
pug,
seang
e
area
o
vascuar IIIb
damage
and
prevenng
urer
o
a
g-ainy
neracons Once
a
co
as
ormed,
s
exen
mus
be
med
o
e
area
hs
s
medaed
by
counerreguaor y
mecansms,
wc
paees
dscuss
aer
n
s
or
GpIIa/IIIb
brnogen.
recepors
Bvaen
and
brdgng
brnogen
o
cump
no
en
aggregaes.
we Decences
w
nvovng
o cause
damage.
recepor
beedng.
o
GpIb,
caper. ma
beedng
(Fg.
3.5).
GpIIa/IIIb,
or
vWF
are
assocaed
w
abnor-
CHAPTER
A.
Hemodynamic
3
Disorders,
Thromboembolism,
VASOCONSTRICTION
and
Shock
33
Deficiency:
Bernard-Soulier Endothelium
Basement
membrane
Arteriole
smooth
muscle syndrome
Deficiency: GpIb Glanzmann Platelet thrombasthenia
Site
of
injury
GpIIb-IIIa Fibrinogen complex
GpIb Endothelium
ADP
Endothelin
causes
release
Reflex
vasoconstriction
ECM
induces
conformational
(collagen)
change
vasoconstriction
von
Willebrand
factor
B.
PLATELET
ACTIVATION
AND
AGGREGATION Deficiency:
von
Subendothelium
Fig.
2
Shape
change
4
3
Granule
Recruitment
3.5
sive
(ADP, Platelet
adhesion
between
and
aggregation.
subendothelial
vWF
collagen
functions
and
the
as
an
adhe-
glycoprotein
Ib
release (GpIb)
1
Platelet
bridge
Willebrand
disease
TXA
adhesion
platelet
receptor.
Platelet
aggregation
is
accomplished
by
fibrin-
)
2
ogen
Aggregation
binding
genital
(hemostatic
to
platelet
deficiencies
in
GpIIb-IIIa
the
receptors
various
on
receptors
different
or
bridging
platelets.
Con-
molecules
lead
vWF plug)
to
the
diseases
indicated
in
the
colored
boxes.
ADP,
Adenosine
diphos-
5
phate.
Endothelium
Basement
reeased
Collagen
by
acvaed
paees
s
romboxane
A
2
,
a
poen
agons
o
membrane
paee
be
C.
ACTIVATION
OF
OF
CLOTTING
FACTORS
AND
A
FORMATION
2
aggregaon.
nbon
Asprn’s
anpaee
o cycooxygenase, an
efecs
enzyme
are
due
requred
o
or
s
rrevers-
romboxane
syness.
FIBRIN
Coagulation
he
nae 2
coaguaon
n
e
cascade
deposon
s
o
a
seres
brn.
o
In
enzymac
e
reacons
aboraor y,
e
a
cascade
cum-
as
wo
e
sec-
Phospholipid
3 complex
Thrombin
naon
activation
Fibrin
ond
polymerization
• Tissue
pons,
one
nvovng
acor
XII
(conac
acor)
and
expression
4
1
Cascade
factor
Tissue
one
e
nvovng
ntrnsc
acor
VII
patway
(Fg.
sars
3.6).
w
acor
XII
and
s
naed
n
e
factor
aboraor y
by
e
addon
o
negavey
carged
maera
suc
as
1
gass
beads,
me
un
aong
e
•
Fibrin
e
extrnsc
addon
factors
protein
induce
Ib
granule
boxane
A
GpIIb-IIIa
a
transient
(GpIb)
matrix
release.
2
(TxA
)
2
vasoconstriction.
receptors
and
to
are
(B)
Willebrand
activated,
Released
induce
von
undergoing
adenosine
additional
Platelets
factor
a
diphosphate
platelet
bind
via
on
shape
change
(ADP)
aggregation
cum
glyco-
(vWF)
and
through
tissue
(C)
factor
binding
Local
and
and
cum,
throm-
to
fibrinogen,
and
form
the
activation
platelet
of
the
coagulation
phospholipids)
results
in
the
platelets
extracellular
into
a
definitive
secondary
Paee
acvaon,
brn
co
s
recorded
pasma.
as
e
he
para
sars
acor,
w
cacum,
acor
and
VII
and
s
naed
pospopds
o
by
pasma.
e
Ca-
e
e
proease
wo
a
occurs
sysems
ceaves
proease-acvaed
recepor
nas
paee
a
augmen
by
or
prorombn
specay
moded
pospopds
acor
IX
and
and
(provded
acor
X
acors
guamae
by
VII,
IX,
resdues
paees
compexes.
he
and
a
n
e
me
X,
a
bnd
body)
un
o
ca-
e
are
or-
o
a
brn
co
s
recorded
as
e
prorombn
me
(PT).
he
hemo-
seps
n
e
coaguaon
cascade,
common
o
bo
paways
are:
(involving
•
converson o acor X o acvaed acor X (Xa), wc s med-
•
converson
polymerization,
hemostatic
by
a
compex
o
acor
IXa
and
acor
VIIIa
plug.
o
prorombn
o
rombn
by
a
compex
o
acor
matrix.
aggregaon
and
coacor
wereas
Xa
bn,
a
o
platelet
primary
cascade
fibrin
a
requred
aed “cementing”
ECM,
o
pospopds,
(PT T).
patway
ssue
conan
maon
receptor
plug.
s
wc
exposed
key static
me
and
Normal hemostasis. (A) After vascular injury, local neurohumoral
extracellular
a
o
cacum
ormaon
rombopasn
Fig. 3.4
w
n
parae
work
ogeer.
brnogen
on
e
o
surace
acvaon
w
and
Mos
creae
o
coaguaon
noaby,
brn,
paees,
aggregaon.
aso
acor
rom-
ceaves
rggerng
Anoer
a
sg-
acor
•
•
he
or
and
Va
converson o
eemens
X,
coacor
common
he
PT
uncon
acor
by
V ,
e
o
brn
exrnsc
prorombn,
medaed
and
and
by
rombn
nrnsc
paways
brnogen)
(ac-
comprse
e
paway.
and
bu
brnogen
sared
e
do
PT T
no
are
useu
recapuae
or
e
evauang
evens
a
e
ead
coaguaon
o
cong
acor
nvvo.
34
CHAPTER
Hemodynamic
3
CLOTTING
Intrinsic
IN THE
Disorders,
Thromboembolism,
LABORATORY
(e.g.,
Shock
CLOTTING
IN VIVO
pathway Vascular
Negatively
and
charged
glass
Exposure
surface
damage
of
tissue
factor
beads) TF
Extrinsic
pathway
TF XII
Tissue
XIIa
factor X* VII*
VIIa
TF
XI
XIa
VII*
IX*
IXa
X*
VIIIa
TF Va
IX*
IXa
VIIa Xa
XI
Xla
VIIIa
Va
Prothrombin*
Thrombin
Xa
Prothrombin*
Thrombin Fibrin Fibrinogen clot
Fibrin Fibrinogen
A
Fig.
ing
or
3.6
The
a
source
tors,
is
the
Factors
acts
min
exampe,
wereas
der.
In
rare
paens
conras,
beedng
w
n vvo
s
nvvo
by
e.
ssue
K
dark
is
hs
acvang
XI
and
acor
an
o
acor
oer
a
a
IX
XII
[see
e
raer
(*)
for
are
a
major
the
pathway).
involving
active
9])
do
X
o
VII
(Fg.
(B)
In
K
no
w
are
vivo.
and
the
all
of
of
light
as
the
these
Once
e
mus
conned
o
o
coaguaon
e
acors
mmedae
se
and
o
eum
coaguaon
cong
ac
Heparin-like
INHIBIT
pathway
near
ncude
acors,
e
serous
as
factor
romb n ,
w c
rom
o
are as
o
laboratory
(intrinsic
initiator
are
e
S
(not
clotting
a
o
we
as
njur y.
co
o
an
a
fac-
cofactors.
Warfarin
factors.
o
Vita-
negave
hese
a
reguaors,
by
nac
mo s
or
and
nacvae
soube
mp or an
e nd o e u m
O ne
su r a c e
w ay
a
proe n
as
s
on
effects
t-PA and
NO
Thrombin III
tissue
complexes
Thrombin
Inhibits Protein
C
Active
protein
platelet
C aggregation
Inactivates
(also
factors
thrombin
IXa
and
(requires
Xa)
protein
S)
Activates
Inactivates
Fig.
tion
3.7
Anticoagulant
cascade
pathway
that
are
inhibitor)
plasminogen
properties
expressed
endothelium,
activator),
which
of
on
as
normal
endothelium.
(heparin-like
well
stimulates
as
and
of
VIIIa
are
of
fibrin
platelets
clot.
fibrinolysis
multiple
thrombomodulin)
inhibitors
breakdown
Va
Highlighted
molecules,
secreted
the
factors
or
inhibitors
secreted
(PGI
2
and
of
from
NO)
the
coagula-
(tissue
and
t-PA
s
a
a c v ae d
w ase d
o c c u rs
Antithrombin
factor-VIIa
acors
s
factor
(tissue
by
w ay
rou g
e nd o e u m
Thrombomodulin
Endothelial
Inactivates
an-
varous
c ou ne r- re g u a -
are
inhibitor
2
mos
endo-
endoeum-derved
nb
an c o ag u an
PGI
e
norma
3.7).
nor ma
d amage.
o
inactive
to
nbors
(Fg.
e
b e c ome s
coagulation,
produced
moecues
nvov ng
v as c u ar
number
paee
o
add-
factors.
consuvey
se
by
pathway)
depicted).
coagulation
surace
romb n
of
are
correspond
nvoves
s e ve r a
me can s ms
b nd ng
and
dssouon
R e ma rk aby,
commences,
preven
Tissue
molecule
THROMBOSIS
o
ces
promoe
3.6).
hs
wc
the
polypeptides
K–dependent
o
coaguans
major
red
C
in
beads
K–dependent
mporan
severe
the
proteins
vitamin
consequences.
ncom-
is
glass
polypeptides
beed,
compexes
paees
njur y
green
initiated
as
The
dsor-
Control
acvaon
be
factor
lines).
are
is
such
vitamin
or y
Coagulation
Clotting
tissue
(dotted
dependent,
of
(A)
substance
vivo,
-carboxylation
synthesis
or
in
thrombin
vitamin
assocaed
and
charged
factors,
beedng
naor
acor
negative
the
md
Caper
laboratory
a
are
decency
ave
acor/acor
an
are
inhibiting
cofactor
acors
ssue
loops
asterisk
by
the
(extrinsic
feedback
decency
emopas
suggess
acor,
with
in
either
polypeptides
essential
w
acor
(e
green
and
factor
by
anticoagulant
an
cascade
calcium,
tissue
marked
an
decences
dsorders
pabe
as
of
amplified
paens
w
coagulation
phospholipids,
which
For
B
clot
caed
CHAPTER
trombomodun.
o ge n
C
and
and
s
c o a c or
d e n
s
by
s een
w c
r sk
n
T e
nc re as e d
p a e n s
a c ors
romb n
su e
X.
or
o
re c e por
bre a kd ow n
o
a
o
ae r.
on
onge r
o
u r n
deep
v ar an
s
a c or
by
e nd o e u m ,
c o s
o
ve nous
o
( - PA ) ,
s
ab e
c e ave
a c or
V
caed
C.
V ,
and
e
mp or an
br n -
a
V
cong
ead
a
ear
L eden,
a c v ae s
o
o
acvaed
acor
et
•
o
abnormaes
or
oowng
ara
urbuen
ders
re e as e
o
s -
may
a c v aor
o
e
ed
s
e
daon
be
bood
due
acors
ound
and
a
n
Shock
and
or
o
e
low :
narcon,
mra
prone
o
acqured
35
mpedes
15%
varan
o
or
o
e
nlow
V
and
s
3.2).
ara
any
ncreases
vesses
o
an
he
norma.
mos
Norern
pasma
can
o
e
areres;
braon.
aeraon
Leden (aready
o
e
daons
aerosceroc
and
romboss
peope
a
ear
aneurysma
senoss;
(Tabe
ncude actor
2%
genec
o
afecng
Hypercoaguaby
more
nered
rsk
acors
bood
myocarda
Hypercoaguabty.
e
( br noy s s ) .
sass
coaguaon
and
nbors.
Numerous
e v -
re u r n
Thromboembolism,
wasou
c r c a
( DV T )
w
Disorders,
Proe n
ma d e
a c or
We
c e ave s
C.
s
romb o s s
s mu a ng
an
c e ave
re a c on
proe n
a s o
o
proe n
n a c v ae
T romb n
a c v a on
br n
n
n a c v a on
DV T
p as m no ge n
S,
no
ab y
mp or anc e
r sk
w
re s s an
e
proe n
a c or
e
romb n
a c qu re s
c o a c or,
or
s
B ou nd
nse a d
Hemodynamic
3
a
he
ren-
causes
common
ner-
menoned),
wc
European
eves
o
descen,
prorombn.
Inered rsk acors are assocaed w romboss a a young age;
THROMBOSIS n
genera,
ess Thrombosis,
the
abnormal
clotting
of
blood
within
intact
vessels,
an
e
50
occurrence
years
o
age
s
o
an
a
romboc
ndcaon
or
even
a
n
genec
an
ndvdua
workup.
Even
is
more common are acqured rsk acors: age over 50 years, mae sex, associated
with
a
serious
risk
of
mortality.
mmobzaon, Pathogeness.
hromboss
relecs
some
abnormay
nvovng
ora vesse
wa,
e
low
o
bood
(speccay,
sass
or
urbuen
conracepves),
bood
coaguaby,
an
aeraon
reerred
o
as
ree
acors
make
up
e
Vrcow
trad
(Fg.
3.8),
named
or
18
cenur y
paoogs
Rudo
n
Abnormates
of
te
vesse
wa
pregnancy
ncrease
use
o
syness
and
o
e
proens
and
reduce
ormaon
o
ancoaguan
pro-
ver.
oer
causes
o
ypercoaguabe
saes,
wo
deser ve
Vrcow.
bre
•
(e.g.,
Esrogens
e
Among amous
saes
smokng.
ypercoaguaby
ens hese
and
low),
procoaguan or
yperesrogenc
e
(endotea
njur y).
In
vesses
menon
because
o
er
unque
paogeness
and
cnca
car-
mporance: r yng
bood
a
g
pressures
and
under
g
sear
orces,
suc
as
e
e
aora
areres
and
s
major
suppyng
e
brances,
CNS,
co
e
coronar y
ormaon
s
areres,
mos
•
Heparn-nduced
thrombocytopena
o
reaed
5%
o
paens
o
aerosceroc
esons
(see
Caper
7).
Rupure
o
paques
acvaon
o
exposes
paees
abnormaes
coagen
and
assocaed
and
ssue
coaguaon
w
acor
acors.
aerosceross
and
he
ead
o
syndrome
unraconaed
occurs
eparn
and
a
n
eads
s
o
paens
caused
by
reaed
w
anbodes
a
ow-moecuar-weg
bnd
o
compexes
eparn.
composed
eparn
and
paee
eads
paee
acor
4.
hroug
uncear
mecansms,
maor y
ead
•
acors
proromboc
o
processes
rombus
by
sae
suc
endoea
seen
as
n
ces,
wc
aerosceross.
vascus
a
may
o
acvaon,
paee
consumpon,
and
deposon
ncreased
conrbue
Trauma
damage
paee-rc
cos
n
e
arera
and
venous
crcuaon.
hese
or
vesses
o
nlam-
aso
may
Table
ormaon.
3.2
Hypercoagulable
States
Abnorma bood ow. Turbuence and sass conrbue o romboPrimary
(Genetic)
ss n e ear and e arera sde o e crcuaon, wereas sass
s e major acor n e deveopmen o venous romb. Sass and Common
urbuen
bood
low
cause
canges
n
endoea
ce
gene
a
avor
romboss.
Stass
aows
paees
(>1%
exended
V
mutation
w
e
endoeum
vesse
or
wa,
areas
were
denuded
ey
o
may
encouner
endoeum;
Population)
V
Leiden)
mutation
dysuncona
sass
aso
sows
e
Rare
Antithrombin
ENDOTHELIAL
the
(factor
conProthrombin
ac
of
expresFactor
son
INJURY
III
deficiency
Protein
C
deficiency
Protein
S
deficiency
Secondary
Higher
Cardiac
Tissue
(Acquired)
Risk
Prolonged
for
bed
Thrombosis
rest
dysmotility
injury
or
immobilization
(myocardial
(surgery,
fracture,
infarction,
atrial
fibrillation)
burn)
THROMBOSIS
Disseminated
Prosthetic
cancer
cardiac
Disseminated
valves
intravascular
Heparin-induced
coagulation
thrombocytopenia
ABNORMAL
BLOOD
Antiphospholipid
antibody
Lower
Thrombosis
Risk
Nephrotic
Fig.
3.8
Virchow
triad
in
thrombosis.
Endothelial
integrity
is
the
for
syndrome
factor.
Abnormalities
of
procoagulants
or
anticoagulants
the
balance
in
favor
of
thrombosis.
Abnormal
blood
flow
(stasis
contraceptive
or Sickle
turbulence)
can
lead
to
hypercoagulability
directly
and
also
cell
indirectly Smoking
through
endothelial
dysfunction.
states
can Oral
tip
(due
to
loss
of
antithrombin
III)
most Hyperestrogenic
important
syndrome
HYPERCOAGULABILITY
FLOW
s
endoea
e
o
e
o
o
expresson o procoaguan acors and e decreased expresson o
ancoaguan
up
ower
aero-
HIT sceroc
w
commony
racon due
(HIT)
and
anemia
use
(during
pregnancy
and
following
delivery)
36
CHAPTER
cos
may
ead
syndrome
•
o
and
oss
ons,
may
o
mbs
cessaon
Antpospopd
romboss,
Hemodynamic
3
an
or
e,
eparn
antbody
repeaed
be
o
and
soaed
recognon
erapy
syndrome,
mscarrages,
anomay
Disorders,
are
assocaed
and
or
o
ereore
w
cardac
e
o
and
Shock
HIT
crca.
recurren
vave
secondar y
Thromboembolism,
vegea-
an
auom-
mune dsorder (e.g., sysemc upus er yemaosus). he name o
s
dsorder
a
bnd
o
mporan
came
rom
e
pospopds
paoogc
deecon
n
e
efecs
n
ab.
o
I
crcuang
s
paens
beeved
are
anbodes
a
e
medaed
mos
roug
bndng o ese anbodes o epopes on proens a are some-
ow
nduced
peced
a
a
or
“unveed”
ese
ypercoaguabe
ever,
us
n
vro,
nb
sae
e
msnomer).
a
componen
he
o
roug
(ence
es
or
o
varous
e
oten
s
and
sus-
nduce
How-
pospopds
upus
cross-reac
syps,
vvo,
mecansms.
w
name
In
proens
unceran
nerere
anbodes
e
pospopds.
bnd
anbodes
coaguaon
a
by
anbodes
and
antcoaguant
w
producng
a
A
s
cardopn,
ase-posve
resu.
Morphology.
esons,
Arera
wereas
occur
a
o
underyng
e
ses
obsruced
propagae
o
sass.
and
oward
a
o
propagae
rerograde
he
and
prone
ses
or
o
drecon).
o
wa.
Venous
porons
ong
are
no
are
aaced
n
paray
romb
romb,
romb
ormng
are
ocaed
bood,
arera
aerosceroc
caracerscay
romb
Wen
lowng
(even
dsance,
overe
romb
naon,
cardac
ear
propagang
ypcay
cardac
exposed
e
some
umen.
and
A
vesse
vesses
n
romb
venous
end
wc
parcuary
cass
wn
aaced
o
o
grow
key
e
vesse
vesse
was
B are
o
ragmenaon
Mcroscopcay,
romb
and
ave
embozaon.
amnaons
caed
nes
of
Zan,
Fig.
3.9
apices,
wc
represen
aernang
pae
ayers
rc
n
paees
and
Mural
darker
ayers
rc
n
red
ces.
Layered
romb
ony
orm
bood,
and
e
presence
o
ese
ayers,
as
we
as
e
o
romb
rom
racon
o
romb.
emboc
o
sed
o
co
o
e
posmorem
red
In
cos.
wa,
V enous
n
days
and
oowng
or
weeks
romb
undergo
romb,
exraceuar
e
brn
may
marx
are
(red
an
o
conan
accompaned
by
connue
eFg.
and
e
var yng
or
speca
3.1).
In
depos-
degrees
o
romb
desgnaons.
ear
vaves
are
ypercoaguabe
era
and
or
may
o
boses
aortic
occurrng
hromb
n
occurrng
e
n
ear
e
or
ear
caed
saes
vegetatons.
and
unga
necons
ead
e
o
are
sere,
(necve
deveopmen
o
Some
aora
and
e
bu
vegeaons
oers
are
endocards;
arge
bear
aorc
occur
caused
see
romboc
(left
aneurysm.
on
the
left
Laminated
Numerous
advanced
side
necon
(DVTs)
emboze.
of
and
right
ventricular
thrombus
in
friable
mural
a
thrombi
dilated
are
atherosclerotic
lesions
of
the
more
also
proxi-
photograph).
by
n
bac-
Caper
8)
masses.
and
n
DVTs
cannes
varcose
arge
aso
eg
may
requeny
ucers.
vens
a
or
cause
pan
crcumven
By
conras,
above
and
e
edema,
e
deep
eve
venous
o
bu
e
coaera
obsrucon.
rom-
knee
oten
venous
Consequeny,
approxmaey 50% o DVTs are asympomac and are recognzed ony
ater
ey
he
umen (Fg. 3.9) are reerred o as mural thromb, wereas romb
on
aorta
skn
recanazaon.
Nonobsrucve
in
(B)
ger
arera
romboc
(Suppemena
ces
a
an
dssouon;
sroma
scar.
anemorem
cos)
na
undergo
organzaon
ngrow
dsngus
romb
enrapped
vascuar
embo;
vesse
ces
e
even,
organzng
on
e
Thrombus
rm mal
aacmen
(A)
fibrous
n superimposed
lowng
white
brn,
abdominal
and
thrombi.
overlying
ave
embozed
cnca
oversaed.
secondar y
narcon
he
o
o
e
mporance
greaes
o
aack)
n
romboemboc
s
aerosceross,
(ear
ungs.
o
aken
wc
e
by
s
e
Wesern
dsease
coronar y
major
word.
arer y
cause
Embo
canno
be
romboss
o
myocarda
sed
rom
e
ear and romboemboc dsease due o aerosceross o e carod
areres
(CNS)
DVTs
and
are
s
oer
an
aa
grea
vesses
mporan
n
cause
approxmaey
suppyng
o
3%
sroke.
o
e
cenra
Pumonar y
afeced
ner vous
sysem
embozaon
o
paens.
EMBOLISM Clncal
Features.
obsrucon
vesses
and
romb
areres
due
e
ss,
o
s
Cnca
vesses
organs
and
occusve
he
hromb
panu
and
and
e
dsease
90%
n
cause
o
s
afeced.
ence
bood
more
o
dea
congeson
and
rarey
edema,
var y
o
due
o
e
accordng
o
e
eared
are
compcaon
romb
cause
organs
romboses
vens
romb
wereas
arera
n
by
and
mos
key
suppy
dscussed
superca
he
aer),
beween
venous
caused
embozaon
(dscussed
reaonsp
cardac
an
o
sympoms
co
are
embozaon
are
More
and
a
obsrucon
bran.
es.
o
a
suc
oca
as
e
romboss,
n
Caper
occur
n
e
emboze,
n
o
smaer
narcon
ear
and
aeroscero-
8
predsposng
embolus
mass
tant
that
site,
function
he
ence,
ey
e
exrem-
may
be
overyng
(.e.,
or
vas
a
is
a
o
detached
carried
it
by
may
the
intravascular
blood
cause
from
vascular
solid,
its
liquid,
point
of
obstruction
or
origin
and
gaseous
to
a
organ
dis-
dys-
infarction.
majory
erm
lud.
orgn
o
embo
are
derved
tromboembosm.
dropes,
coesero
amnoc
se
is
where
e
ncude
ower
bu
An
bubbes
embo),
Embo
un
ey
o
ar
umor
are
Less
or
nrogen,
ragmens,
ranspored
odge
n
e
rom
bs
roug
rs
dsodged
common
vesse
ypes
romb;
o
embo
aerosceroc
o
bone
e
a
bood
s
debrs
marrow,
oo
rom
and
er
narrow
o
CHAPTER
Supplemental
stained
elastic
for
lamina
punctuated
spaces).
eFig.
elastic
(arrows)
by
3.1
tissue.
and
several
Low-power
The
is
original
totally
recanalized
Hemodynamic
3
view
lumen
filled
is
with
of
a
thrombosed
delineated
organized
endothelium-lined
by
the
Disorders,
artery
internal
thrombus,
channels
now
(white
Thromboembolism,
and
Shock
36.e1
CHAPTER
perm
son.
urer
he
scemc
ung,
passage,
major
necross
wc
as
Nevereess,
boembosm
morbidity
romb
and
ca
and
•
o
cnca
vascuar
one
proecs
assocaed
compee
w
occu-
beds
excepon
agans
s
s
from
an
rom-
dsease.
95%
e
and
o
are
frequent
o
s
as
e
ound
w
per
embo
e
causes
rg
n
year
n
orgnae
knee.
vascuaure.
assocaed
number,
he
no
A
vascuar
bend
arge
e
e
undergo
of
sde
A
anoxa.
o
embous
may
burcaon
o
occude
e
somemes
or
causng
webs
e
rg
Caper
rom
oer
•
Fa
a
ear
compee
n
he
cn-
s
embo
var y
become
recanazaon,
(Suppemena
man
and
eer
et
vruay
pumonar y
pumonar y
or
areres
nsananeous
•
3.1)
arer y
aa
orrage,
bood
bu
roug
Lodgng
oten
narcon
of
nac
embo
resus
genaon
an
o
n
s
n
bronca
te
narcon,
e
ung
s
uncommon
sma
may
cause
because
crcuaon
(dua
parcuary
n
by
aso
(sadde
ndvduas
congesve
n
o
emboc
em-
receves
Sot
ssue
o
10%
e
o
oxc
efecs
compcaon
moray
rae
deas
e
o
o
n
enson
and
Rarey,
and
an
eners
odgng
n
rg
venrcuar
embous
e
sysemc
end-arera
(paradoxca
passes
ear
aure
roug
crcuaon,
vascuar
beds
an
e
(cor
ara
were
n
cause
on
oxy-
o
raer
aure.
a
may
bran
yper-
•
venrcuar
cause
(sroke)
deec
narcs
or
s
e
ay
ces
abor
e
odge
end
o
occur
or
marrow)
caber
ssue’s
n
n
no
end
o
e
vuner-
areres,
dsnc
causng
racure
can
a
anema,
mecanca
acds
cause
o
reease
cnca
ong
3.2).
by
bones
mcroscopc
embosm
eFg.
caracerzed
e
and
syndrome
hs
syndrome
pumonar y
nsu-
rombocyopena,
obsrucon
reeased
rom
e
o
and
sma
pd
ves-
gobues
njur y.
dever y
Uned
neuroogc
maerna
or
oowed
pumonae).
or
bu
uerne
Saes,
decs.
crcuaon
ven
(1
80%.
I
n
and
o
lud
ears
(Suppemena
brs)
responsbe
85%
Amnoc
roug
40,000
s
n
eFg.
s
o
ave
conens
pacena
3.3).
as
10%
sur vvors
and
e
a
or
he
mem-
onse
s
sudden and s caracerzed by severe dyspnea, cyanoss, and sock,
brances
pumonar y
on
afeced
oten
(Suppemena
and
e
by
sezures
componens
an
crss,
Ar
Gas
vascuar
coma.
e
mecanca
embosm.
obsruc
and
o
dssemnaed
secondar y
o
e
njures
er
approxmaey
lud.
bed
o
endoea
amnoc
vascuar
n
sympoms,
Bo
deveops
pumonar y
dsease
crcuaon,
cases
poron
e
depend
and
embo
crus
a
paens
Mupe sma embo occurrng over me may obsruc a suicen
o
suppy,
arera
abundan
no
permanen
wom
ear
(10%),
Emboli
beedng.
maerna
crcuaon).
pumonary
bran
Amnoc lud embosm. Amnoc lud embosm s a rare bu ser-
a
dea.
area
or
oucome.
neuroogc
and
ous
odge
pumonar y
e
end-arteroar
compromsed
n
nearby
branes
capares
ave
mnory
he
o
embozaon
Because
orms
cency,
ncorpo-
somemes
eFg.
o
coaera
common
gobues
a
ener
rupure
e
embosm.
o
10.
(75%)
37
sengs:
(wc
e
exremes
Shock
In addon o rombus, embo may be composed o oer subsances.
Smaer embo may obsruc smaer, brancng areres (Fg. 3.10).
subsequen
a
peeca
and
undergo
brous
s
Fragmened
more
pumonar y
e
ower
consequences
aby
oows:
organzaon
wa
brdgng
e
vesse,
on
ey
n
and
spared.
occuded
ses
me,
odge
s
narcon
deas
e
roug
embosm
and
cases,
pumonar y
eaures
sze
100,000
proxma
pass
Thromboembolism,
Nonthrombotic
DVTs
abou
vens
usuay
n
organ
e
narcon.
pumonar y
embo
hese
eg
pumonar y
e
embous),
•
ssues;
a
or
mos
W
a
•
n
Most pumonary embo (60% to 80%) are sma and cncay sent.
eavng
•
DVTs
paoogc
raed
•
canges
cause
more
deep
arresed
o
para
mortality.
In
rom
accordng
afeced
suppy
sgncan
originate
embo
wn
dscusson
n
Disorders,
Thromboembolism
and
become
resu
embozaon
o
bood
cause
emboli
Saes.
romb
dua
crcuaor y
Pumonar y
Uned
ey
o
(nfarcton)
a
oten
Pulmonary
Pulmonary
were
consequence
Hemodynamic
3
o
paogeness
mmune
obsrucon.
I
nravascuar
e
bubbes
low,
he
nnae
reease
wn
causng
sysem
e
paen
coaguaon
o
nvoves
and
sur vves
(Caper
rombogenc
e
crcuaon
dsa
scemc
acva-
coaguaon,
e
9)
n-
oten
subsances
can
coaesce
njur y.
Gas
n
and
may
be
by
nroduced no e vascuaure accdenay durng surgca, obse-
esewere
rc, or aparoscopc procedures; oowng a severe ces wa njur y ;
embosm).
or
as
a
consequence
o
sudden
decreases
n
e
amosperc
pres-
sure (e.g., wen dvers surace oo rapdy, dssoved nrogen comes
Systemic
he
mos
(80%),
Thromboembolism
common
oowed
vavuar
by
vegeaons,
source
o
aerosceroc
and
ou
sysemc
DVTs
(by
romboembo
aorc
esons,
paradoxca
aorc
s
e
ear
o
souon,
condon
ormng
known
as
e
gas
bubbes
n
e
bood
and
e
ssues,
a
bends).
aneur ysms,
embozaon).
Mos
INFARCTION
An
infarct
the
is
vascular
and
an
important
Arera
V enous
area
supply
of
to
cause
ischemic
the
of
clinical
romboembosm
romboss
can
necrosis
affected
tissue;
by
occlusion
is
a
of
common
disease.
underes
cause
caused
infarction
e
narcon,
vas
bu
majory
more
o
narcons.
commony,
ere
s
smpy congeson, as coaera cannes open rapdy and resore e are-
ra
nlow.
Inarcs
caused
by
venous
romboss
occur
n
organs
w
a
snge eferen ven (e.g., ess or ovary) and ypcay sem rom a mecan-
ca probem (e.g., wsng o a esce, eadng o venous obsrucon).
No
weer
•
a
bood
weer
w
3.10
Embolus
derived
from
a
lower-extremity
deep
venous
in
a
pulmonary
artery
branch.
ead
ncude
e
o
narcon.
Deermnans
o
oowng:
bood
o
s
o
e
an
suppes
narcon,
mos
mporan
ndvdua
(ung,
wereas
vesse
ver,
ose
and
w
acor
causes
and
kdney,
and
speen)
are
key
o
n
deermnng
damage.
and
narc.
Tssues
orearm)
end-arera
throm-
(ear, lodged
suppy
occuson
dua
ressan
bus
occusons
occurs
Anaomy o he vascuar suppy. he presence or absence o an aer-
nave
Fig.
vascuar
narcon
are
crcuaons
38
•
CHAPTER
Rate
of
cause
•
occuson.
narcon
Ceuar
o
mnues,
rom
Morphology.
(anemc)
occur
ssues
ng
w
vabe
may
w
angopasy
w
arera
can
be
eer
venous
o
o
ours
eer
low
ater
n
o
o
n
red
o
ony
mnues,
3
and
o
4
bro-
(as
n
(e.g.,
Re d
ovaran
e
narcon
we
(Fg.
orson);
ung);
as
or
narcts
and
occurred
Whte
narcts
end-arera
n
oow-
(e.g.,
occur
crcuaons
Fig.
(e.g.,
ear,
wedge
speen,
saped,
w
and
kdney)
(Fg.
e
occuded
3.11B).
vesse
a
e
Inarcs
apex
end
and
e
o
3.12
Remote
ormng
e
base
(Fg.
3.11A);
wen
e
base
s
a
ere
s
oten
an
overyng
brnous
mos
ssues,
n arc s
W n
de veops
a ong
a
e w
d sp ay
ours ,
co agu a ve
an
ne c ros s
n ammaor y
marg ns
o
narc s;
replaced
by
a
large
fibrotic
scar.
(cardac
(e.g.,
amponade)
pumonar y
(see Caper
8),
or
ou-
embosm).
Hypovoemc
e
es on
s
sock
resus
rom
oss
o
bood
or
pasma
voume
(s e e
due
o
emorrage
or
lud
oss
rom
severe
burns).
resp ons e
• e
compresson
obsrucon
(e.g., 1).
now
exudae.
• In
C aper
infarct,
serosa
low surace,
kidney
be
organ
exrnsc perper y
Shock
suscepby
ater
(emorragc)
band.
w
key
and
crcuaons.
er
de
30
ess
Thromboembolism,
scema.
obsrucon).
organs
are
coaera
range
20
or
suppes
arera
occusons
or
sepc
o
Neurons
occusons
bood
an
as
many
may
coaera
Ces
occuson:
Disorders,
occusons
deveopmen
ypoxa.
ater
be
reesabsmen
ater
to
ces
Inarcs
and
deveopng
e
vascuar
myocarda
reman
3.11A)
o
vunerabty
damage
bass
Sowy
due
Hemodynamic
3
usu a y
S eptc
sock
s
rggered
by
mcroba
necons
and
s
assocaed
we
w e sysemc nlammaor y response syndrome (SIRS). In addde ne d
w n
1
o
2
d ay s.
In amma on
s
o owe d
by
rep a r,
on b eg n nng
n
e
pres er ve d
marg ns
(s ee
C aper
2).
are
u maey
rep ace d
by
s c ar
ssue
(Fg .
3.12).
s
an
excep on
o
es e
genera za ons ,
as
s cem c
Neurogenc
n
e
CNS
resu s
n
queac ve
ne c ros s
o owe d
by
(s e e
Caper
may
be
rggered
paogeness
o
by
sepc
severe
sock
burns,
s
rauma,
dscussed
sock
resus
rom
e
oss
o
vascuar
one,
aer.
as
oowng
spna
cord
may
njur y.
g -
• oss
SIRS
he
ssue
occur njur y
mcrobes,
pancreas.
Te
• bran
o
Mos
and narc s
Anapyactc sock resus rom sysemc vasodaon and ncreased
17).
vascuar permeaby a s rggered by mmunogobun E–medSepc
narcs
occur
wen
neced
cardac
vave
vegeaons
aed emboze
narc
or
s
wen
mcrobes
convered
no
seed
an
necroc
abscess,
ssue.
w
a
In
ese
greaer
cases,
mmedae
Pathogeness. response
and
eang
by
organzaon
and
bross
ypersensvy
reacons
(see
Caper
4).
e
nlammaor y
(see
Caper
Sock,
regardess
o
s
cause,
as
ceran
common
ea-
2).
ures.
I
probem
n
e
aorc
sock
•
s
a
s
progressve
no
seng
Ina
are
Sock
n
and
sages
are
stage:
and
ypes,
stage:
organ
ssue
meaboc
eads
ends
(e.g.,
oer
va
a
njur y
hese
seen
Progressve
cuaor y
•
massve
nonprogressve
acvaed
•
correced.
o
aneur ysm).
bu
dsorder
o
dea
evove
e
roug
exsangunaon
bes
as
o
underyng
sages,
rom
documened
n
a
excep
rupured
ypovoemc
we:
relex
peruson
compensaor y
s
mecansms
are
mananed
ypoperuson
occurs,
w
worsenng
cr-
derangemens
Irreversbe stage, n wc ceuar and ssue njur y s so severe a
even
e
emodynamc
deecs
are
correced,
sur vva
s
no
pos-
sbe
In
oops
e
B
A
3.11
Red
and
white
pulmonary
infarct
infarcts.
(red
(A)
Hemorrhagic,
infarct).
(B)
Sharply
roughly
in
the
spleen
(white
nonprogressve
e
cardac
consrcng
and
pase,
oupu
e
decreasng
neura
and
areroes
e
urne
and
bood
(n
ormona
pressure
by
ypovoemc
oupu.
C oronar y
eedback
ncreasng
and
and
cardo-
cerebra
wedge-
demarcated
are
ess
sensve
o
sympaec
sgnas
and
manan
a
rea-
pale
vey infarct
rae,
sock),
vesses shaped
eary
manan
ear
genc Fig.
e
norma
caber,
bood
low,
and
oxygen
dever y.
hus,
bood
s
infarct).
suned
e
away
rom
e
skn
o
e
va
organs
suc
as
e
ear
and
bran.
Wou
correcon
o
e
underyng
cause,
sock
proceeds
o
e
SHOCK
Shock
is
a
circulating
diminished
state
volume
tissue
Proonged
oten
•
aa.
in
Is
diminished
causes
perfusion
sock
causes
Cardogenc
which
a
and
evenuay
a
sock
no
resus
fall
in
cardiac
blood
pressure,
consequent
eads
severa
rom
o
output
cellular
rreversbe
caegores
cardac
pump
effective
resulting
in
njur y
and
s
3.3):
aure.
I
may
pase,
a
oxygen
perssen
yss
nsead
ssue
hypoxia.
ssue
(Tabe
or
progressve
be
caused by myocarda damage (narcon), venrcuar arrymas,
pH
o
bood
pu,
owerng
dec,
aerobc
buns
and
caracerzed
poos
e
n
bood
ces
by
are
respraon,
vasomoor
e
wdespread
orced
causng
response;
mcrocrcuaon,
pressure,
and
pung
o
ssue
rey
acc
as
a
on
ypoxa.
Due
anaerobc
acdoss.
resu,
worsenng
he
owered
areroes
e
endoea
dae
cardac
ces
a
o
gyco-
ou-
rsk
or
anoxc njur y. Endoea dysuncon en ses e sage or e deve-
opmen
o
wdespread
ssue
edema
and
dssemnaed
nravascuar
CHAPTER
Supplemental
eFig.
circulation.
cellular
The
hematopoietic
cells,
3.2
Bone
marrow
elements
whereas
the
on
the
Hemodynamic
3
embolus
left
cleared
side
in
of
vacuoles
the
the
Disorders,
Thromboembolism,
The
relatively
uniform
red
area
on
the
right
of
represent
the
organizing
38.e1
are
marrow
embolus
is
eFig.
3.3
Amniotic
fluid
embolism.
Two
small
pulmo-
an
nary early
Shock
pulmonary
embolus
Supplemental fat.
and
arterioles
are
packed
with
laminated
swirls
of
fetal
squamous
cells.
thrombus.
There
is
marked
small
organizing
coagulation.
edema
and
thrombi
(Courtesy
Dr.
congestion.
consistent
Beth
Elsewhere
with
Schwartz,
the
lung
disseminated
Baltimore,
MD.)
contained
intravascular
CHAPTER
Table
Type
3.3
of
Major
Types
of
Shock
Disorders,
Thromboembolism,
and
Shock
39
Shock
Clinical
Cardiogenic
Hemodynamic
3
Examples
Myocardial
infarction
Ventricular
Principal
Pathogenic
Failure
myocardial
rupture
of
damage,
extrinsic
Mechanisms
pump
resulting
pressure,
or
from
intrinsic
obstruction
to
myocardial
outflow
Arrhythmia
Cardiac
tamponade
Pulmonary
embolism
Hemorrhage
Hypovolemic
Fluid
Septic
loss
Inadequate
(e.g.,
vomiting,
Overwhelming
microbial
diarrhea,
blood
infections
Activation
of
damage;
uson.
begn
o
In
o
wc
wdespread
may
ssue
urer
compromse
ypoxa,
va
organs
e
are
ssue
per-
afeced
and
a.
e
o
approprae
conrace
oxde
Pathogeness.
(mos
uncon
syness.
ner venon
worsens,
Progresson
o
or
n
pary
rena
severe
owng
aure
cases,
o
occurs
e
ncreased
because
o
and
ropages,
componens
Sepc
(PAMPs).
ensue
ung)
suc
wen
sock
on
ces
and
ssues
o
ypoxc
njur y
(see
Caper
1)
and
are
caused
(Fg.
by
a
o
ypoperuson
and
mcrovascuar
romboss.
acvae
by
bacera,
e
compemen).
consuens
oowed
nnae
ces,
leukocyte-induced
coagulation
by
mmune
endoea
hese
ces
o
mcrobes
gram-negave
sysem
ces,
and
(.e.,
and
acors
mac-
soube
recognze
acvaon,
or
ason
3.13).
o
a
o
produce
Facors
sepc
number
wdespread,
sock
o
nlammaor y
nerac
sepc
beeved
ncude
o
e
n
a
sock
pay
responses
compex,
and
major
ncom-
muorgan
roes
n
e
oowng:
Inf ammator y
resp on s es .
PA M Ps
a c v ae
n am m aor y
combre sp ons e s
naon
rggered
activation/injury;
blood;
resembe
• ose
s
dendrc
massve
paopysoog y o
as
undersood
dysuncon
efecs
a
of
intravascular
gram-posve
Foowng
a,
peey
he
sock
endothelial
pooling
and are acvaed by mcroba paogen–assocaed moecuar paerns
n
dea.
and
disseminated
neurops,
rena scema (see Caper 11). he downward spra oten cumnaes
Morphology.
volume
cascades;
vasodilation
commony,
bacera
absence
myocarda
nrc
bo
W
plasma
cytokine
peripheral
coaguaon,
or
burns)
Any
by
e ng ag ng
re c e pors
on
n n ae
m mu n e
ce s,
su c
organ as
To - ke
rece ptor s
(s ee
C ape r
2),
w c
re c o g n z e
a
os
o
may be afeced; e bran, ear, kdneys, adrenas, and gasronesm c rob e - d e r ve d na
rac
are
mos
commony
nvoved.
Fbrn
romb
are
n
kdney
gomeru
bu
may
be
ound
rougou
he
ungs
are
ressan
o
ypoxc
njur y
n
occurrng
ater
emorrage,
bu
sepss
and
rauma
dfuse
alveolar
damage
and
acue
c y ok n e s
respraor y
ce
su c
(see
Caper
oss,
10).
afeced
Excep
or
ssues
can
rreversbe
recover
ur er
neurona
compeey
Features.
nsu.
ypoenson,
skn.
lused
s
e
due
In
a
he
ypovoemc
weak
rapd
conras,
o
perpera
even
necon).
pumonar y
manesaons
By
rggerng
bacera
canges
n
and
o
puse,
acypnea,
sepc
sock,
rapdy
sock,
and
coo,
may
prmar y
e
cardac,
on
e
precp-
paens
skn
narcon,
secondar y
aggravae
e
he
myocarda
However,
depend
cardogenc
vasodaon.
(e.g.,
sock
exb
cammy,
be
n
w
a
approprae
sock
s
(TNF)
an d
e n d o e a
a d e s on
an d
m o e c u e
c e m ok n e
a c v ae d
rou g
r ag m e n s
na
severe
rea
o
oxde
e
rena,
and
suaon.
w
by
o e r
ce s
( an d
e x pre s s on
by
pro du c on .
m c rob a
Te
c omp on e n s ,
e
o
proe oy c
a c v y
an apy aox ns
o
(C3a,
p a s m n ,
C5a),
subsanay
worse
sepc
or
oucomes,
car-
even
care.
Inducton
sock,
wc
admssons.
de.
s
ere
are
more
responsbe
Despe
or
mprovemens
an
750,000
cases
approxmaey
n
care,
20%
2%
o
per
o
30%
year
a
o
o
osp-
afeced
edema
e
o
and
op s on ns
njury.
juncons,
a
body.
oer
an d
pro n am m aor y
g
ms
(C3b),
resung
n
e
dever y
endoeum
nlammaor y
smoo
a
c e -
o
w c
cyoknes
oosen
s ae.
Inlammaor y
nuren
Acvaed
vasoacve
vascuar
a
procoaguant
drecy
endoea
many
by
of
coaguaon
aered
acors
ncrease
so
musce
as
ssue
endoea
low
vesses
sma
wasou
o
o
accumuaon
and
aso
wase
reaxaon
nrc
wc
and
o
remova
produces
medaors,
and
(e.g.,
may
sysemc
decrease
coaguaon
up
a
paens.
msed
o
by
e
brn-rc
sysemc
romb
sma
aers
producon
and
sass
acors.
o
and
hese
(see
s
rombn
and
In
(and
o
ac-
roug
expresson
cyo-
poss-
endoea
proen
peruson
vesses.
e
monocyes
coaguaon
Tssue
acvaon
n
e
producng
nravascuar
sepc
by
can
ndrecy
Pronlammaor y
rombomodun
dssemnaed
o
componens
and
sepss
producon
cause
o
XII
coaguaon.
decreases,
acvaed
Mcroba
acor
Moreover,
avor
acor
ces)
acors
n
state.
roug
uncon.
ancoaguan
e
Saes,
e
(C5a),
ypoenson.
•
vae
comparson,
and
conrbue
emorrage,
cerebra,
o
rougou
and
Shock
Uned
paens
managemen;
assocaed
sae-o-e-ar
sepc
a s o
pro du c on
ce
knes
e
an d
endoea
sur vve
In
c y ok n e
s
actvaton
o
Septic
cas cade
e
proen-rc
cya-
warm
he prognoss vares w e orgn o sock and s duraon. More
w
upre g u ae
Endotea
an 90% o young, oer wse eay paens w ypovoemc sock
dogenc
o
s mu ae
d re c y
c on r bue
noc
a c or
n du c e
sur vves.
•
ang
n e c ro s s
a
e
m o a c c
Clncal
u m or
and
re su ng paen
pro -
dsress
b o cardomyocye
as
m e d aors
yp es)
c omp e m e n syndrome
ce s
oten an d
precpae
m mu n e
ypovoemc o e r
sock
n n ae
e pro n am m aor y
body.
Ac v ae d
ready du c e
vsuazed
PA M Ps .
C).
Bood
dmnsng
derangemens
Caper
urer
e
u-bown
9)
n
compro-
deposon
dssemnaed
40
CHAPTER
Hemodynamic
3
Disorders,
Thromboembolism,
Microbial
and
Shock
products
(P AMPs) Neutrophil
and
monocyte
activation
Endothelial
Complement Factor
XII activation
activation
C3a
C3
TNF ,
Direct
and
Cytokines
Procoagulant
Antifibrinolytic
IL-6,
IL-8,
reactive TF
IL-1,
HMGB1
indirect
NO,
oxygen
and
cytokine-like
mediators
P AF ,
IL-10,
species,
apoptosis,
sTNFR
P AI-1 etc.
TFPI,
thrombomodulin,
protein
Secondar y
C
antiinflammator y
mediators
VASODILA TION MICROVASCULAR
SYSTEMIC INCREASED
THROMBOSIS
IMMUNOSUPPRESSION
PERMEABILITY
(DIC)
EFFECTS DECREASED
PERFUSION
Fever,
diminished
myocardial
TISSUE
Adrenal
insufficiency
Fig.
3.13
and
humoral
Major
multiorgan
nitric
nravascuar
ors
and
supermposed
•
Metaboc
and
and
neogeness.
suppress
acc
S epc
reease
ssues.
I
severe,
pospor yaon
may
suc
as
suc
and
ceuar
o
o
e
exb
umor
as
septic
ncreased
text.
sTNFR,
necross
ressance
and
acae
acor
drve
Sysemc
romboss
ypoenson,
decrease
e
dmns
and
or-
that
TF,
cells
lead
intravascular
e
ver
and
edema,
oxygen
o
tissue
and
Hg
ssue
and
to
cellular
end-stage
coagulation;
factor;
drome
Caper
he
a
(see
e
and
undere
TFPI,
luds,
remans
a
suc
o
and
ssue
daunng
o
e
NO,
tissue
organs,
n
and
e
cnca
vascuar
ese
medaors
urer
com-
permeaby
respraor y
acors
compexy
dsress
may
e
acor.
underyng
Even
caenge.
o
ner venon
necross
suppemena
ypoxa.
oupu,
and
syn-
conspre
kdneys,
o
ver,
dea.
e
umor
rea
secondar y
parcuary
erapeuc
as
and
cardac
acue
Umaey,
acors
anbocs
m
10).
mupe
precude
pressors,
and
ead
eves
and
Increased
cumnang
o
medaors,
remans
pressure
sepss
may
o
ear,
mupcy
specc
care
aure
cyokne
conracy
peruson.
njur y
ungs,
o
ssues.
myocarda
endoea
cause
guco-
producon
o
endothelial
events
receptor;
promsng
ox-
dever y
TNF
nurens
a
dmnsed
nersa
of
Disseminated
ac-
c yoknes
n
activate
cascade
n
ressance
grow
a
DIC,
a
soluble
reaenng.
nsun
products
initiating
nous
dysfuncton.
sma-vesse
FAILURE
Microbial
the
contractility ,
abnor malities
factor.
resung
pronlammaor y
ypoxa
in
inhibitor-1;
coaguaon
gucagon,
nsun
shock.
system,
provided
necrosis
acors,
caecoamnes
e
promoe
ead
be
are
activator
tumor
ese
paens
me,
and
TNF,
o
a
ormones
same
details
in
immune
acdoss.
Organ
and
e
nsun
oer
dave
A
innate
consumpon
dsorder
Cyoknes
pathways
the
Additional
inhibitor;
e
gucocorcods,
of
plasminogen
decences
abnormates.
sress-nduced
mone,
•
beedng
ypergycema.
IL-1,
and
causes
pathogenic
PAI-1,
pathway
coaguaon,
paees
MULTIORGAN
elements
failure.
oxide;
factor
metabolic
ISCHEMIA
oxygen
n
e
e
he
necon
o
bes
neracons
w
anagonss
sandard
and
manan
ceners,
o
nrave-
e
bood
sepc
sock
4
Diseases
of
the
Immune
System
O U T L I N E
Hypersensitivity
Immediate
Disorders,
(Type
I)
Antibody-Mediated
Immune
T
41
Rejection of Transplants, 52
Hypersensitivity,
(Type
II)
Complex–Mediated
Cell-Mediated
(Type
IV)
42
Immune
Hypersensitivity,
(Type
III)
44
Hypersensitivity,
Hypersensitivity,
47
of
47
Systemic
Lupus
Systemic
Sclerosis
Sjögren
he
o
Innate
ces
sysem
and
mmunty
pasma
50
Human
Life
51
nnae
s
e
proens
us
agans
mmuny
rapd
a
necons
and
aways
and
adapve
response
are
o
cancers
necons
presen
by
wo
•
mmuny.
cyes,
macropages,
epea
mecansms.
a
no
hese
recognze
recepors,
moecues
nnae
sared
and
poc ye
ave
a
by
s
and
gy
s
medaed
ready
med
paogens
e
B
speccy.
he
and
o
bu
by
Cell
uraon
o
e
gen-recepor
o
umors
and
are
To-ke
necroc
B
aack
and
•
ympoc yes.
derved
a
a
(see
or
e
are
and
ces.
a
unque
o
hese
mmunty
by
and
ces
neuraze
e
er
e
ces.
e
o
by
T
recepors
se
express
mecansms
medaed
by
dferenaed
opsonze
sysem.
a
occur
o
T
o
and
B
Lympoc yes
e
a
56
and
B
and,
s
o
ym-
rearranged
o
normay
e
ympoc yes
uncon
e
erm
angen
ypes
o
deense
emnae
an-
and
and
reacons:
eosnops,
can
go
progeny,
em
or
pasma
are
ces.
pagocyoss,
efecor
mcrobes
produced
Anbodes
and
ces.
CD4+
o
ces
are
ces
Heper
h1
ces
h17
make
ces
and
conss
acvae
ces
unc-
uncon
CD4+
poen
nduce
(APCs),
er
macropages
o
T
CD8+,
reacons.
acvaed
ces
perorm
and
acvae
B
c yoknes
and
T
o
o
desroy
anbodes,
severa
dferen
sub-
ypes
macropages,
smuae
d-
eper
h2
neurop-rc
e
awry
ces.
mmune
and
cause
sysem
ssue
evoved
njury
as
and
a
proecve
cnca
orce,
dsease.
In
a
mes
s
cap-
er, we dscuss e mos mporan paoogc reacons and dseases a
are caused by mmune responses, many adapve mmune responses, as
we
as
decences
Persistent,
tions
o
e
mmune
acvae
misdirected,
against
sysem
and
er
consequences.
DISORDERS
a
variety
or
of
inadequately
antigens
may
regulated
cause
immune
tissue
reac-
injury.
An ndvdua wo as been exposed o and reacs agans an angen
s
sad
o
be
senstvty
dicu
o
dseases
wc
T
paoogc
a
nlammaon.
ransormed
Aoug
sen
ncude:
anbodes,
ces,
ep
dferen
by
angen-presenng
smuaon
T
c yoknes
nlammaor y
by
and
mcrobes,
produce
acvae
medaed
by
adapve
produce
and
ma-
ympoc yes
are
(ence,
Structure
ence,
creaed
durng
Virus:
nlammaon. CD8+ c yooxc T ympoc yes (CTLs) k neced
o
spe-
os
secree
a
ces
ces
n
major
smuae
ses
(dam-
specazed
ces
and
moecuar
ces
reacon
recepor
presence
angens
acvaon,
mcrobes,
compemen
genes
marker
o)
mecansms
Humora
B
ese
(adap
56
dspayed
repea
pagoc yosed
are
2).
E ac
T
hese
rggered
major
hese
angens.
dversy
hus,
53
54
Immunodeficiencies,
mmunty
angens
Two
ereny
recepors
ces.
damaged
Caper
poweru
express
reabe
rom
by
Foowng
possess
umor
s
Allografts,
58
requre
ons.
deense
ympocyes,
ey
rom
ympoc yes.
angen-recepor
genes
acvaed
mmuny).
ces
o
53
Transplantation,
Disorders,
HYPERSENSITIVITY rearrangemens
Allografts,
Solid-Organ
59
proen
and
ympo-
nrnsc
(paogen-assocaed
[DAMPs]).
recepors
progeny
T
as
o
dversy.
reeased
more
and
suc
o
ces,
possess
producs
nlammaon
s
dverse
cona
and
paerns
T
dendrc
aso
recepors
subsances
acue
and
ypes
recepors
ave
many
mmunty
unque
express
angen
by
ce
producs
and
and
medaed
and
oer
moecuar
mmuny
Adaptve
cc
e
[PAMPs])
responses
ces
specc
age-assocaed
neurops,
and
mcroba
unke
paogen
paerns
ces,
of
Immunodeficiency
Cycle,
C e-medated
by
(ence, nnate). he prncpa ces o nnae mmuny are myeod ces,
ncudng
Stem
(Congenital)
Amyloidosis,
51
proecs
mecansms:
Organ
Acquired Immunodeficiency Syndrome, 58
(SLE),
(Scleroderma),
Syndrome,
mmune
ypes
Erythematosus
49
to
Rejection
Immunodeficiency
Primary
Autoimmunity,
of
Hematopoietic
Autoimmune Diseases, 49
Mechanisms
Responses
Mechanisms
•
senszed,
reactons.
conro,
may
R eactons
dseases
aer,
gens,
be
and
caused
aganst
ey
njurous
are
by
sef
cause
ndvduas
and
so
mmune
Hypersensvy
ereore
are
mporan
reacons
o
antgens
are
are
ree
normay
resus
end
wen
be
caed
probems.
ypes
o
As
er
yper-
cronc
o
we
sa
own
se-oerance
and
hese
angens.
auommuny,
dseases.
oeran
are
o
cnca
man
caed
autommune
auommuny
reacons
dseases
and
e
dscuss
(se )
breaks
an-
down.
41
42
CHAPTER
Table
4.1
Diseases
4
Hypersensitivity
Type
(type
I)
of
Immune
System
Mechanisms
Production
hypersensitivity
the
Reactions
Immune
Immediate
of
of
IgE
histamine
cells;
later
antibody
and
other
→
immediate
mediators
recruitment
of
release
from
Histopathologic
Lesions
Vascular
edema,
mast
inflammatory
dilation,
muscle
cells
contraction,
production,
tissue
Prototypical
smooth
Disorders
Anaphylaxis;
mucus
asthma
allergies;
(atopic
bronchial
forms)
injury,
inflammation
Antibody-mediated
(type
II)
Production
hypersen-
target
sitivity
of
of
cell
target
IgG,
or
cell
receptors;
IgM
tissue
by
→
→
binds
to
antigen
phagocytosis
activated
recruitment
or
complement
of
on
Phagocytosis
lysis
or
cells;
Fc
diseases,
leukocytes
and
lysis
inflammation;
ments
functional
without
cell
of
in
Autoimmune
some
hemolytic
Goodpasture
anemia;
syndrome
derange-
or
tissue
injury
Immune
complex–
mediated
(type
Deposition
III)
→
hypersensitivity
of
leukocytes
receptors
toxic
Cell-mediated
(type
IV)
Ig,
•
→
→
complement
release
of
complexes
recruitment
products
enzymes
and
Inflammation,
of
and
litis
an
aganst
abnorma
neous
mmune
E x cessve
y
T
lymphocytes
→
cytokines,
inflammation
activation;
(2)
c u oss,
o
e
resp ons e
b owe
he
reacon
T
(1)
release
and
cangeaby,
maon.
of
Perivascular
edema;
cytotoxicity
cell
cellular
infiltrates;
granuloma
Contact
formation;
erythematosus;
of
serum
glomerulone-
sickness;
dermatitis;
sclerosis;
destruction
mcrob e
e
ey
c aus e
oug
o
w c
are
no
be
and
Arthus
type
1
multiple
diabetes;
tuberculosis
p ers sen
cua-
s
e
suc
nor ma
as
e
ub er-
m mune
In am maor y
re ac ons
mmune
ag ans
ce s
w en
synonymous.
I
s
requeny
assocaed
w
antibodies
are
oten
used
Hypersensvy
caused
by
mcrobes
and
oer
auommuny,
envronmena
bu
agens.
ner-
reers
some
auommune
svy,
suc
wou
as
reacons
depeon
accompanyng
o
do
no
red
ave
ces
a
and
componen
paees
by
o
an
aso
that
cells,
angens
based
on
hs
the
gens
are
reac
of
casscaon
nsms
and
(type
I)
mmunogobun
by
are
and
because
cnca
eac
eaures
ypersenstvty
E
(IgE)
medaors
s
eary
e
by
mas
ype
as
(Tabe
o
•
armess
be
ew
Actvaton
ypes
smuaes
dsnc
rgger
nlammaon,
Immune
or
on
ces
ces
s
nduce
compex–medated
n
uncona
(type
III)
and
•
desroy
ces,
s
caused
ses
and
ssues
and
ce–medated
ces,
wc
desroy
os
ec
(type
nduce
ces.
cronc
ypersenstvty
nlammaon,
s
or
caused
CD8+
T
by
IgE
sensitize
nsec
e
bu
srong
dea.
and
n
some
aergc
(ae-pase)
are
mos
suc
an-
sysem
does
ndvduas,
a
propensy
smoo
and
(were
mmune
reacons
he
ypca
venoms,
socees
can
o
o
deveop
reacon
musce
ead
nlammaor y
sg-
ese
consss
response,
no
ese
o
an
wc
response
over
4.1).
mmedae
ceuar
ypersensvy
responses
(Fg.
reacons
oow
a
4.2).
by
CD4+
ces,
T
wc
ces
srong
and
and
IL-5
IL-13
IL-5,
roes
specc
of
responses
IL-4,
negra
soype.
producon
h2
or
n
e
and
on
anbody.
some
IL-13,
o
ac
nd-
h2
on
ces
a
and
e
are
ces
severa
ypersensvy.
produce
eosnops
epea
Aopc
angens.
wc
mmedae
aergen
acvaes
acs
IgE
o
IgE
IL-4
mmu-
recrued
smuaes
o
mucus
IgE
Te
es e
of
ma s
re cepor
a erg c
s
ce s
re cepor
s
key
a
p or on
express e d
ce s
ce s
anbody.
Fc
o cc ur
mas
Mas
IgE
e
a s o
re ac ons
re ac ons.
by
or
n
are
bnd
on
ssues
e
IgE
Mas
o
e
bo o d
and
maj or
and
ce s
ε
ce
n
e
yp e
on
a
can
b as op s,
no
re an
express
e av y
bu
crc u -
nvove d
er
sur-
aces.
•
nlammaon.
IV)
ec
sower
o
ces
S ensz aon
n
by
compexes o anbodes and angens a become deposed n ves-
T
B
reacon,
a on,
abnormaes.
ypersenstvty
and
angens,
he
cyoknes
g -a n y
ssues
and
secreon.
and
rggered
ces.
or
a
2
w
nogobun
meca-
e
h2
of
e
b e c aus e
angens
caused
mediators.
ndvduas,
vascuar
(Fg.
Mos
make
o
arge
atopy.
by
ours
oods,
even
mnues)
sequence
a
o
mos
and
caed
oowed
nex
Antbody-medated (type II) ypersenstvty s caused by anbodes
bnd
of
ndusrazed
angens
morbdy
s
In
n
envronmena
(wn
ce
types
4.1).
by
release
is
antigens
ypersen-
major
Inlammaon
allergy,
may
auoanbodes
four
called
Conversey,
reaction.
caused
anbodes.
reeased
into
immune
the
areas
abundan).
vduas
classied
adaptive
useu
paoogc
Immedate
many
s
the
to
also
environmental
envronmen,
urban
agans
ncan
may
e
n
normay
nlammaon.
reactions
nature
recognize
leading
n
requen
secree
Hypersensitivity
Hypersensitivity
reaction,
Aerges, e mos common mmunoogc dseases, are reacons o
reacons
d ee c ve.
autommunty
I)
inammatory
mast
and
by
This
yp ers ens v -
njur y.
c aus e d
a
drugs.
c as es ,
ssue
s
(Type
wc
armess
wc
m crob es
ac vae
are
aerg y,
normay
c aus e
s ome
o
may
me can sms
ypersenstvty
bu
n
and
a s o
agans
unusu a y
b e comes
are
cemcas
sysem,
ncude
and
sensvy,
mc robes
d eens e
s
b ac er a,
antgens
sereoypc
•
lupus
forms
reaction
Pathogeness.
•
some
other
mmunoogcay medaed ssue reacon a s domnaed by nlam-
•
Systemic
phritis;
macrophage
cell–mediated
common
conac
agans
mmune
proe c ve
and
aganst
A oug
ds e as es
erms
agans
subsances,
e
s e
commens a
nor ma
envronmenta
reacon
reac tons
re ac ons.
unc on
•
vascu-
necrosis)
Fc
Immediate
Reactons
envronmena
be
necrotizing
(fibrinoid
Immunoglobulin.
s
•
by
activation
molecules
Activated
hypersensitivity
antigen–antibody
complement
Acvaon
of
mas
ces
and
reease
of
medaors.
Wen
e
angen
s renroduced, bnds o e IgE, us cross-nkng e assocaed
Fc
o
recepors,
e
wc
secreon
o
n
urn
ransm
medaors
rom
nraceuar
e
mas
ces.
sgnas
a
ead
CHAPTER
Immediate
Diseases
4
of
the
Immune
System
43
Late-
reaction
phase
reaction
Allergen
exposure
Mast
cells
snoitatsefinam
Vascular
lacinilC
Eosinophils congestion
Edema
B
0
1
A
Hours
after
4
allergen
Fig.
ate
4.1
8
exposure
and
in
a
late-phase
cells.
C
20
hypersensitivity.
smooth
muscle
previously
Morphology
The
16
exposure
Immediate
vascular
(B)
12
of
the
(Micrographs
sensitized
immediate
reaction
is
(A)
Kinetics
reaction
Dr.
an
individual),
reaction
characterized
courtesy
to
Daniel
by
is
of
the
immediate
allergen
develops
and
late-phase
the
characterized
an
inflammatory
Friend,
Department
by
and
minutes
reaction
rich
in
Pathology,
reactions.
after
develops
vasodilation,
infiltrate
of
late-phase
within
2
to
congestion,
eosinophils,
Brigham
and
The
immedi-
challenge
24
(allergen
hours
and
later.
edema.
neutrophils,
Women’s
(C)
and
T
Hospital,
Boston.)
hree
groups
o
medaors
are
mporan
n
mmedae
ypersens-
Morphology. vy
s
•
he
Vasoactve
amnes,
many
stamne,
are
sored
n
mas
ce
ypcay
ues
and
rapdy
reeased
upon
mas
ce
degranuaon.
rapd
vasodaon
causes
smoo
and
ncreased
vascuar
rggered
permeaby
musces
o
conrac.
Cemoacc
acors
and
eases
are
generae
aso
D
)
s
e
mos
paway
as
4
as
and
I
ypersensvy
va on.
4
are
w c
mmune
o
vduas
mos
I
re cr u
IL-4
o
asma,
Caper
causes
vasoacve
s e cree d
ne cross
ac vae
I L- 5,
ave
2.
Prosagan-
nense
he
and
are
mu-
generaed
o ow ng
ac or
by
e
bronco-
eukorenes
spasmogenc
mas
( T NF)
eu ko c yes
w c
o
and
abnormay
o
n
ese
amp y
medaors
ypersensvy.
reacons
acors
exposure
o
mmedae
rggered
a
may
be
e
ony
secreon
o
manesaons.
ere
may
be
sgncan
nlammaor y
bronca
nraes
n
gand
yperropy,
bronca
pugs
a
obsruc
e
umens
(see
Caper
was,
and
10).
aso
Cln cal
s e ver y
Feature s.
rom
(a erg c
cronc
s
e
rn s),
ds e as es
o c a ze d
e
sk n
Imme d ae
m d
o
w en
e
as
o
ves
s ome mes
bronc a
an gen
con ac )
Sysem c
yp ers ens v y
nus ance
s er ous ,
suc
(o ow ng
nges on).
n
e
e
ce
and
ac -
cemo -
ae-pas e
T 2-n ae d
In
anapy axs,
cng ,
s
or
e
re ac ons
( ur c ar a)
a a ,
as ma
con ne d
exp osure
and
by
sensve
accoun
no
cear
angens
accounng
angens
or
do
no
(caed
acvaon
are
nvove
manes-
some
ncude
cdood.
suc
h2
as
ces
aerg y),
nd-
gnored
reacons,
smu,
varous
e
wy
aopy
nonatopc
by
or
a
durng
ypersensvy
and
cases
o
o
s
nonangenc
exercse,
ese
I
n
genec
Tweny
especay
may
IgE.
mas
nonmmune
I
ces
smu.
by
Te
ac ue
(Tabe
o
a
o
proen
and
range
ay
Te
p ar c u ar
an gens
and
re ac on
se,
rac
n
e ver
anapy ax s
4.2).
gas rones na
p a en
w
may
o
by
n
suc
as
(o ow ng
(e. g . ,
mme d ae
n
prog ress
o
n
bee
e
by
pressu re
crc u aor y
s ens ze d
by
os ,
proound
L ar y nge a
c aus ng
en re
vom ng ,
a
bronco c ons r c on
muc us .
upp er
e d ema
ar way
g as ro nes na
ab d om na
ner ven on ,
bo o d
o
o
n
o owe d
pu monar y
bre a ng
resu an
a
exp osure
app e ar,
yp ers e cre on
mus c u aure
a
e
er y ema
c aus e d
e
w
W ou
vas o d a on
m nues
sk n
d c u y
a e c e d,
d ar re a.
ere
may
( anapy ac c
c o ap s e
and
rac
cramps ,
be
and
s ysem c
so ck) ,
de a
and
w n
mnues.
Tre a m e n
empera-
or
exacerb ae
be
and
d c u y
accenu ae d
obs r uc on.
e
w n
ur c ar a,
respraor y
may
many
and
exremes
beeved
and
njurous
he
30%
are
and
umor
and
acons
mmedae
deveop
samne
produce
eukotrenes,
and
secreon.
poen
and
o
re ac on.
peope.
asma,
e
ncu d e
and
suscepby
percen
are
and
acd
medaor
ces.
mucous
n
by
venom) or dr ugs (e.g . , p en c n) may resu n sysem c anapy ax s.
combned
aons
mas
ncreased
sy n esze d
Tes e
re ac on,
he
LTD
n
descrbed
excessve
acors.
aracdonc
abundan
ssues
componens
known.
Cy toknes
k nes,
we
damage
prostagandns
nlammaon,
2
may
nlammaor y
membrane
spasm,
agens
are
and
cycooxygenase
LTC
s
n
aer
compemen
ncudng
rom
(PGD
2
he
ceave
cemoacc
acons
dn
and
medators,
syneszed
pe
reeased.
knns
addona
Lpd
ure
ype
pro-
mucous
mos
o
and
and
eosnop-rc
•
appearance
C ongeson
Hsamne
In causes
unmpressve.
gran-
mucus
•
soogc
reacons:
a c ng
are
e
or
es e
a c ons
an s am n e s ,
n e p r n e
( o
o
c on d ons
v ar ou s
c or c o s e ro d s
c or re c
e
re e s
m e d a or s .
( o
pre c pou s
on
b o c k ng
C om m on y
re a
d rop
or
c ou n e r-
us e d
dr ugs
n am m a on ) ,
n
b o o d
e p -
pre s s u re
n
44
CHAPTER
Allergen
Diseases
4
(e.g.,
of
the
Immune
System
pollen)
Table
4.2
Immediate
Clinical
Syndrome
Anaphylaxis
caused
Dendritic
Hypersensitivity
(Allergic)
Disorders
lining
ot
erusopxE
negrella
Mucosal
by
(may
Clinical
be
Fall
drugs,
in
and
blood
vascular
Pathologic
pressure
dilation;
Manifestations
(shock)
airway
caused
by
obstruction
due
cell bee
sting,
Bronchial
food)
to
asthma
laryngeal
Airway
edema
obstruction
caused
by
bronchial
Naive smooth
T
and
phase
Allergic
rhinitis,
sinusitis
cells
class
of
and
T
caused
inflamma-
by
late-
mucus
airways
secretion;
and
inflammation
of
sinuses
2
fever)
T
2
H
B B
upper
injury
reaction
Increased
(hay
tissue
H
IgE
switching
in
hyperactivity;
cell tion
Activation
muscle
Food
allergies
Increased
peristalsis
due
to
contraction
of
cell cell
cells
intestinal
and
muscles,
resulting
in
vomiting
diarrhea
IgE-secreting Production
of
IgE
IgE plasma
cell
Antibody-Mediated
Antibody-mediated
by
antibodies,
(Type
(type
usually
II)
IgG
II)
Hypersensitivity
hypersensitivity
or
IgM
disorders
autoantibodies,
are
directed
caused
against
FcεRI
target Binding
of
IgE
Mast FcεRI
on
mast
antigens
surface
of
cells
or
other
tissue
components.
cells
membranes
exogenous
o
be
he
or
angens
n
e
or
may
(e.g.,
oer
responsbe.
be
exraceuar
angens
mcroba
may
a
moecues
or
drug
angens
he
norma
marx,
ey
meaboe).
a
o
ce
be
Rarey,
cross-reac
mecansms
nrnsc
may
w
njur y
ce
anbodes
os
n
o
adsorbed
s
angens
orm
o
exposure
ypersensvy to
the
cell
Pathogeness.
Repeat
on
to
are
e
oowng:
allergen
•
Pagocytoss:
(suc
as
red
Anbodes
ces
or
compemen-medaed
mosy
Activation
cell;
of
mast
release
cnca
emnaed
bene
n
may
paees)
n
coa
and
desrucon.
e
speen,
(opsonze)
arge
em
Opsonzed
expanng
anbody-medaed
ces
pagocyoss
bood
wy
dseases
crcuang
or
eemens
spenecomy
marked
by
ow
or
are
s
o
bood
of
couns. mediators
•
Inlammaton: Anbodes a are deposed n exraceuar ssues
bnd
eukocye
Fc
recepors
or
acvae
compemen
(descrbed
Mediators
aer), bo resung n e recrumen and acvaon o eukocyes
(neurops
Vasoactive
•
amines,
and
macropages)
and
acue
nlammaon.
Ceuar dysfuncton: Anbodes can aso cause ceuar dysuncon
Cytokines lipid
mediators
wen
o
ey
ces,
ona Immediate
hypersensitivity
Late
phase
or
repeat
(minutes
exposure
to
after
(2–24
allergen)
hours
exposure
4.2
diate
The
sequence
hypersensitivity
allergen,
which
of
events
reactions
stimulates
in
are
Th2
immediate
initiated
cells
and
to
the
III
orms
IgE
binds
to
Fc
receptors
introduction
immunoglobulin
(Fc εRI)
on
mast
E
cells,
of
(IgE)
and
and
exposure
to
the
allergen
activates
the
mast
an
cells
that
are
responsible
for
the
pathologic
an - Ig E
er
e
o
A n b o d e s
n b
a
are
c d o o d
e
re e ve
o
re c e pors
E ar y
re du c e s
an d
an b o dy
re a c on .
s.
or
recepors
moecues,
ssue
on
e
surace
producng
unc-
njur y.
to
pay
of
bre
an
essena
dscusson
o
roe
n
ype
compemen
II
and
acva-
oows.
and
Functions
complement
system
of
Complement
consists
of
several
circulating
and
mem-
subse-
secrete
reactions
a
proteins
that
play
important
roles
in
host
defense,
as
well
as
one
o
the
inammation
and
tissue
injury
in
immunologic
diseases.
immedi-
are
ree
paways
o
compemen
acvaon,
ony
hypersensitivity.
an apy a x s ,
or
ce
proens
ypersensvy,
uncon
here ate
compemen
o
Activation
in mediators
nb
pro-
brane quent
wou
or
essena
Imme-
The
duction.
acvae
depee
repeat
allergen)
hypersensitivity.
by
and
and
reaction
after
on
Fig.
o
o
decences
Because reaction
bnd
bnd
s
e
b o ck
us e d
o
e x p o s u re
ncdence
m e c an s m
bron c o s p a s m ) ,
n o
o
e
an
o
u n d e rs o o d .
as ma
a e rge n
a
an d ,
m ore
n a or
c y ok n e s
re a
o
a e rg y
pr m ar y
a ge n
I L- 4 ,
an d
( e. g . ,
a e r
o
re c e n y,
e
I L- 5 ,
an d
aop c
e,
I L- 1 3
d e r m a -
p e anu
n
a e rg c
exrac)
a ou g
wc
nvoves
natve
patway
anbodes
s
acvaed
compemen
proens.
compemen
proens
orm
compexes
(Fg.
w
he
o
by
4.4).
pyogenecay
mcroba
cassca
anbodes
angens.
he
hs
moecues
patway
a
s
are
s
a
acvaed
deposed
mporan
n
oder
saby
by
on
ater-
bnd
bndng
suraces
adapve
o
and
mmuny
and s e ony paway a parcpaes n e anbody-medaed (ype
II)
and
mmune
compex–medaed
(ype
III)
orms
o
ypersensvy.
he ectn patway s acvaed by a pasma ecn a bnds o mcroba
CHAPTER
A
Opsonization
and
Diseases
4
of
the
Immune
System
45
phagocytosis
Phagocytosed
Opsonized cell
cell
C3b
C3b
Phagocyte
receptor Phagocytosis
Complement
B
Complement-
and
activation
Fc
receptor–mediated
inflammation
Fc
receptor
Neutrophil
Complement enzymes,
by
products reactive
(C5a,
oxygen
C3a) intermediates
Tissue
C
antigen
Antibody-mediated
Complement
cellular
Inflammation
activation
and
tissue
injury
dysfunction
Acetylcholine Nerve
Antibody
ending (ACh)
against
TSH
TSH
receptor
receptor
Antibody
Thyroid
to ACh
ACh
epithelial
receptor receptor
cell
Muscle
Thyroid Antibody
inhibits
neurotransmitter
Fig.
4.3
Mechanisms
plement
components
receptors
normal
of
function
carboydraes.
proeoyc
o
e
C3b,
mos
a
uncons
ceavage
o
producs.
abundan
ree
compemen
proen,
C3,
o
examples,
ead
o
a
to
the
antibodies
the
varous
ragmen,
a
proeoyc
samne
he
a
producs
rom
ermna
arge
oes
ceaves
n
pd
aby,
C5a
n
e
acvaon
a
o
and
we
C3a,
as
eads
s
wc
oer
o
osmoc
acvaon
by
ead
o
e
e
compex,
yss
severa
damage
durng
compemen
Among
smuae
aack
coaera
componen
pronlammaor y
acvaon
conroed
preven
ese
componens.
membrane
and
compemen
decences
as
compemen
membranes
proens
unresraned
compemen
ces,
canne,
Compemen
secreed
are
mas
seps
proen
aer
a
o
e
ead
o
a
oer
reease
o
acves.
ormaon
wc
o
creaes
ces.
norma
ces
deense.
o
ce
caed
Paroxysma
nocturna
emogobnura
o
ere
excessve
s
e
red
ces
bood
o
an
acqured
decency
o
an
enzyme
nvoved
C3
C1
ces
o
Fc
the
impair
hormone
are
er
factor,
ceaves
durng
seep,
acvy
a
o
C3.
and
ce
rom
yss
e
eary
serne
o
e
o
ces.
ncreases
nocurna
resus
rom
ms
s
e
or-
reguaor,
membrane
or
he
aack
urnar y
e
naure
o
a
pH
e
nered
many
excre-
suscepby
wen
nbor
proens,
o
compemen-med-
accounng
red
proease
compemen
normay
absence
sensve
was,
ence
e
ormaon
ysed
angoedema
pasma
wc
In
especay
n
reeased
Heredtary
nbor,
eoyc
a
breakdown
bood
decreases
and
ens,
and
accumuaon
Predc-
njur y
(PNH)
n
receptor
compemen-medaed
breakdown.
o
acceeratng
enzyme
emogobn
wc
e
red
ce
decency
ms
C1.
o
o
e
pro-
Decency
o
serous
s
ncrease
n
eaure
e
vascuar
skn,
because
permeaby
gasronesna
coud
ead
o
and
cause
rac,
ar way
and
epsodes
ar ynx
o
(e
lud
mos
obsrucon).
and Features.
In
many
auommune
dseases,
e
cnca
caused probems
by
to
disturb
thyroid-stimulating
decay
maon
Clncal
nlammaon.
com-
binding
antibodies
(ACh)
and
hormone
s nbor eads o excessve producon o numerous vasoacve pro-
ce-assocaed
o
norma
reguaors
anbody
reguaor
because
s
without
antibodies
antibody
acetylcholine
against
yss
aso
by
by
Antireceptor
o
C3b
cells
receptor
disease.
ceavage
o
antibodies
and
(C)
on
pagocyes.
ses
products.
of
induced
aed
on
or
by
e
generae
(mcrobes
gravis,
Graves
medaed
paways
suraces
in
breakdown
Opsonization
Inflammation
ors
expressed
nearby
cells
(A)
(B)
bndng). C3b opsonzes ces or pagocyoss by bndng o C3b recep-
are
on
are
these
myasthenia
thyroid
diseases.
phagocytes.
complement
In
in
by
stimulates
Red
proease
deposed
receptors.
compemen
A
by
transmission
activate
Antibody
compex.
a
s
he
receptor
of
ingestion
and
hormones
of
receptor
antibody-mediated
and
leukocytes
neuromuscular
(TSH)
of
binding
to
syness
o
are
caused
by
auoanbodes
by
nlammaon
(Tabe
4.3).
he
paoog y
a may
be
domnaed
(as
n
anbody-medaed
46
CHAPTER
Diseases
4
of
the
Immune
System
EFFECTOR
C5a,
C3a:
FUNCTIONS
Inflammation
Alternative Microbe pathway
Recruitment
activation
of
and
Destruction
leukocytes
by
C3b:
of
microbes
leukocytes
Phagocytosis
C3a
C3b
Classical
C3b pathway
C3b
is
deposited Recognition
Antibody on
of
bound
C3b
Phagocytosis
microbe by
phagocyte
C3b
receptor
of
MAC:
Lysis
microbe
of
Lectin microbe
pathway
For mation
Mannose
binding
membrane
lectin
complex
Fig.
4.4
ment
of
C3b.
tein
of
Pathways
system
C3b
4.3
called
polymerized
duced
at
of
complement
early
initiates
complex
complement
Table
(the
C9
the
the
late
are
steps
Antibody-Mediated
may
activation
be
steps
membrane
molecules
activation
different
steps)
that
the
are
and
initiated
of
by
functions
three
complement
attack
causes
complex
lysis
of
(MAC)
of
distinct
complement.
pathways,
activation,
(MAC),
thin-walled
inflammation-inducing
C3a
of
attack
culminating
which
is
a
microbes.
and
all
C5a.
The
activation
of
which
in
the
lead
formation
transmembrane
Peptide
The
of
to
of
functions
comple-
production
a
channel
by-products
principal
the
the
multipro-
composed
released
of
during
proteins
pro-
shown.
Diseases
Clinicopathologic
Disease
Target
Autoimmune
hemolytic
anemia
Red
Antigen
cell
Mechanisms
membrane
proteins
Opsonization
of
Disease
Manifestations
and
phagocytosis
of
red
blood
and
phagocytosis
of
platelets
Hemolysis,
anemia
cells
Autoimmune
thrombocytopenic
purpura
Platelet
Illa
Pemphigus
vulgaris
membrane
Proteins
in
intercellular
epidermal
Vasculitis
caused
by
ANCA
proteins
(Gpllb:
Opsonization
Bleeding
integrin)
Neutrophil
sumably
cells
junctions
of
(desmogleins)
granule
proteins,
released
from
Antibody-mediated
disruption
pre-
Neutrophil
of
activation
intercellular
degranulation
of
proteases,
Skin
vesicles
(bullae)
adhesions
and
inflammation
Vasculitis
activated
neutrophils
Goodpasture
syndrome
Protein
in
kidney
Acute
rheumatic
fever
basement
glomeruli
Streptococcal
body
cell
membranes
and
wall
cross-reacts
lung
antigen;
with
of
alveoli
anti-
Complement-
and
Fc
receptor–mediated
inflammation
Inflammation,
Nephritis,
lung
hemor-
rhage
macrophage
activation
Myocarditis,
arthritis
myocardial
antigen
Myasthenia
gravis
Acetylcholine
receptor
Antibody
inhibits
acetylcholine
down-modulates
Graves
disease
(hyperthyroid-
TSH
receptor
Antibody-mediated
ism)
Pernicious
stimulation
Muscle
weakness,
paralysis
of
TSH
Hyperthyroidism
receptors
anemia
Intrinsic
factor
of
gastric
parietal
cells
ANCA,
binding,
receptors
Antineutrophil
cytoplasmic
antibodies;
TSH,
Neutralization
absorption
thyroid-stimulating
hormone.
of
of
intrinsic
vitamin
factor,
B
12
decreased
Abnormal
anemia
erythropoiesis,
CHAPTER
Antigen
Immune
in
Complex
Diseases
4
Table
Formation
4.4
of
the
Immune
Immune
Complex
System
47
Diseases
circulation
Clinicopathologic
Disease
B
Antigen
Involved
Manifestations
cell
Systemic
lupus
Nuclear
erythematosus
antigens
lating
or
(circu-
“planted”
Nephritis,
in
kidney)
Poststreptococcal
skin
lesions,
arthritis,
others
Streptococcal
cell
wall
Nephritis
Plasma
Free
glomerulone-
antigen(s);
phritis
“planted”
may
be
cell
antibody
in
basement
Polyarteritis
Hepatitis
nodosa
in
B
some
glomerular
membrane
virus
antigens
Systemic
vasculitis
cases
AntigenReactive
arthritis
Bacterial
antigens
(e.g.,
Acute
arthritis
Endothelium
antibody
Yersinia) complex
Serum
Immune
sickness
Various
Complex
proteins
foreign
Deposition
such
(e.g.,
serum
as
mocyte
Arthritis,
protein,
horse
vasculitis,
nephritis
antithy-
globulin)
Neutrophil
Arthus
reaction
Various
foreign
proteins
Cutaneous
(experimental)
Pathogeness.
n
anbody
Typcay,
excess
pagocyes
bu
vascu-
litis
and
are
paogenc
are
o
capabe
a
o
sze
mmune
suc
a
deposng
compexes
ey
n
avod
vesses.
are
produced
emnaon
Tssue
by
deposon
Complement
eads
o
compemen
acvaon
and
acue
nlammaon
(Fg.
4.5).
Antigen-
Consumpon
o
compemen
durng
e
acve
pase
o
e
dsease
antibody
complex
Immune
Complex–Mediated
Inflammation
Tissue
and
eads
o
o
decreased
dsease
serum
acvy.
eves
Serum
o
C3,
sckness
wc
s
a
can
be
sysemc
used
as
mmune
a
marker
compex
Injury
dsease
n
wc
a
snge
anbody
produced
Immune
compexes
acvae
n
arge
oer
orm
compemen,
n
and
dose
o
speces,
e
nduce
a
s
bood,
oregn
njeced
become
nlammaon.
angen,
no
an
suc
deposed
he
as
an
ndvdua.
Artus
n
ssues,
reacton
s
Platelet
an
aggregation
expermena
vascudes
(Caper
Morphology.
compex
he
njury
brnod
Wen
mode
o
cuaneous
acue
necross
o
deposed
a
resembes
uman
7).
prncpa
s
vascus
e
n
morpoogc
vascus,
vesse
e
manesaon
wc
wa
kdney,
may
and
e
be
o
mmune
assocaed
neuropc
compexes
w
nraon.
can
be
seen
Vasculitis
on
Neutrophil
lysosomal
mmunoluorescence
4.5
Immune
complex
disease.
The
sequential
phases
in
the
of
systemic
immune
granuar
deposs
complex–mediated
diseases
(type
III
and
compemen
and
on
eecron
o
mcroscopy
as
induc-
eecron-dense
tion
as
enzymes
mmunogobun
Fig.
mcroscopy
deposs
aong
e
gomeruar
basemen
membrane.
hyper-
sensitivity).
Clncal
gomeruoneprs),
(auommune
uncona
e
gravs,
moor
ransmsson,
smuae
agans
yrod
end
anema
paes
w
o
ceuar
ces
o
In
depeon
Graves
(TSH)
yrod
dsease).
(AC)
dsease,
c omp e xe s
n am m a on
aso
anbodes
recepor
ormones,
smuae
resung
c ap ar e s
o
j o n s
T e
T
(Type
III)
circulation
may
inammation.
(immune)
become
complexes
deposited
in
e
( ar r s ) ,
proo y p c
s e s
k dne ys
an d
u m an
( SL E ) ,
Cell-Mediated
T e
o
m mu n o o g c
ssu e
p a o o g c
d e p o s on
( c au s ng
b o o d
m mu n e
a ss o c ae d
o
ds e as es
d e p o s on
p c u re
o
s
c omp e xe s ,
ve ss e s
n
w
any
ssu e
ds e as e
p e rs se n
s
o
a c ue
y p c a y
g om e r u on e p r s ) ,
c omp e x
are
m mu n e
e
s y n ov u m
( v a s c u s ) .
s y se m c
an b o dy
upu s
re sp ons e s
types
of
(Type
T-cell
IV)
reactions
Hypersensitivity
are
capable
of
causing
tissue
injury
Hypersensitivity and
Antigen–antibody
4.4).
e
an d
auo an ge ns .
Two
Complex–Mediated
o
n
s y se m c
or m a on
( Tab e
e r y e m ao su s
o
Many
e
n
yperyrodsm.
Immune
w
In
recepors
can
Features.
a ss o c ae d
or
neuromuscuar
Anbodes
Graves
ormone
secree
ce
nb
weakness.
responses:
yrod-smuang
epea
and
aceycone
musces
musce
o
romboc yopena),
gravs
agans
skeea
resuan
efecs
and
(myasena
anbodes
excessve
e
secondar y
emoyc
derangemens
myasena
n
e
that
blood
are
formed
vessels
and
in
the
induce
disease:
(1)
delayed-type
duced
CD8+
hypersensitivity),
mainly
T
cells
cytokine-mediated
by
CD4+
(Fig.
4.6)
T
cells,
in
inammation
which
and
(2)
the
(also
cytokines
cytotoxicity,
called
are
pro-
mediated
by
48
CHAPTER
Diseases
4
Cytokine-mediated
of
the
Immune
System
inflammation
Inflammation
Cytokines + CD4
T
APC
cell
presenting
tissue
antigen Tissue
injury
Nor mal
tissue
A
T
cell–mediated
cytolysis
+
Cell
CD8
T
APC
killing
tissue
cell
and
injury
presenting
tissue
antigen
B
Fig.
4.6
injury
Mechanisms
and
disease
of
by
T
two
cell–mediated
mechanisms.
tissue
(A)
injury
(type
Inflammation
IV
hypersensitivity).
may
be
triggered
by
T
cells
may
cytokines
cause
tissue
produced
mainly
+
by
CD4
T
cells
in
which
tissue
injury
is
caused
by
activated
macrophages
and
inflammatory
cells.
(B)
Direct
+
killing
of
target
cells
is
mediated
by
CD8
cytotoxic
T
lymphocytes
(CTLs).
Pathogeness.
efecor
cay
ces,
n
APC,
Antigen-presenting
Cyokne-medaed
bu
cases
h17
were
ces
aso
cell.
ypersensvy
may
neurops
conrbue
are
s
o
promnen
a
reacon
e
n
o
reacon,
e
h1
espe-
nlammaor y
nrae. h1 ces secree cyoknes, many nereron-γ (IFN-γ), wc
are
responsbe
sensvy.
subsances
a
T
a
promoe
recru
ces
k
Clncal
A
B
4.7
Delayed-type
hypersensitivity
s
accumulation
(cuffing)
of
reaction
mononuclear
in
the
skin.
inflammatory
(A)
a
and
deposition.
perivascular
bodies.
Health
(B,
macrophages),
(B)
cellular
Courtesy
Sciences
with
associated
Immunoperoxidase
infiltrate
Dr.
Louis
University,
that
staining
marks
Picker,
dermal
reveals
prevousy
positively
Department
Portland.)
a
with
of
some
ypca
deveops
ssues,
ces
ces.
CD8+
nvoved
n
(Fg.
over
4.7).
1
ndvdua
o
I
2
(n
o
T
s
caed
days
medaors
cyooxcy,
ces
especay
s
ater
conras
yper-
produce
cyoknes
aso
nlammaor y
conac-senszng
manesaon
and
secree
ce-medaed
ypersensvy,
o
senszed
are
damage
h17
deayed-ype
macropages
a
CD8+
produce
reacons
oowng
vrus
agens.
orm
o
ypersens-
deayed-ype
an
w
angen
yper-
caenge
and
anti-CD4
hs
me
ag
s
due
o
e
mupe
mmedae
seps
nvoved
yper-
n
e
(lym-
ncudng
e
capure,
processng,
and
presenaon
o
e
fibrin
predominantly
Pathology,
arge
and
nlammaon
because
In
o
acvaed)
and
Acvaed
monocyes.
IFN-γ,
he
manesaons
Perivas-
cells
edema
and
exposure
Features.
reacon, phocytes
e
(casscay
mcrobes
deayed-ype
cronc
sensvy). cular
o
angen-expressng
and
sensvy
n Fig.
desroy
noaby
resembng
necons
many
nlammaon.
neurops
cyoknes,
vy
or
IFN-γ–acvaed
anti-
Oregon
angen,
angen
seen
n
acvaon
caenge,
many
anagonss
prognoss
o
TNF
s
T
and
ces,
erapeuc
paens
gy
mgraon
producon
mmunoogc
as
or
o
efecve
dseases
agens
w
o
ese
n
e
o
cyoknes.
(T abe
as
efecor
4.5).
T
hs
he
revouonzed
dsorders.
reamen
For
o
ces
ype
o
o
adven
e
exampe,
reumaod
e
se
reacon
o
o
s
cyokne
reamen
and
neurazaon
arrs.
CHAPTER
Table
4.5
T
Cell–Mediated
Disease
Specificity
Rheumatoid
Collagen
arthritis
Hypersensitivity
of
Pathogenic
T
self
of
the
Immune
Cells
Principal
Mechanisms
Inflammation
proteins
cytokines;
mediated
role
of
of
Tissue
by
Th17
antibodies
Injury
(and
and
Clinicopathologic
Th1?)
Chronic
immune
sclerosis
Protein
antigens
myelin
basic
in
myelin
(e.g.,
Inflammation
protein)
cytokines,
articular
mediated
myelin
by
Th1
and
destruction
by
Th17
1
diabetes
Antigens
of
pancreatic
islet
β
49
cells
T
cell–mediated
mellitus
islet
cells
by
inflammation,
cytotoxic
destruction
of
with
in
central
with
mation;
paralysis
of
nervous
perivascular
(chronic
islets),
synovial
destruction
system
Insulitis
lymphocytes
Manifestations
cartilage
Demyelination
activated
macrophages
Type
arthritis
inflammation,
complexes
Multiple
System
Diseases
(postulated)
Citrullinated
Diseases
4
inflam-
inflammation
destruction
of
β
in
cells;
diabetes
Inflammatory
bowel
Enteric
disease
bacteria;
self
antigens
Inflammation
(unknown)
Psoriasis
Self
antigen
mediated
by
Th1
and
Th17
Chronic
cytokines
(unknown)
Inflammation
intestinal
inflammation,
obstruction
mediated
mainly
mediated
by
by
Th17
Cutaneous
plaques
cytokines
Contact
sensitivity
Various
environmental
urushiol
from
chemicals
poison
ivy,
(e.g.,
Inflammation
therapeutic
Th1
(and
Th17?)
Epidermal
cytokines
mation,
drugs)
Examples
of
human
T
diseases
are
rash
inflam-
and
listed.
DISEASES
Genetic
Autoimmune
dermal
skin
blisters
cell–mediated
AUTOIMMUNE
necrosis,
causing
diseases
are
caused
by
adaptive
immune
Environmental
triggers
responses susceptibility
against
self
antigens. Infections,
I s es mae d a es e d s e as es a e c 1% o 5% o Weser n p opinflammation,
u a ons,
re as ons.
and
er
B as e d
auommune
on
nc d ence
e
ds e as es
sysemc
d s e as es
a
c aus e d
s e ems
nvove d
are
o
be
ssues
bro ad y
(summar ze d
nc re as ng ,
and
dv de d
n
Tabe
c n c a
no
4.6).
or
un k now n
organ -sp e c c
In
tissue
injur y
man es a ons ,
sysemc
and
ds e as es Susceptibility
are
by
mmune
compexes
and
auo an b o d es,
e genes
esons
pr ncp a y
o
nvove d
as
co agen
a e c
organs.
e
conne c ve
T ereore,
vas c u ar
d s e as es
es e
or
ssues
d s e as es
and
are
conne c ve
b o o d
o en
ssue
Tissue
vess es
reer re d
d s e as es,
o
Failure
e ven
of Activation
self-tolerance
oug
e
agans
mmunoog c
cons uens
Mechanisms
of
o
re ac ons
con ne c ve
are
ssue
no
or
sp e c c a y
b o o d
d re c e d
of
tissue
Autoimmunity Influx
Self-tolerance
against
self
in
T
and
B
lymphocytes
prevents
harmful
reactions
lymphocytes
tissues.
norma
of
self-reactive
into
he
APCs
vess es .
mmune
sysem
can
reac
o
an
enormous
dversy
tissues
o
Self-reactive
oregn angens bu does no recognze or respond o se angens. he lymphocytes
ack
e
o
reacvy
presence
agans
resus
one’s
rom
mecansms
o
s
e
own
a
caed
angen);
ssues
s
breakdown
o
toerance
e
caed
o
(mpyng
absence
o
a
ces
mmune
sef-toerance.
se-oerance,
e
responsveness
Because
we
rs
“oerae”
auommuny
dscuss
e
major
Activation
of
self-reactive
oerance.
lymphocytes
•
C entra
toerance.
(deeed)
(or
T
gens
beore
ces)
are
and
presen
S e-reacve
ey
bone
n
compee
marrow
ese
ympoc yes
er
(or
organs,
B
and
are
mauraon
ces).
wen
n
emnaed
e
Numerous
mmaure
ymus
se
an-
ympoc yes
w g-ainy recepors or ese angens encouner em, e
ces
de.
C enra
oerance
emnaes
many
poenay
Tissue
dangerous
injury:
autoimmune
se-reacve
maure
•
and
Reguatory
escape
ympoc yes
ener
T
perpera
ces.
deeon
bu
s
he
s
mperec,
and
some
o
ese
ssues.
response
prevened
by
o
Fig.
se-reacve
e
acons
o
ympocyes
reguaor y
T
a
ces
4.8
model
Postulated
of
genetic
n
perpera
ssues.
he
bes-dened
Tregs
are
CD4+
loci
express
e
ranscrpon
acor
Foxp3.
A
severe
afecng
many
organs
occurs
n
boys
wo
such
ner
of
muaons
n
e
X-nked
FOXP3
cell–mediated
susceptibility
maintenance
of
to
In
this
proposed
autoimmunity,
autoimmunity,
self-tolerance.
various
probably
Environmental
by
trig-
as
infections
lymphocytes
and
into
other
tissues
inflammatory
and
the
stimuli,
activation
of
promote
the
antigen-pre-
deeersenting
ous
the
confer
autoimmunity.
auommune influx
dsease
may
T
of
ces
gers,
a
mechanisms
organ-specific
influencing
(Tregs)
disease
ces
cells
(APCs)
gene. ing
in
tissue
injury.
and
subsequently
of
self-reactive
T
cells,
result-
50
CHAPTER
Table
4.6
Diseases
4
Organ-Specific
and
of
the
Systemic
Immune
System
common y
Autoimmune
Diseases
Organ-Specific
Diseases
Systemic
“o dds
p are d
ndv du a s
Mediated
by
hemolytic
anemia
Autoimmune
thrombocytopenia
Systemic
lupus
pernicious
atrophic
gastritis
a
an
ng
a
bu
e
HL A
do
o c us,
r sk
no
o
w
sp e c c
de veopng
n e r
a
a
HL A
a ees
ds e as e
a ee)
o
ess
com -
an
n
d eren
HL A
a
moe c u es
g ven
ds e as e
ds e as es.
HL A
Environmental
Factors
Environmental
factors
s
a e c s
a ee
rema ns
I
re as onab e
e
o
2
p osu ae
pres en a on
n uences
e
r sk
o
o
s e
d e veop -
un k now n .
of
participate
in
causing
autoimmunity
in
a
anemia
susceptible
host.
gravis
A Graves
s
( re a ve
w o
or
ow
p ar c u ar
genetically Myasthenia
100
var a on
an gens,
erythema-
tosus
Autoimmune
more
a
Antibodies
Autoimmune
o
ra os”
Diseases
o
Diseases
ncr mnae d
sow ng
nk
beween
necons
and
auommuny
as
been
posuaed
disease
based
Goodpasture
on
resus
rom
expermena
modes
and
because
o
e
ac
syndrome
a
necous
prodromes
somemes
precede
auommune
dseases
a
Diseases
Type
1
Mediated
by
T
Cells
n
diabetes
Multiple
Rheumatoid
sclerosis
Systemic
arthritis
sclerosis
paens.
and
In
(sclero-
I
may
overcome
e
addon
o
be
a
mcroba
norma
paogens
mecansms
necons,
e
o
dspay
acvae
mmune
ces
se-oerance.
o
ssue
angens
aso
may
be
b
aered
derma)
b
Sjögren
by
radaon
syndrome
angens Diseases
Postulated
Inflammatory
bowel
to
Be
diseases
a
varey
causes
a
o
ce
ec
envronmena
dea
and
paoogc
nsus.
may
ead
mmune
o
For
e
nsance,
uravoe
exposure
responses
(e.g.,
o
n
nucear
SLE;
see
Autoimmune aer).
Smokng
due
o
cemca
any
reason
s
a
rsk
acor
or
reumaod
arrs,
peraps
(Crohn
modcaon
o
se
angens.
Loca
ssue
njur y
or
c
disease,
ulcerative
colitis)
b
Primary
biliary
may
ead
o
e
reease
o
se
angens,
w
subsequen
b
cholangitis
Polyarteritis
nodosa
auommune
responses.
Many
auommune
dseases
are
more
com-
b
Autoimmune
(chronic
active)
hepatitis
Inflammatory
myopathies
mon
a
A
role
also
be
for
T
cells
involved
has
in
been
tissue
demonstrated
in
these
disorders,
but
antibodies
may
n
women
deveopmen
an
o
n
men,
suggesng
auommuny,
bu
a
e
ormones
underyng
nluence
mecansms
e
are
injury.
obscure. b
An
autoimmune
basis
of
these
disorders
is
suspected
but
not
established.
In
c
These
enteric
The
disorders
may
microbes,
features
of
result
from
autoimmunity,
many
of
excessive
or
these
a
immune
combination
diseases
have
of
responses
the
been
to
eases
summarized
in
Tables
and
oowng
a
afec
dscuss
and
seeced
usrae
auommune
mporan
ds-
aspecs
paogeness
and
manesaons
o
s
group
o
dsorders.
o
Oer
dseases
are
dscussed
n
reevan
capers.
Inbtor y receptors. S e-re ac ve y mpo c y es a ave maure d Systemic c an
a s o
be
p er pera
a
T
or y
us
w
nac vae d
ssues.
re cepors
and
ds c uss
es e
(a s o
n
re cog n on
e
c a e d
o
“ce ckp ons”
and
5,
o
s e
ur er
n
umors
bo ck ng
s
express
no aby
wo
e
s raeg y
name d
we
express on
or
s
n b-
As
Lupus
SLE
o
is
characterized
immune
cells
I
complexes,
and
s
resp ons es
aga ns
c ancer
ce s.
w
de veop
ce ckp o n
bo ckad e
or
Pre d c aby,
c anc er
s
bes
and
the
genes
he
factors
contribute
of
environmental
suscepby
envronmena
dspay
o
to
the
breakdown
autoimmunity,
insults
genes
acors,
and
ese
dseases
may
suc
responses
dverse
are
as
o
(Fig.
self-tolerance
including
susceptibility
4.8).
nluence
necons
se
of
n
women
erms
o
an
e
hallmark
antigens,
50%
of
cases),
ympocye
or
angens.
ssue
he
oerance,
njur y,
compex
may
and
aer
anbodes
compexes
svy).
er
genec
and
envronmena
and
damage
and
many
n
men
(∼10:1
rao)
and
ends
anbodes
a
are
produced.
of
SLE
including
is
autoantibodies
double-stranded
produced
DNA (present
nucleoproteins,
no
compeey
diseases
are
n
Anbodes
desrucon
bodes
em,
depos
orm
and
by
mmune
wc
may
ead
compexes
and
e
others.
reeased
kdneys
and
oer
bnd
and
opsonze
aso
o
pagocyes
compexes
o
w
a
a
n
(ype
II
usuay
serum
organs
angens,
(ype
bood
III
ces,
ypersensvy).
acvae
e
compemen
and
e
ypersen-
eadng
hese
o
an-
compemen
sys-
eves.
neracons
acors
n
e
eoog y
and
mecansms
o
SLE
are
no
esabsed,
auom-
pausbe
ypoess
s
e
oowng:
Exposure
o
uravoe
g
(a
undersood.
Susceptibility
Autoimmune
n
The
nuclear
about
known
Genetic
autoantibodies
m muno er apy
a mune
of
inammation
p a en s
Aoug beween
elicit
auom mun y.
development
and
which
common
undersood
he
Numerous
(SLE)
production
s mu a ng
in a s o
the
o occur n women o reproducve age. he paogeness o e dsease
against re ae d
by
tissues.
more
Pathogeness. mmune
Erythematosus
n
ac va on ,
resp ons es .
nduce
a
an gens
nac va on
y mpo c ye
mmu ne
a s o
em
s e
o
an gens
conbtors),
su
o
me can s ms
resp ond
a
C aper
re cepors,
o
a
PD-1,
es absng
up on
O ne
y mpo c yes
CTL A-4
e
we
organs
4.5 .
organ-specc
•
secons,
mupe
4.3,
e 4.4,
e
commensal
two.
multigenic,
meaning
that
rsk
ance
o
ance
causes
acor)
nucear
eads
o
ragmens
acvaon
o
apoposs
combned
o
varous
w
ympocyes
ces;
aure
specc
or
o
B
se
mproper
and
T
ce
nucear
cear-
oer-
angens.
polymor-
Hg-ainy anbodes produced agans ese angens orm mmune phisms
in
many
different
genes
are
associated
with
an
increased
or
compexes, decreased
risk
of
the
cyes. E xcep
or
s ome
rare
mend e an
c aus es
o
auommune
he
auommune
ds e as e
c an
be
a r bue d
o
a
s ng e
gene.
wc
p oy mor pc
are
endocyosed
genes
n ke d
o
auo mmun y,
by
ar
DNA
and
RNA
by
dendrc
smuae
acvae
ympocyes
Among
perssen e
nucear
ces
and
producon
o
B
ympo-
ype
I
ner-
ds e as e,
erons, no
wc
disease.
e
mos
auoanbody
producon.
and
APCs,
seng
up
a
cyce
o
CHAPTER
Diseases
4
anbodes
Morphology.
SLE
can
afec
vruay
any
organ.
he
esons
resu
rom
mmune
compex
deposon
cong,
vesses,
kdneys,
and
a
Bood
es,
vesses.
sma
he
An
areres,
arers
cronc
acue
sages,
o
areroes
brnod
vesses
System
pospopd–proen
51
o
e
anpospopd
compexes
anbody
nvoved
syndrome
Neuropsycarc
manesaons
(ncudng
(see
sezures,
skn:
necrozng
and
eads
orm
3).
psycoss,
•
o
Immune
n Caper
bood
bnd
the
mos n
caracersc
a
of
vascus
may
be
necross
undergo
brous
nvovng
presen
o
e
n
any
vesse
ckenng
capar-
ssue.
was.
w
ever
are
and
neuropay)
common.
compex
Md
and
sysemc
arrs
may
manesaons
occur
secondar y
suc
o
as
mmune
deposon.
In
umna
Systemic
Sclerosis
(Scleroderma)
narrowng. Systemic
•
Kdney.
Up
o
50%
o
SLE
paens
ave
cncay
of
rena
nvovemen,
dence
e
kdney
examned
vruay
by
(Suppemena
men
o
akes
a
number
deposon
o
orms,
mmune
a
eFg.
sows
ev-
mcroscopy
and
4.1).
Rena
nvove-
Pathogenes s.
poory
are
assocaed
w
and
e
gomeru.
Pro-
annucear
o
e
paoog y
(see
Caper
11).
reason
nraes
produce
and
seen
or
on
e
50%
e
vacuoar
ss
may
be
paens,
4.2).
In
or
a
maar
smar
Exposure
o
e
e
basa
derms,
ayer
juncon
eFg.
aso
may
e
n
be
nces
areas
epderms
paee
even,
n
brnod
necro-
n
aong
sows
e
deveopmen
e
o
e
e
presence
and
eoog y,
oten
and
by
brosis
o
o
conan
probroc
of
the
skin
and
walls
dsease
a
puzzng
sysem,
crcuang
e
h2
suc
o
nvoves
bood
afeced
reevan
s
known.
and
especay
sugges
angen
he
bu
s
nor
mmune
macropages
grow
endoea
eaure,
a
acor-β.
acvaon
bass
a
vesses,
skn
se
ransormng
evdence
conssen
n
ces
as
dsease
sma
auoanbodes,
nraes
neer
CD4+
w
s
s
abnormalities.
se-oerance
c yoknes
aggregaon
o
mmune
T-ce
bu
aure
vascular
s
and
aso
no
known. One ypoess saes a e vascuar dsease s e nang
edema
mcroscopy
or
Mcrovascuar
varabe
compemen
(Suppemena
seen
nvoved
o
s
w
s
sung
e
Immunoluorescence
and
ras
ere
Vascus
ras)
o
Hsoogcay,
mmunogobun
moepderma
bu
runk.
nlammaon.
promnen.
o
and
er yema.
eFg.
pervascuar
deposs
buerly
degeneraon
(Suppemena
and
o
(e
exremes
accenuaes
sow
ceeks
tract
anbodes,
auommune
o
nose
characterized
nerpay
brobass.
Skn. Caracersc er yema afecng e ace aong e brdge
e
e
dened
wc
an
rena
is
gastrointestinal
wn
o
compexes
aways
eecron
the
erave gomeruoneprs s e mos common manesaon
approxmaey
•
and
abnormay
mmunoluorescence
e
•
o
sclerosis
sgncan
and
ssue
a
njur y
brobass
causes
and
a
e
bross.
are
cronc
scema
Aernavey,
sponaneousy
e
a
umaey
prmar y
acvaed
o
deec
produce
resus
may
e
excessve
coagen.
der-
4.3).
Cardovascuar system. here may be damage o any ayer o e Mor pholog y.
ear.
Sympomac
or
asympomac
percarda
nvovemen
mos
presen
n
up
o
50%
o
paens
and
may
be
acue,
subacue,
Sysemc
sceross
s
a
mu-sysem
dsease.
he
s promnen
canges
occur
n
e
skn,
amenar y
rac,
mus-
or cuoskeea
sysem,
and
kdney,
bu
esons
aso
are
oten
pres-
cronc. Durng e acue pase, brnous exudae s seen on e en
percarda
surace
and
an
efuson
may
be
presen.
W
n
e
o
e
exudae
may
ead
o
bross
and
a
Myocards
s
ess
common
and
may
cause
and
eecrocardograpc
Lbman-Sacks)
abnormaes.
endocards
ave
4.9),
(Suppemena
more
common
pror
endocards
o
akes
e
e
wdespread
orm
o
use
snge
o
or
any
•
verrucous
ear
Oter
seen
serosa
n
e
brnous
•
Oter
vs.
vave,
s
I
may
vague
exudaes,
a
bu
be
may
rees
acue
and
on
or
no
s
a
n
serods.
mupe,
generc
specc,
wereas
o
surace
smar
peura,
a
o
o
souders,
o
e
a
musysem
by
syno-
nma
requre
paens
an
asue
anbodes
ound
n
anbodes
and
ndngs.
presen
w
pyscan
(ANAs)
vr uay
o
dsease,
morpoogc
Many
100%
a
o
o
bnd
paens
doube-sranded
DNA,
deeced n 40% o 60% o cases, are gy specc or SLE, and ence
a
useu
o
dagnosc
ndngs,
neproc
s
a
ncudng
syndrome
presenng
cnca
es.
Rena
emaura,
(see
Caper
manesaon
probem.
nvovemen
n
red
11).
some
romboemboc
ce
may
paens
produce
cass,
Anema
or
and
penomena
a
proenura,
are
skn
e
and
ngers
assocaed
and
dsa
aropy
regons
exends
proxmay
o
nvove
e
o
upper
neck,
and
ace.
oss
Fbross
o
ree
oten
pegs,
s
accompaned
aropy
o
e
by
derma
and
and
yane
ckenng
o
e
was
o
derma
ar er-
capares.
nge rs
be
a
and
s
dy spag a
or
s ce m a
R ay nau d
D us e
aca
and
o
nvove me n .
pro g re ss ve
c ou rs e,
and
Two
and
are
s
m e d
bu
are
d e ve opme n
DNA
w
a
n
s
o
e
o e n
T e
C R E ST
c on ne d
and
s
re qu e n ,
o
s
an
no
s ow y
om nous
s c e ro s s .
sp e c c
pu mon ar y
bro s s
an c e n rome re
nge rs ,
or
d e ve op
a
g y
s y nd rome,
ae
an
s y se m c
o e r,
o
ave
s
caed
nd c a ng
s ome me s
I,
e
e ads
re sp ons b e
we a e r,
p a e n s
ke o o d
c a c c a ons ;
c o d
w
o
e s op ag us
y p e r e ns on
ass o c ae d
d s e as e.
e
p a e n s
Mo s
op o s ome r as e
g re ae r
w
d s e as e,
sub c u ane ous
re as ons ,
m mob z a on
o
n ar row ng
e sp e c a y
proe nu r a
s rong y
ass o c ae d
Vas c u ar
y p e r e ns on .
v as c u ar
sk n
pu monar y
M d
c aus e s
Invove me n
o e s ,
u nc e ar
ag a ns
p e r pe r a
ace;
and
A NAs
ass o c ae d
an b o dy,
For
s y se m c
d re c e d
s
and
pe nome non .
or
O ne,
bro s s
ob s r u c on .
nge rs
pu monar y
sgn.
sk n
e au re s .
n
w c
e re
ore ar ms ,
e s op age a
and
e s ons
y p e r e ns on .
varey
and
romboc yopena
may
and
epderms,
Clncal Features.
re na
and
e
n
o
a
eadng
nonerosve
vesses
o
begns
eales.
o
by
sma
varabe
onse.
are
e
Mos
o
CNS.
annucear
angens
eer
o
ner ves.
hs
1-
bross.
seroogc,
n
e
nvoved
e
gy
cnca,
sympoms
nucear
be
on
Inlammaon
occuson
seen
orm
surace
nvove
and
may
nsdous
puzzng
o
be
may
eer
may
efusons,
jons
SLE
S o-caed
varey
are
he
on
nvovement.
Nonnlammaor y
Features.
dagnose.
o
cavty
organs.
dagnoss
wc
percardum
proeraon
Clncal
deposs,
dsncvey
perpera
4.4)
oes
3-mm
bross
usuay
exremes
appendages,
sere
and
Vavuar
eFg.
nnng
was
dfuse
wc
upper
arms,
(so-caed
ungs,
resng e
acycarda
ear,
resrcve (Fg.
percards.
vesses,
me, paens
organzaon
bood
domnan
secondar y
o
Sjögren
In
this
and
Syndrome
disease,
salivary
chronic
glands
inammation
lead
to
reduced
and
destruction
production
of
tears
of
lacrimal
and
saliva.
CHAPTER
A
B
C
D
Diseases
4
of
the
Immune
51.e1
System
E
Supplemental
2
o’clock
increase
ing
by
in
a
light
San
with
microscopy.
University
of
of
Lupus
stain).
(E)
the
Deposition
Brigham
Southwestern
California.)
(A)
Focal
of
(H&E
immune
IgG
and
Medical
not
stain).
dense
antibody
Women’s
is
complexes
Subendothelial
of
proliferative
proliferation
glomerulus
deposits
nephritis.
Pathology,
Texas,
Francisco,
SLE
nephritis.
Extracapillary
throughout
subendothelial
patient
Department
4.1
(H&E
cellularity
extensive
from
eFig.
positions
in
a
School,
(C)
Lupus
(periodic
deposits
granular
Hospital,
Dallas,
glomerulonephritis,
prominent
this
nephritis
case.
pattern,
stain).
on
detected
Courtesy
of
two
a
(D)
necrotizing
proliferative
glomerulus
Electron
with
membrane
Courtesy
Jean
of
Olson,
Dr.
several
of
(arrow)
(A
Edwin
lesions
to
a
the
“wire-loop”
renal
C,
of
11
Courtesy
to
of
the
lesions
Dr.
represent-
loops”
Helmut
University
of
of
and
marked
capillary
“wire
Department
Pathology,
o’clock
Note
glomerular
correspond
Eigenbrodt,
Department
at
glomerulonephritis.
micrograph
immunofluorescence.
D,
Dr.
focal
Diffuse
basement
by
Massachusetts.
E,
with
(B)
showing
acid-Schiff
(arrowheads)
Boston,
Texas.
in
loop
seen
Rennke,
Pathology,
California,
51.e2
CHAPTER
Diseases
4
of
the
Immune
System
Supplemental
the Supplemental
eFig.
4.2
Systemic
lupus
erythematosus
involving
skin.
An
H&E
stained
section
shows
liquefactive
degeneration
of
of
Ig
layer
of
the
epidermis
and
edema
at
the
dermoepidermal
(Courtesy
Boston,
lupus
Boston,
Bhawan,
eFig.
4.4
erythematosus.
thickened
Schoen,
Jag
Boston
University
School
of
Medicine,
MA.)
Supplemental
in
Dr.
valve
leaflet
Department
Libman-Sacks
The
are
of
Massachusetts.)
endocarditis
vegetations
indicated
Pathology,
by
attached
arrows.
Brigham
to
of
the
the
(Courtesy
and
mitral
margin
of
Women’s
valve
of
Dr.
Systemic
lupus
erythematosus
micrograph
along
the
dermoepidermal
Department
of
stained
junction.
Dermatology,
juncwestern
tion.
4.3
for
involving
IgG
(Courtesy
Dr.
reveals
Richard
the Sontheimer,
basal
eFig.
immunofluorescence
the deposits
skin.
An
the
Fred
Hospital,
Medical
School,
Dallas,
Texas.)
University
of
Texas
South-
52
CHAPTER
Diseases
4
of
the
Immune
System
A
B
C
Fig.
4.9
Systemic
extensive
and
foci
of
creating
Richard
Pathogeness.
dsorders
auommune
owards
s
as
o
e
dsease
eoog y.
even
he
s
O
been
savar y
deveopng
rggers
oten
gands,
o
e
a
w
(C)
w
of
and
oer
dsease
perssen
s
SS-B
are
naed
Skin
dermis
extensive
of
are
by
specc
vra
an
or
and
necon
T-ce
reacon
subsequeny.
from
virtual
has
University
dreced
known,
with
supply
auommune
wo
biopsy
subcutaneous
blood
supporng
no
auommune
(B)
the
Loss
auoanbodes,
ormaon
in
Dermatology,
auoanbodes,
SS-A
skin.
The
deformity.
Department
varous
e
a
Normal
collagen
(arrow).
assocaed
anbody
(A)
dense
flexion
serum
angens
or
suggesed
clawlike
Sontheimer,
presence
of
inflammation
a
rbonuceoproen
dsease.
e
he
and
sclerosis.
deposition
of
patient
fibrosis
led
to
e
n
some
seen
and
e
Te
and
s a var y
g ands
are
e
maj or
o
abou
e
ds e as e,
bu
o er
exo cr ne
g ands ,
ncud ng
e
respraor y
and
gas ro nes na
rac s
and
e
a
may
be
nvove d.
T e
acr ma
and
s a var y
g ands
dens e
n raes
o
C D 4+
T
o ces
ce s
w
(Fg .
4.10);
ger m na
n
e
ceners ,
arger
ce
re ac on,
may
a s o
be
s e en .
S a v ar y
g ands
mos
Lack
dr yness
sepum.
ncude
More
an
e
o
may
o
and
sava
ead
Lesons
synovs,
a
requeny
acrma
gands,
causes
o
paens
reumaod
o
dr yness
uceraon
ousde
perpera
e
ere
uceraon
e
and,
gands,
neuropay,
ave
anoer
arrs.
TRANSPLANTS
o
damaged
organs
rom
or
oer
unconay
ndvduas
mpared
as
organs
become
by
rans-
sandard
Abou
30,000
organ
ranspans
are
perormed
med-
yeary
Uned
Saes,
e
mos
common
beng
e
kdney
(accounng
n
or
s a var y
nd c a ve
may
o
pracce.
o
a ),
be
oowed
by
e
ear,
ver,
ung,
and
pancreas.
Trans-
a panaon
B
OF
e
o
nlammaon
scca).
Nasa
paens,
dsease,
repacemen
amos y mpod
desrucon
Dr.
Dallas.)
c on a n e
g ands,
o
bross.
School,
secondar y
o
fingers,
vag na, ca
a s o
o
the
Courtesy
o s e panaon
nng
Medical
the
follicles)
arhe
ges
and
(C,
Note
hair
immobilized
Because
eyes
(e.g.,
ulcerations.
peroraon
pumonar y
auommune
acr ma
virtually
(xerosoma).
cases,
REJECTION
Morphology.
sclerosis.
(keraoconjuncvs
mou
n
systemic
appendages
Southwestern
o
cornea
o
has
Features.
dr yness
e
with
of
cutaneous
Texas
Clncal
s
a
absence
o
emaopoec
sem
ces
s
dsorders
o
wdey
used
o
rea
bo
v s by neopasc
and
nonneopasc
bood
ces.
Excep
n
rare
en arge d. cases
o
denca
wns,
e
grat
donor
and
recpen
are
genecay
CHAPTER
A
4.10
Sjögren
infiltration
ment
of
Burns,
em
and
Some
are
rejecton.
same
o
ese
Grats
caed
syndrome.
ductal
or
of
are
mmune
beween
(A)
epithelial
Dermatology,
Department
excanged
are
with
dferences
responsbe
speces
Enlargement
hyperplasia
University
Pathology,
recognzed
of
e
o
nondenca
Texas
a
of
Texas
mmune
e
the
salivary
salivary
grat,
sys-
caed
ndvduas
o
e
(A,
Immune
system
and
Responses
principal
are
As
e
as
(so,
ssue)
among
encoded
by
T
School,
Medical
dferen
o
grat
en
up
ces
ces
by
e
or
In
grat
cause
grat
ypes
paoogc
ese
T
grat
e
(drec
s
dspay
rejecon.
immune
both
moecues
and
and
or
e
Recpen
resung
n
s
n
MHC
grat
and
MHC
presened
mgrae
B
ces
e
o
CD4+
aso
may
be
T
ces
no
o
by
may
(ndrec
CD8+
T
e
a
e
n
CD4+
of
T
be
o
ces
o
grat
Rejection
allografts
nlammaon
bnd
of
is
specc
n
e
ssues
crcuang
Solid-Organ
mediated
or
grat;
of
grat
T
angens
CD8+
(noaby
by
CTLs
acvae
grat
because
ces;
compemen,
s
e
and
a
and
e
cause
e
cell
Depart-
Dr.
Dennis
paerns
eaures,
eac
s
s
were
dened
caused
medaed
presen
rapdy
n
anbodes
and
and
bood
e
by
on
e
specc
bnd
o
scemc
group
grat
bass
mmune
necross
o
a
o
e
e
ackng
angen.
grat
a
vas-
lood
acvang
grat
e
or
ranspan-
anbodes
causng
was
specc
o
endoeum,
cascade,
ndvduas
agans
pror
preormed
ncompaby
snce
anbodes
anbodes
connecon
wen
coaguaon
by
recpen
oowng
crcuaon,
rejecon,
Careu
bood
w
donor
rejecon.
CTLs
group
T
and
macng
eads
grat
o
(Fg.
o
argey
rapd
(Fg.
e
rom-
4.11).
greaes
rsk
parcuar
Recpens
recpens
grat
In
aure.
acue
damage
Immunosuppressve
reang
acue
rejecon
an
In
ces
and
In
or
ABO
wo
ave
prospecve
e
any
as
oer
weeks
ceuar
e
A
bnd
e
grat,
vascuar)
o
ater
rejecon,
same
wc
rejecon,
grat
endo-
compemen-dependen
ceuar
erapy
(or
probem.
o
4.12).
n
angens,
by
s
days
acue
(Fg.
umora
donor
many
Oten,
coexs.
deveops
nlammaon
agans
4.13).
emnaed
rejecon
parencyma
damage.
cause
o
smuae
produced
and
ave
orm
ces
e
are
ssue
hs
k
CD4+
mecansms
or
and
been
umora
more
reacons
successu
n
orm.
Cronc rejecon. W ncreasngy efecve erapy o acue rejec-
on,
cronc
rejecon,
wc
deveops
over
mons
o
years,
as
become e major cause o grat aure. Cronc rejecon s carac-
nduce
erzed
anbodes
mos
Courtesy
hs
ver y
os
vesses
make
eum,
antibodies.
cyoknes
plasma
Dallas.)
are
sysem
ABO
anbodes
Allografts
and
secree
k
endoeum
anbodes),
cells
a
hese
exacerbaes
and
specc
Acue
me,
specc
moecues
rsk.
CD8+
aken
ranspan,
B,
and
Sontheimer,
aoug
cnca
ranspanaon
recogn-
ces
anbodes
on
recp-
be
a,
e
e
reacve
•
•
Rejection
53
donors and cross-mac esng or serum anbodes n e recpen
moecues.
Mechanisms
System
been senszed by bood ransusons or prevous ranspan are aso
dfer
presened
recognzed
recognze
producon
be
d-
by
o
pas,
angen
proens
a
Dallas.
rejecon.
yperacue
recognon
oregn
moecues
and
back
as
e
HLA
a
MHC
or
moecues
grat
or
Richard
School,
occurs
o
grat.
boss
grats
acceped
genes
o
recognzed
e
be
(MHC,
angens
dscov-
ssue
woud
uncon
APCs)
recpen’s
acvaed,
I
cuaure
cellular
were
no
compex
pepde
grat
or
poymorpc
expresses
e
ces
e
ndvduas
pysoogc
o
APCs
are
evoke
moecues
weer
gy
recognon),
cases,
oregn,
o
donor
MHC
recpen’s
angens
Immune
lymphocytic
Dr.
angens
compemen
beween
recpen,
ces.
recipient’s
s
and
Hyperacue
aon.
the
which
socompaby
he
genes
e
n
by
molecules,
deermne
coecon
ese
bo
s
as
major
(parencyma
T
on).
a
the
mecansms.
Allografts
recognized
socompaby
a
excanged
he
s
I
ose
recpen’s
mpes,
ndvduas.
by
ces.
rom
Organ
Intense
Medical
responses.
moecues
umans)
er
immune
name
e
(compabe).
n
to
antigens
histocompatibility
humoral
ered
graft
(B)
Courtesy
Southwestern
•
aograts.
gland.
gland.
Southwestern
University
by
desrucon
of
in
donor
The
of
B
Fig.
dferen.
Diseases
4
o
access-
njury
by
vesses
vascuar
and
nlammaon
njur y
scema,
and
and
and
scemc
nma
bross,
nersa
ssue
njur y
eadng
bross
(Fg.
due
o
narrowng
o
proonged
4.14).
o
e ssues. A ree mecansms may be nvoved smuaneousy, bu as
Treatment
of
Graft
Rejection
s dscussed aer, ey pay domnan roes n dferen ypes o rejecon. In
The
major
graft
injury
hese
kdney
a
patterns
and
have
paerns
ranspans,
sod
organ
of
rejection
different
were
bu
rs
e
ranspans.
reect
morphologic
descrbed
same
he
different
and
prncpes
uy
o
and
are
mechanisms
clinical
bes
appy
o
features.
esabsed
e
cassyng
of
or
rejecon
rejecon
o
no
a
grat
excep
denca
sur vva.
wns,
mmunosuppresson
Corcoserods,
an–T-ce
s
needed
anbodes,
and
o
proong
drugs
a
nb T-ce uncon are e mansays o reamen. Immunosuppres-
son
carres
vaon
o
e
rsk
aen
o
opporunsc
vruses
(e.g.,
unga
and
poyomavrus
vra
and
necons.
Reac-
cyomegaovrus),
as
54
CHAPTER
Diseases
4
of
the
Immune
Complement Blood
System
activation,
inflammation vessel
and
damage,
thrombosis
cell
Alloantigen
(e.g.,
endothelial
Endothelial
blood
Circulating
group
antigen)
specific
alloantigen-
antibody
A
B
Fig.
4.11
causes
Hyperacute
thrombosis.
neutrophil
rejection.
(B)
infiltration,
Hyperacute
and
+
A
Alloantigen-specific
CD8
(A)
severe
Deposition
rejection
ischemic
of
of
a
injury
antibody
kidney
on
endothelium
allograft
(necrosis)
in
a
showing
and
activation
platelet
and
of
fibrin
complement
thrombi,
early
glomerulus.
+ and
CD4
T
cells
+ +
CD8
Direct
Cytokines
CD4
killing
Recruitment
of
Parenchymal
macrophages
cells and
neutrophils
B
+ CD8
Neutrophil
+ CD8
Macrophage
Parenchymal
Interstitial
cell
damage
inflammation
C
Fig.
4.12
involves
T
cells.
direct
(B)
between
tory
Acute
cells
cellular
killing
Acute
of
rejection.
graft
cellular
epithelial
cells
damaging
rejection
of
the
cells
the
(A)
by
of
CD8+
a
tubules
endothelium
Destruction
CTLs
kidney
of
and
graft,
(tubulitis).
(C)
graft
cells
by
T
inflammation
manifested
Acute
by
cellular
cells.
caused
Acute
by
inflammatory
rejection
T
cell–mediated
cytokines
cells
involving
in
an
produced
the
rejection
by
CD4+
interstitium
artery
with
and
inflamma-
(arrow).
we as an ncreased rsk o cancers, are aso seen n mmunosuppressed
paens.
he
process
because
e
was
HSCs
sorcay
were
soaed
caed
rom
bone
e
marrow
donor’s
ranspanaon
bone
marrow,
bu
now ese sem ces are mobzed rom e marrow o donors by rea-
Hematopoietic
The
transplantation
treat
rect
Stem
leukemias
numerical
and
or
of
Cell
Transplantation
hematopoietic
other
stem
hematologic
functional
cells
men
(HSCs)
malignancies,
deciencies
of
blood
cells.
is
and
used
to
to
cor-
er
rom
w
grow
marrow
e
acors
“nce” ,
perpera
or
agens
aowng
HSCs
a
o
be
nb
bndng
ar vesed
n
o
mos
HSCs
o
nsances
bood.
Recpens o HSCs need “condonng” o abae er own mmune
sysem
(o
preven
grat
rejecon),
creae
“space”
or
e
ranspaned
Blood
Endothelial
cell
vessel
Alloreactive
antibody
Endotheliitis
Complement
activation
A
C
B
Fig.
4.13
vessels.
graft.
tesy
Blood
vessel
(C)
Dr.
Acute
(B)
antibody-mediated
Light
micrograph
Immunoperoxidase
Zoltan
Antibody
Laszik,
(humoral)
showing
staining
Department
shows
of
rejection.
inflammation
C4d
Pathology,
(A)
Graft
(capillaritis)
deposition
University
in
of
damage
in
caused
peritubular
peritubular
California
by
capillaries
San
antibody
capillaries
and
deposition
(arrows)
a
in
glomerulus.
in
kidney
(Cour-
Francisco.)
binding Chronic
to
a
inflammatory
reaction
endothelial in
vessel
wall
antigens Intimal
smooth
muscle
proliferation
Vessel
Cytokines
occlusion
+ CD4
Alloantigen-
specific
CD4
+
T
cell
Cytokines
A
Vascular
smooth
muscle
cell
B
C
Fig.
4.14
Chronic
rejection.
(A)
D
Graft
arteriosclerosis
caused
by
T -cell
cytokines
and
antibody
deposition.
(B)
Graft
arteriosclerosis in a cardiac transplant. (C) T ransplant glomerulopathy, the characteristic manifestation of chronic anti-
body-mediated
eruliitis),
fibrosis
and
(asterisk)
ing
tubular
shows
prominent
Hospital,
rejection
accumulation
in
of
the
atrophy,
fibrosis,
C,
courtesy
(B,
Dr.
The
glomerulus
matrix,
resulting
contrasted
arteriosclerosis.
Boston;
kidney.
mesangial
from
with
Dr.
inflammatory
of
narrowing
normal
Laszik,
shows
duplication
vascular
the
Courtesy
Zoltan
and
kidney
Richard
the
and
on
the
Mitchell,
Department
of
cells
capillary
ischemia.
top
right.
In
At
Department
Pathology,
within
basement
of
this
the
the
trichrome
bottom
Pathology,
University
capillary
membrane.
of
stain,
right
is
the
an
Brigham
California
loops
(D)
blue
artery
and
San
(glom-
Interstitial
area
show-
Women’s
Francisco.)
56
CHAPTER
sem
ces,
umor
and
ces.
versus-os
maure
and
T
beng
e
ver,
jaundce,
ndoen
o
(probaby
ympocyes).
can
canno
wc
due
o
he
o
T
rac,
and
cronc
magnances)
ony
ssues
and
e
oregn,
e
skn
nlammaon)
(because
soogc
o
o
may
o
decency
a
B ecause
e
s
ake
o
HSC
e
and
severa
T
ranspans
aso
ranspaned
may
ces
ympocyes.
ave
produce
Recover y
o
proound
adequae
mmune
grs
mos
mmuno-
o
make
T
e
o
individuals
susceptible
to
infections
and
common,
ous
w
decences
cncay
dseases
necons.
he
paens
and
cancers
Paradoxcay,
deveop
auommuny,
reason
or
mecansms
mmune
s
are
or
may
mos
some
a
mmune
deecs
ge
be
oten
relecon
s
because
are
e
vrus
w
o
a
sysem
resu
or
o
nduced
he
new
may
bu
be
be
uae
nec-
o
can
because
nduce
que
or
secondary
to
may
other
e
o
n
o
o
a
X
e
o
are
X-nked
IL-2
T-ce
boys
by
eads
cromosome
cans
proound
dseases,
bo
SCID
ese
deamnase,
n
e
o
o
wc
or
and
e
IL-7.
progenors,
decenc y
are
oer
recessve
T-ce
and
auosoma
s
s
n
e
afeced
o
and
purne
a
g
ave
been
e
eves
n
decenc y
meaboes,
ces
he
encodng
deamnase
proerang
genes
recessve.
gene
expressed
Adenosne
oxc
rapdy
Many
are
cases
ymus.
be
primary
(resulting
sysems
on
sysem.
ns
oerance
by
excessve
from
recurren
wc
suc
as
are
mma-
dened
n
rare
SCID.
B-ce
necons
(cyomegaovrus,
e
paens
w
responses
w
X-SCID
s
varcea).
norma
a
are
wde
e
rs
HSC
mmune
dsease
agammagobunema
and
s
a
an
resuan
od
name
muaons
yrosne
n
knase.
maure
B
aure
or
e
mpared,
range
o
ranspanaon
ces
a
due
e
a
s
and
as
s
been
e
paens
paogens,
can
repop-
mansay
reaed
a
deec
anbodes).
a
ce
n
anbodes
w
w
recepor
requred
or
deec
o
gene
maura-
B
B-ce
B-ce
ce
gobu-
s
moecue,
e
n
B-ce
(gamma
he
sgnang
assocaed
pre-B
are
o
produce
encodng
knase
and
sgnas
s
o
crcuang
gene
hs
ces
devers
caused
Bruon
recepor
progenors,
proeraon
and
muta-
are
c aus e d
by
mu a ons
a
Wou
ese
sgnas,
B
ces
de
a
e
pre-B
sage,
er m
congenta
mmunode f c enc y
s
n
e
absence
o
anbody-producng
B
ces
and
pasma
are
ces. so
cases
e
ep
disorders.
mmunode f c e nc es
n er e d,
ces
w
resung
usu a y
one
T-ce
nereukns
proeraon
eads
X-nked
accumuaon
mauraon.
Pr mar y
cases
muaon
auosoma
X-nked
and
tions)
e
e
on
suscep-
caused
and e ces are ranspaned no e paens.
•
n
diseases
a
(γc),
o
oten
erapy, n wc a norma γc gene s nroduced no HSCs o paens
acvaon.
Immunodeciency
w
a
gene
ncudng
sgnang
damagng
reamen.
aen
be
mmune
necons
que
necons
mmune
yperacve
uncear ;
rare.
o
reacvaon
deecve
perssen
seem
reavey
mcrobes
paens
assocaon
os
e
paogenc
are
dverse.
he
o
sgncan
ese
opporunsc
or
e
can
mos
absence
Abou
n
s
nanc y
ncudng ung (Candda, Pneumocysts), bacera (Pseudomonas), and
vruses
md
γ
e
I
n
and
DISORDERS
cancers.
Aoug
IL-7
ympoc yes.
presen
Immunodeciencies
muaon
requred
As
and
c yoknes,
adenosne
Because
IMMUNODEFICIENCY
necons.
presens
mmuny
carrers.
o
cases
a
common
remanng
especay
ure
s
requen
eads
mons.
e
o
o
(SCID)
ce-medaed
producon.
by
many
ces.
deveopng
compeence
range
anbody
or
and
mauraon,
caused
IL-7
are
he
sys-
numbers
T-ce
T
mmunodeicency
umora
dverse
absence
maure
var-
n
encodes
recepors
enzyme
beore
granuocyes
n
reduced
acvaon
resembe
a
(X-SCID),
more
are
o
deecs
aure
a
combned
deecs
by
ces.
ssues
ere
proonged
pcure
s
oer
and
aso
epea
ver
S evere
w
recpen,
GVHD
and
•
serous
aackng
producng
Cronc
k
dferences
he
kng
System
grat-
bu
cause
non-MHC
skn,
s
HSCs
response.
and
o
Immune
s
rases.
auommuny
and
no
ce–medaed
bross
cnca
oer
sma,
rejec
by
darrea,
os
ec
the
ranspanaon
conan
Even
can
and
HSC
aack
probems.
of
sceross.
Recpens
may
ces
gasronesna
n
w
Grats
recpen
boody
manesaons
emc
eukema
caracerzed
condon
promnen
ous
ese
and
s
o
probem
(GVHD).
cnca
donor
GVHD
o
w
and
aa
case
mmunodecen,
Acute
ces
e
major
dsease
ces,
even
beween
(n
he
Diseases
4
Afeced
cdren
are
suscepbe
o
many
bacera
and
vra
o en
necons. us e d,
bu
s ome mes
e
mu a on
s
a
ne w
one
n
e
a e c e d
• p a en.
Pa ens
y p c a y
pres en
w
re c ur ren
n e c ons
X -nked
absence nanc y
or
e ary
c d o o d,
bu
n
s ome
d s e as es
e
rs
y per-IgM
o
cass-swced
aer
n
mmunodeicences
are
muc
more
common
an
ones.
In
ger-ncome
counres,
e
mos
requen
cause
mmunodecency
s
erapy
a
desroys
e
mmune
sysem
e
and
radaon
mmune
or
cancer)
or
a
s
used
o
o
sysem
ower-ncome
mmunodecency.
(e.g.,
or
grat
counres,
rejecon
manuron
and
s
a
s
an
he
acqured
major
mmunodecency
or
mporan
cause
o
mmunodecency
(Congenital)
wordwde,
and
Because
n
mmuny.
e
on
eper
T
acvae
(ep)
B
on
B
ces
B-ce
w
a
proound
e
de-
gene
he
or
dsease
s
mos
CD40-gand
requeny
(CD40L),
ces
and
s
a
mecansm
by
wc
wc
CD4+
and
ces
and
macropages.
macropages,
and
devers
CD40L
sgnas
bnds
a
o
sm-
responses
o
as
we
as
ce-medaed
macropage
mmuny).
acvaon
Afeced
(e
cdren
cen-
sufer
necons
by
pyogenc
and
nraceuar
bacera,
vr uses,
ung.
components
of
are
caused
innate
or
by
o er
mutations
adaptive
C ommon
that
o
e
e
ncreasng
genec
bass
use
o
o
many
DNA
sequencng
prmar y
Tabe
4.7
and
Suppemena
eFg.
ecnoog y
mmunodecences
4.5
Pa ens
ave
a oug
e
ese.
Seeced
dseases
a
usrae
summarze
e
beow.
de c ences
o
more
bu
p asma
re quen
s
ce s
b ass
and
s
an
e
obs c ure.
numb er
o
B
ce s
s
v r u a y
nor ma ,
an b o d es,
sug ges ng
mporan
n
e
d eren a on
o
maure
B
c e s.
Te
gene c
a
b ass
k now n
n
e wer
an
10 %
o
c as es;
mu a ons
a e c ng
re c ep -
s
or
g row
ac ors
and
o er
y mpo c ye
sg na ng
p a ways
mos
b e en
prncpes
ons. dscussed
s
d s c uss e d,
n
ave o
mmunodef ce nc y
impact
ors known.
var abe
mmuno de c enc es
immunity.
s medcne,
are
assocaed
s
Immunodeficiencies
immunodeciencies
more
common
muaons
reacon
bo ck
now
usuay
aer.
Primary
one
s
cause
•
Primary
I
syndrome
and dscussed
e
auommune
rom (AIDS)
IgM.
ce-medaed
by
ces
ra o
by
ence,
nenonay
uae In
o
expressed
CD40
dseases).
and,
(e.g.,
T
suppress
dened
anbodes,
o
s
cemoerapy
orgnay
IgA
pr-
caused mar y
was
and
e.
cenc y Secondary
IgG
sy mpoms
domnance app e ar
sy ndrome
n
rep or e d.
Pa ens
are
sus cep be
o
b ac er a
n e c-
CHAPTER
BONE
Diseases
4
of
the
Immune
56.e1
System
MARROW
THYMUS
Pluripotent
stem
cell
ADA
deficiency
Pro-B
cell
Pro-T
cell
X-linked
SCID
Common γ
(cytokine
chain)
myeloid-lymphoid
progenitor
Pre-B
cell
Immature
Di
receptor
heavy
agammaglobulinemia
cell
T-cell
IgM
X-linked
T
George
syndrome
chain
(BTK)
MHC
class
II
deficiency
CD40L
IgM
+
CD4
T
cell
Mature
T
cells
IgD
Hyper-IgM
Immature
B
cell
syndrome
(CD40L)
+
+
CD8
CD4
CVID
IgA
deficiency
IgM
Mature
Supplemental
in
these
ADA,
eFig.
pathways
adenosine
in
4.5
B
IgA
IgE
cells
Primary
selected
deaminase;
immunodeficiency.
IgG
immune
primary
CD40L,
deficiency
immune
CD40
diseases.
deficiency
ligand
(also
Shown
diseases.
known
as
The
are
the
principal
affected
CD154);
CVID,
genes
pathways
are
common
of
indicated
variable
lymphocyte
in
development
parentheses
for
immunodeficiency;
some
SCID,
and
of
the
blocks
the
disorders.
severe
combined
CHAPTER
Table
4.7
The
Major
Primary
Immunodeficiency
Disease
A.
Functional
Defects
in
lymphocyte
Severe
combined
X-linked
SCID
Diseases
4
of
the
57
Diseases
Deficiencies
Mechanism
immunodeficiency
of
Defect
(SCID)
Markedly
decreased
reduced
T
cells;
serum
normal
or
increased
B
Cytokine
Ig
tions,
of
cell
System
maturation
cells;
B
Immune
receptor
common
defective
IL-7
T-cell
ℽ-chain
maturation
gene
due
muta-
to
lack
signals
immunodeficiencies
X-linked
agammaglobulinemia
Decrease
in
all
serum
Ig
isotypes;
reduced
B-cell
Failure
numbers
of
maturation
because
of
beyond
mutation
in
pre-B
Bruton
cells,
tyrosine
kinase
Ig
heavy-chain
deficiencies
Deficiency
with
Disorders
DiGeorge
of
T-cell
in
Decreased
lymphocyte
hyper-IgM
variable
IgA
or
sometimes
associated
Chromosomal
IgE
deletion
involving
Ig
heavy-chain
locus
T
cells;
normal
B
cells;
normal
or
decreased
Anomalous
Ig
chial
development
pouches,
leading
of
to
3rd
and
thymic
4th
bran-
hypoplasia
activation
syndrome
Defects
in
phage
Common
subclasses;
maturation
syndrome
Defects
X-linked
IgG
absent
serum
B.
of
immunodeficiency
helper
T-cell–dependent
B-cell
and
macro-
Mutations
in
CD40
ligand
Mutations
in
receptors
activation
Reduced
or
no
subtypes
bacterial
of
production
of
selective
immunoglobulins;
infections
or
no
isotypes
susceptibility
clinical
or
to
tors,
for
B-cell
growth
fac-
costimulators
problems
+
Defective
the
class
bare
II
MHC
lymphocyte
expression:
Lack
syndrome
of
T-cell
and
X-linked
lymphoproliferative
class
disease
T
Chronic
in
innate
Uncontrolled
disease
deficiency-1
adhesion
Absent
deficiency-2
Complement
C2,
deficiency
C4
Defect
or
deficiency
in
and
•
Epstein-Barr
Disorders
of
D G e or g e
a
n
T- c e
spe en,
rd
o
s
a or c
( t y m c
v ra ,
ou r
a rc .
m ay
T
bo o d,
o
e a ny,
In
as
and
Mutations
defective
genes
encoding
for
class
II
transcription
MHC
gene
protein
in
gene
involved
encoding
in
SAP
signaling
in
(an
adaptor
lymphocytes)
responses
we
90%
o
and
o
g and
as
a b s e n
n
n a n s
pro o z o a
g ands ,
and
e
o
to
MHC,
of
e
Mutations
by
s
d e e c
p or on s
a
and
integrins
causing
Mutations
functions
leukocyte
causing
18)
ligands
failure
to
for
comple-
in
β2
of
Mutations
encoding
oxidase
gene
components
of
enzyme
encoding
the
β
chain
(CD
integrins
in
E-
Mutations
of
immune
genes
gene
synthesis
nent
pathway
clear
of
Mutations
of
activation
in
in
of
and
encoding
the
P-selectin
C3
gene
C2
or
C4
a
protein
sialyl-Lewis
X
required
compo-
ligands
gene
complexes
disease
histocompatibility
complex.
a
c on g e n -
n
From
Abbas
AK,
e
r s e
ace
and
e
T- c e
d e e c s ,
n
y p o -
d e v e opm e n a
s y n d rom e ,
e re
s
a e c ng
p a e n s
Lichtman
AH,
Pillai
( o e r
an
c rom o s om a
mprov e
or
m mu n o d e c e n c e s ,
a re
d e e c
ds-
g ve
Mo s
m e n
no des,
Te
d e e on
6).
de -
a e c ng
re s u n g
md ne
of
lupus-like
d e e c
a
o
β2
in
phagocyte
S:
Basic
Immunology:
Function
2016.
y mp
s r u c u re s
D G e or g e
intermedi-
tissues
cascade
classical
of
re s u n g
w
y m c
into
major
Elsevier,
of
P-selectins,
failure
n e c on s .
y p op a s a ,
a d d on a
cas es
migration
c au s e d
y mu s ,
p ou c e s ,
and
activation
interleukin;
s
oxygen
adhesion-dependent
expression
E-
development
d e v e opm e n a
a d d on
p a r a y ro d
a bn or m a e s .
in
required
expressions
proliferation
antibody
reactive
expression
deficient
leading
Philadelphia:
e
a re
and
a
p a r a y ro d
n
o
ce s
u ng a ,
IL,
ed.,
y p o p a s a )
par y nge a
T u s ,
be
5th
d e v e opm e n
p e r p e r a
o
y mu s ,
cacemc
System,
c on s e qu e n c e
and
e
e re
a
e
immunoglobulin;
m au r a on .
and
v u ne r ab e
ord e r
Immune
s y n drom e
d e e c
c e n
disease; Ig,
the
factors
immunity
activation;
and
Mutations
the
complement
Deficient
and
of
leukocyte
endothelial
ment,
EBV,
function
deficient
leukocyte
C3
B-cell
(CTL)
CD4
immunity
phagocytes
or
Absent
for
Complement
CTL
production
by
defective
Leukocyte
EBV-induced
impaired
cell-mediated
humoral
lymphocyte
and
Defective
ates
adhesion
defective
and
immunity
granulomatous
Leukocyte
expression
cell–dependent
NK-cell
Defects
MHC
activation;
cytotoxic
C.
II
•
bu
s
n o
w
n e c on s ) .
D G e or g e
re g on
age
and
22q11
do
Un k e
n o
mos
s y n d rom e
s
a
(see
C ap e r
re qu re
o e r
re a -
pr m a r y
d e v e opm e n a
e r a b e .
D efects n nnate mmunty. Deecve producon o reacve oxygen
speces
n
neurops
s
caused
by
muaons
afecng
e
pago-
cye oxdase enzyme (Caper 2). hs dsease s caed cronc gran-
uomatous
dsease
(CGD)
because
srong
macropage
acvaon,
oten resung n granuoma ormaon, compensaes or e nab-
y
o
neurops
o
desroy
pagocyosed
mcrobes.
he
eukocyte
adeson deicences are caused by muaons afecng e uncons
58
CHAPTER
o
e
adeson
kocye
moecues
recrumen
mpared
n
ese
neurops
no
Diseases
4
negrns
ssues,
dsorders.
resu
n
and
and
the
seecns
ence
Decen
ncreased
of
acue
(Caper
o
2).
System
Leu-
nlammaon,
recrumen
suscepby
Immune
and
uncons
bacera
conamnaed
are
bood
o
roune
•
necons.
can
occur
bu
s
bood.
now
Transmsson
ver y
by
uncommon
bood
or
because
o
screenng.
occur
breas
IMMUNODEFICIENCY
HIV-neced
can
Moter-to-nfant transmsson s e major cause o pedarc AIDS.
I
ACQUIRED
w
producs
by
mk.
ranspacena
Abou
2%
o
spread
new
cases
durng
are
n
dever y
babes
and
born
roug
o
neced
SYNDROME moers.
AIDS
virus
is
caused
(HIV),
by
which
infection
destroys
with
CD4+
human
T
cells
immunodeciency
and
leads
to
Human
profound
Life
immunodeciency.
hs
e
dsease
grea
drugs
was
scourges
ave
rs
o
provded
dened
e
modern
ope
o
n
e
1980s,
word.
paens,
and
Recen
bu
as
become
successes
remans
a
o
one
o
HIV is
anvra
major
grates
medca
to
ere
word,
on
o
de
he
ree
•
are
more
wom
eac
S exua
n
Asa,
or
are
by
hs
20%
n
ndvduas
Asa,
and
n
amos
1
ans
m-
and
e
domnan
o
rapdy
or
carred
o
neced
luds.
he
are:
75%
accouns
ranser
n
a
or
e
or
o
Abou
bsexua
ncreased,
a
mode
cases.
necon,
50%
men,
bu
especay
more
semen
o
and
o
new
e
here
caed
HIV-1
e
e
occurs
20%
by
o
cases
sarng
o
are
n
needes
capsd
infects
cells
genome,
o
are
and
coner
vra
wo
(e
Structure
via
and
CD4
kills
o
and
cells
and
coreceptors,
when
corecepors,
ces.
HIV
necon,
T
n
o
bu
it
is
inte-
activated
are
we
o
and
gene
and
ce
are
some
rare
we
(Fg.
o
HIV ,
To
ener
subsequeny
corecepors
membrane
ose
a
CCR5
muaons
or
and
s
express
macropages
encodng
ceran
orms
HIV-2.
and
con-
as
repcaon
(caed
os
core
negraon,
proens,
and
CD4
neced
ces
e
wose
vra
reaed
CCR5
e
n
ese
AIDS)
bnds
or
w
many
Poymorpsms
o
dferen
a
a
expresson
gp120
ces
vrus
nvoved
encode
cause
CXCR4
uses
e
enveoped
gene
requen
en
an
wc
vra
proen
hereore,
e
RNA,
recepors
vrus
s
enzymes
genecay
mos
capsd
he
HIV
proens,
reguaors
ouer
dendrc
nravenous
and
cell
rerovruses,
cemokne
vrus).
CD4
body
that
host
srands
suscepby
Anoer
Transmsson
wo
nernazed.
abrasons.
transmsson:
oer
numerous
e
necons
eners
the
4.15).
o
Arca
retrovirus
srucura
ces,
e
eero-
n
a
into
Lke
e
as
omosexua
as
s
and
drec
s
an
n
vrus
mucosa
users.
Arca
HIV-neced
dsease.
ransmsson
more
were
he
Parentera
drug
o
ransmsson
roug
•
n
mon
ransmed
cases
adus.
35
e
transmsson:
repored
and
s
are
rom
modes
accounng
sexua
70%
year
dsease
man
an
Virus:
replicate.
and socea probem, especay n deveopng counres. I s esmaed
a
Immunodeficiency
Cycle
and
aer
n
e
CCR5
ressance.
syrnges
VIRUS
gp120
CD4
Conformational
binding
gp120,
change
bind
CD4
gp41
CCR-5
membrane
Fusion
penetration
with
Membrane
of
host
entry
HIV
cell
of
into
fusion
membrane
membrane;
viral
genome
cytoplasm
gp41
gp120
Cytokine VIRUS
gp41
p17
ENTRY
matrix
Cytokine
receptor
gp120
p24
capsid CD4
Lipid
Chemokine
bilayer
HIV
RNA
genome
receptor
Reverse
transcriptase–mediated
synthesis
of
proviral
DNA
Integrase Cytokine
of
cell;
of
HIV
activation
transcription
Protease
RNA
genome;
transport
RNAs
VIRUS
Reverse
Integration
REPLICATION
into
transcriptase
Synthesis
of
assembly
HIV
of
host
of
cell
to
provirus
genome
proteins;
virion
core
structure
HIV
HIV HIV
DNA
RNA provirus
core transcript
structure
Nucleus
A
VIRUS New
HIV
RELEASE virion
Budding
of
B
Fig.
4.15
covered
(B)
The
with
The
by
life
a
structure
lipid
cycle
permission
Macmillan
and
bilayer
of
HIV
from
Magazines
life
cycle
derived
showing
from
the
Wain-Hobson
Limited.)
of
the
the
steps
S:
HIV.
human
host
from
One
cell
mature
release
virion
immunodeficiency
and
viral
on
and
studded
entry
one
to
the
meets
with
virus
viral
production
two.
Nature
(HIV).
(A)
The
glycoproteins
of
infectious
viral
gp41
virions.
1996;384:117.
particle
and
is
gp120.
(Adapted
Copyright
1996,
of
viral
cytoplasm
CHAPTER
Ater
enr y
produce
pasm
be
o
or
n
ce
us),
provra
compee
s
e
ces
DNA
are
ce,
years,
(e.g.,
s
vra
persss
genome
or
acvaed
vrons
e
wc
no
neced
neced
no
DNA,
negraes
sen
e
HIV
provra
by
o
o
s
an
e
neced
necon
vra
connue
reverse
epsoma
esabsng
ranscrbed,
reeased
RNA
n
a
ce.
aen
or
n
he
e
cyce
are
o
o
neuropaes,
cyo-
vrus
necon.
nlammaor y
proens
e
ranscrbed
orm
caed
may
I
e
smu-
produced,
and
necon.
Diseases
4
B ecause
ree
500
viral
replication
Exacy
s
y
ow
uncear ;
caused
ce
HIV
in
CD4+
infected
e
buddng
syness.
mainly
as
a
consequence
of
vrons
an
and
medaes
ncrease
s
n
membrane
compeve
consequence
s
a
cyopac
s
permeab-
nererence
progressve
efec
w
oss
o
T
os
ces,
prmary CD4+ ces. hs decne s nay mos promnen n muco-
sa ssues (e major se o vrus enr y), en s seen n dranng ymp
nodes,
In
o
and
ony
addon
mmune
e
hese
o
s
e
a
e
numbers
oer
deeced
drec
decency
obser vaon
an
aer
ave
o
T
ces.
neced
T
posuaed
o
neced
mecansms
bood
oss
severy
o
n
been
e
o
ces,
decs
(measured
e
dea
o
oer
accoun
mmune
ces
ncude
useu
o
mecansms
or
s
mosy
e
requen
muc
n
unneced
greaer
e
ces
Te
on
499
vaed
pds,
s
nsun
erapy,
AIDS
sde
cardovascuar
or
s
necon
ewer
RNA
assocaed
Dsease
couns:
and
greaer
an
and
s
o
and
paens
an
200
n
w
C onro
sraes
eves
prevousy
reaed
efecs
and
are
a
dsease,
w
erapy
w
ressance,
kdney,
encepaopay
or
equa
ces/μL.
e
vaue
he
bood,
n
e
s
a
man-
ndvduas.
eradcaed,
paens
ce
HIV-1
anrerovra
no
HIV
progresson
ndvduas
sgncan
cardovascuar,
CD4+
as
progressve
59
dsorder.
C eners
o
descrbed
or
a
System
conanmen
e
ces/μL,
dsease
course
acve
vrus
are
and
HIV
decenc y
ere
erm
o
measured
Curreny,
e
mmune
couns,
HIV-neced
(gy
mmune
ever,
o
o
commony,
neurocognve
o
based
vrema,
Immune
casscaon
200
dsease
paens.
drugs
oss
groups
marker
agemen
vrus
ncude
he
cells,
cells.
repcang
possbes
by
proen
depletes
mos
T-ce
(CD C)
ces/μL,
exen
Pathogeness.
e
CD4+
Prevenon
o
and,
the
HIV-assocaed
decnng
no
of
s
so
o
e
[HAART])
s
a
anvra
deveop
and
ncudng
ee-
and
dseases
How-
cure,
Furermore,
or
unreaed
o
no
no
neuropay,
rsk
unknown
do
medcaons,
dsease.
o
compcaons.
reamen
ese
ncreased
or
ypca
aendan
perpera
ver
s
combnaons
premaure
w
suc
as
ong-
cancer
reasons.
bood).
as
a
con-
AMYLOIDOSIS sequence
on
o
o
er
ympod
cronc
ssue
acvaon,
deecs
n
APCs,
and
e
desruc-
arcecure.
Amyloid Oer
ce
ypes
a
are
afeced
ncude
B
ces
(wc
are
bu
sow
excessve
acvaon),
macropages,
and
is
many
e
CNS.
Macropages
and
mcroga
may
be
reser vors
o
n
ae
sages
o
HIV
necon,
wen
CD4+
T-ce
greay,
macropages
may
be
an
mporan
se
o
nsoube
proens
of
brillar
protein
that
can
a
brs
are
are
produced
produced
n
by
excess
e
aggregaon
amouns,
are
o
no
var-
ceared
or
od
mpropery.
he
proen
deposs
bnd
carboy-
a
resembe
connued
drae-rc vra
deposit
tissues.
numbers
adequaey, decne
and
nec-
ous on;
extracellular
organs
mcroga
hese n
an
no
affect neced
moecues,
mparng
sanng
properes
repcaon.
sarc
(ence,
e
name).
Amyodoss,
reerrng
o
amyod
deposs
and er paoogc efecs, s dscussed ere because some o e mos Clncal
Course.
HIV
dsease
may
be
dvded
no
ree
sequena
common pases
•
(Fg.
Acute
CD4+
T
Vrus
ces
a
eners
e
roug
se.
mucosa
Dendrc
ces
and
a
necs
mucosa
and
ses
desroys
carry
e
vrus o regona ymp nodes, were e vrus repcaes and evenu-
ay spreads o oer ssues. he ndvdua mouns anvra umora
and
ce-medaed
wn
cc
•
3
o
7
CD8+
HIV
many
oer
pod
ce s
do
no
no
ave
•
o
T
a
hs
n
T
no des
p er o d
ce s
n
paens
o
e
n
s
n
oten
n
s
a
o
4
weeks.
ne c e d
p a ens
e
pas e
depe on,
de cne
n
e
opporunsc
ra
by
oncogenc
cer vca
o
e
o
DNA
ana
s
a
ncude
cepas
or
vruses,
B-ce
carcnoma
an
(e.g.,
ceran
common
na
asepc
•
Pneumocysts
canddass,
umors,
many
ncudng
ympoma
(uman
and
o
Kapos
and
n
amyod
cursor
se-med
are
sarcoma
(Epsen-Barr
vra
caused
(Kapos
vrus),
and
Invovemen
manesaon
presumed
vacuoar
cyomeg-
o
AIDS.
menngoen-
myeopay,
perpera
or
by
(see
anbody
the
disease,
chemically
cona
moecues.
each
associated
distinct
serum
o
dsorders
deposs
AL
protein
with
in
a
the
mor-
depos-
amyodoss.
durng
wc
A
s
nrequen
seen
(ubercuoss
especay
o
o
mmunogobu-
can]),
neopasm
he
s
(SAA)
s
now,
a
o
wc
pasma
pasma
deposs
generaed
proen.
nlammaon.
SAA
an
by
made
gt
ces
are
ces
pro-
caed
wou
over
9).
proen,
amyod
are
[amyod
proeraons
Caper
(AA)
produced
he
amouns
secondary
A
amyodoss
•
of
but
(caed
excessve
amouns
num-
mycobace-
wc
papomavrus).
mporan
menngs,
jrovec,
cans
Reactve
en
forms
amyodoss.
g
queny
cr ypococcoss,
and
erpesvrus),
and
CNS
Lesons
o
4.17).
myeoma
bo o d.
necons
necons,
necons)
sarcoma
composed
identical
myeoma,
o
ound mmune decency. Paens w AIDS ave a g ncdence
aovrus
are
several
P rmar y
duced
and
AIDS. he progressve oss o CD4+ T ces umaey eads o pro-
o
(Fig.
n
y m-
bu
c a e d
•
n
ne c e d
y mpo c ye
ere
2
its
se-med
ose
are
phologically
(usuay
s e cond ar y
ssues,
B e c aus e
s
sow
ye ars,
es e
a
There
vrus-spe-
resembng
resoves
man y
bo o d.
o
deveop
sympoms
ce s
e
seroconverson
deveopmen
ypcay
sy mpoms,
Ly mp
over
me,
n
e
repc aes
des roys
numerous
and
sysemc
v r us
s e vere
CD4+
s
w
necons.
and
resung
exposure)
Around
he
aenc y.
e venu a y,
b er
acue
organs
cnc a
o
syndrome,
pas e.
are
responses,
weeks
CTLs.
acue
C ronc
orms
4.16).
pase.
n
n
n
cronc
SAA
pas;
s
an
o
s
acue-pase
nlammaon,
o
o
producon
so
cronc
reumaod
deveoped
composed
proeoyss
Proonged
compcaon
e
are
by
s
o
e
pre-
pro-
arge
orm
o
nlammaory
arrs
more
re-
counres).
O ter forms of amyodoss. Deposs o Aβ amyod are seen n e
brans
o
o
paens
demena.
peraps
e
mos
Mederranean
wc
one
paens
muan
SAA.
In
e
and
pas,
deposs
an
o
o
In
a
composed
deveop
ner ves,
e
some
assocaed
o
sysemc
producon
orms,
ransporer
undergong
o
s
and
oer
amyodoss
e
known,
w
ama
gvng
rse
o
emodayss
β2-mcrogobun
I
dsease
n
nlammaon,
o
amyod
yroxne.
orms
are
“auonlammaor y”
ncreased
ama
perpera
paens
s
o
wc
nered
wc
oer
dsease
orms
sponaneousy
ransyren,
auonomc
Azemer
ama
common
ever,
consequence
precursor
w
S evera
e
s
s
amyod
made
up
o
deposed
n
poyneuropaes.
deveoped
proen
amyod
because
dd
60
CHAPTER
Infection
mucosal
Diseases
4
System
+
Dendritic
cell
cell
mucosal
memory
T
Immune
of
T
of
the
tissues
CD4
Death
of
CD4
+
cells
Virus
to
transported
lymph
ACUTE
nodes
Primary
CHRONIC
AIDS
infection
8
10
1200 Acute
HIV
syndrome
Death
Infection
Wide
1100
established
dissemination
lymphoid
e.g.,
tissues,
lymph
of
lymphoid
virus
organs
7
10
1000
Opportunistic
node 900
diseases
)amsalp
Seeding
in
of
6
Clinical
10
latency
3
of
infection Viremia the
5
10 symptoms
500
T
throughout
Constitutional 600
body
VIH(
4DC
4
10
400
300
10
100
Anti-HIV
HIV-specific 2
0
antibodies
CTLs
10
0
3
6
9
12
1
2
3
4
5
Weeks Partial
control
of
viral
Establishment
infection;
Clinical
in
latency
virus
Other
microbial
infections;
7
8
Years
B
chronic
concentrated
lymphoid
low-level
of
replication
6
virus
tissues;
production
cytokines
Increased
Destruction
viral
of
replication
lymphoid
tissues:
AIDS depletion
of
CD4+
T
cells
A
Fig.
4.16
involving
to
Pathogenesis
mainly
viremia
and
the
and
patient
then
continues
a
erosion
gradual
G,
et
al:
N
of
of
enters
CD4+
J
Med
T
a
phase
but
cells,
AIDS.
(B)
328:327,
course
cells
seeding
unabated,
full-blown
Engl
clinical
CD4+
widespread
rophages
symptoms
and
memory
of
of
and
HIV
clinical
is
1993.
cells,
tissue.
latency.
some
ultimately,
Clinical
infection.
dendritic
lymphoid
there
and
of
course
Copyright
The
this
CD4+
T -cell
infection.
1993
initial
is
to
infection
lymph
controlled
phase,
containment
of
HIV
The
spreads
viremia
During
immune
(A)
and
numbers
CTL,
Massachusetts
viral
of
starts
nodes.
by
the
host
replication
virus
decline
(not
and
Cytotoxic
Medical
T
in
in
mucosal
Viral
immune
both
illustrated).
the
patient
lymphocyte.
Society.
All
tissues,
replication
T
cells
There
and
rights
mac-
continues
develops
(B,
leads
response,
from
clinical
Pantelo
reserved.)
9
10
11
aimeriV
3
200
Immune
response
ANR
mm/sllec
Spread
700
Lm/seipoc
800
CHAPTER
PRODUCTION
AMOUNTS
Diseases
4
OF
OF
of
the
Immune
ABNORMAL
System
PRODUCTION
PROTEIN
AMOUNTS
PROTEIN
Native
folded
OF
OF
(e.g.,
61
NORMAL
MUTANT
transthyretin)
Acquired Chronic
inflammation
Inherited
mutations
mutations
protein
Macrophage
Monoclonal activation
B-lymphocyte
proliferation Amyloidogenic
intermediate IL-1,
(e.g.,
misfolded
IL-6
protein)
Plasma Liver cells cells
Monomers
assemble
to
Immunoglobulin
Mutant SAA
form
β-sheet
structure
light
FIBRIL
AL
A
4.17
Pathogenesis
amyloidosis,
in
of
serum
(TTR)
the
pass
roug
in
excessive
form
no
transthyretin
Limited
Limited
proteolysis
proteolysis
PROTEIN
AA
which
production
amyloid.
amyloid
lead
of
to
(C)
A
amyloidosis.
unknown
of
(SAA),
deposition
as
General
cause
is
and
amyloidosis,
converted
amyloid
mechanism
monoclonal
immunoglobulin,
systemic
which
(A)
mutations
one
Reactive
fibrils
to
the
(ATTR,
in
the
B
of
amyloid
amyloid
formation
cell
light
which
or
(AA)
TTR)
form
amyloid
cell
the
amyloid
(D)
of
fibrils.
(B)
proliferations,
AL
inflammation
protein.
in
of
plasma
chains
chronic
A
PROTEIN
(amyloid
leads
to
Mutations
aging,
Primary
resulting
light
chain)
production
in
of
transthyretin
especially
affecting
heart.
oder
emnaed
ATTR
PROTEIN
D
dayss
membranes,
bu
newer
ers
ave
Morphology. argey
Aggregation
C
B
Fig.
Protein
chains
s
Exraceuar
deposs
o
amyod
may
be
presen
n
probem.
vruay any parencyma organ. In roune secons, ey appear as
•
L ocazed
amyodoss.
e
prmar y
and
secondar y
amyodoses
pnk, gassy, aceuar maera, oten n vesse was. Deposs can be descrbed
earer
are
sysemc
n
naure
and
afec
many
ssues
dsngused and
ses.
By
conras,
n
some
cases
e
amyod
deposs
are
mpars ed
o
a
snge
organ
or
se
(e.g.,
skn,
ung,
ongue).
A
eas
a
may
•
ocazed
us
Amyod
paens
s
be
of
(n
a
orms,
er
In
a
pro du c e d
amy o d,
are
Unke
es e
n
o d
n o )
acd
or
o
e
Bu
n
ear,
e
e
any
are
agng
n
s
e
a
n o ,
p ar c u ar
amyod
s
and
by
e
Congo
yeow-green
red
san,
wc
brerngence
(Fg.
o
e
4.18).
and
as
a
wd
In
e
p ar c u ar
a
d e e r m n e s
w y
edery
cases
ere
resrcve
o
rans-
ype.
re sp ons b e
mpy ng
c a s e,
afecs
many
comprsed
s e qu e n c e.
c a n
AL
presenng
amyod
su g ge s
g
and
ransyren
u nu su a
o e rs
o
subsances
coor
amyodoss.
w
eges)
orms,
an
d a a
o
prmar y
amy o d o s s ,
as
an d
s e qu e n c e
u n k n ow n .
and
o
ama
yp es
or m .
o
consss
assocaed
Bocemcay,
e x p e r m e n a
br s
s
sevenes
n
e xc e ss
amy o d o ge n c
am n o
Amyod
nvovemen
cardomyopay.
yren.
amyod
manesaon
agng.
domnan
e
oer
caracersc
n
deposs some
rom
m-
proe n
e
o
s
AL
c a ns
pr m ar y
w e er
amy o d
organ
resu
Features.
were
rom
(congesve
cas e
g
Clncal
amy -
or ms
( or
he
n
poor,
Amyod
he
o
n
aure),
he
e
and
amyodoss
prognoss
parcuary
nereres
deposed.
deposon
ear
dagnoss
ssues.
s
ose
o
w
mos
kdneys
depends
sysemc
norma
on
rac
o
e
compcaons
syndrome),
ear
(maabsorpon).
demonsraon
w
AL
uncon
cnca
(neproc
gasronesna
ndvduas
w
e
requen
sysemc
amyodoss.
o
amyod
amyodoss
he
course
s
o
reacve sysemc amyodoss depends on e conro o e underyng
condon.
62
CHAPTER
Diseases
4
of
the
Immune
System
A
B
C
Fig.
the
4.18
walls
observed
by
the
Amyloidosis.
of
blood
by
a
polarizing
massive
Courtesy
Medical
Dr.
(A)
vessels
section
Worrell
Dallas.)
along
of
and
of
liver
stained
sinusoids.
microscope.
accumulation
Trace
School,
A
and
(C)
In
amyloid.
Sandy
(B)
with
Note
the
kidney,
The
stain,
Hinton,
Congo
the
the
red
glomerular
called
Department
reveals
yellow-green
a
of
PAS
pink-red
architecture
stain,
Pathology,
deposits
birefringence
reveals
is
of
the
almost
totally
glycogen-rich
University
of
of
Texas
amyloid
deposits
in
when
obliterated
deposits.
(B,
Southwestern
5
Neoplasia
O U T L I N E
Definition
Benign
of
and
Neoplasia,
Malignant
Nomenclature,
63
Hallmarks
Neoplasms,
Benign
Nomenclature
of
Malignant
of
Benign
Differentiation
of
Invasion,
Metastasis,
Molecular
Cancer
of
Role
of
of
Neoplasia,
Saes.
of
of
feared
death
a
cancer
both
deas
1.69
were
of
n
and
o
Cancer
and
remains
reamen,
morbdy
new
n
boog y
ras
moray
cases
2017
second
n
o
e
srkng
mass
e
cancer
and
the
adults.
undersandng
recorded
ony
n
o
counr y.
sudy
cardo-
and
Uned
ay
e
cancer
neo-
and
over
o
Our
sudy
pologc
oowed
and
e
e
o
ogos,
by
a
dscusson
common
so-caed
and
DEFINITION
Neoplasia
cells
that
because
In
a
se
o
posed
ce,
ons
the
cause
and
and
o
bologc
a
bass
magnan
we
and
neoplasms.
moecuar
by
Fnay,
dagnoss
of
reaed
dscuss
mor-
hs
o
s
cancer
neopasms,
e
cnca
cancer.
neopasa
sur vva
are
ce
o
e
(descrbed
be
clonal
a
proliferation
control
gven
a
ces
of
mechanisms
sas
81
Enabler
of
as
Malignancy,
an
83
Enabler
83
of
Tumors,
of
83
84
Cancer,
84
85
rom
cona
o
neopasms
n
genes
ereby
a
are
rom
snge
orgn
a
sares
n
are
snge
progen-
he
mua-
reguae
conerrng
e
ce
mos
neopasms,
a
umor
caed
o ”).
aso
er
(rom
oncoog y
he
may
aby
e
produce
tumere,
e
a
nered.
o
L an
(rom
muaons
be
Greek
cause
We
w
a
o
ocazed
swe).
oncos,
neopasms
reurn
o
he
“umor, ”
are
e
usu-
ssue
o
aer.
begn
ssues
e
s
o
ceared,
AND
do
not
neoplasms
to
are
mcroscopc
ormones
e
uerus
mpes
compee
generally
a
response
s
o
sweng
pror
o
yperpa-
enargemens
and
pregnancy.
node
o
n
resu,
ncude
durng
revers
as
medaors
Lymp
to
inltrate
distant
dened
o
a
a
are
from
as
e
Unke
abaes
sae
o
uerus
neo-
as
ater
an
dev-
gven
a
surgca
well
and
e
w
remova.
of
origin,
are
easily
whereas
malig-
tissues
and
have
the
(metastasize).
umor’s
umor
circumscribed,
surrounding
sites
o
NEOPLASMS
their site
bengn
appearance
predcve
Bengn
o
yperpasas
reversbe:
spread
often
spread
Neopasms
s
and
sgnas;
nlammaor y
MALIGNANT
and
•
are
o
smuaneousy
grow
eus.
neoplasms
wc
by
gesaona
excised,
and
proerae
Exampes
caused
Benign
capacity
o
paopysoogc
yperpasas
necon
o
or
poycona.
response
pasas,
com-
a
o
as
cancer
ssues
ympod
nant
neopasm
derved
orgn
uncon
aer),
an
In conras o neopasa, yperpasa occurs wen many ces wn
er y
aberrations.
er
o
a
wn
ndcang
sad
aer
to
growth
“dauger”
B ecause
ces
refers
genetic
ever y
79
80
Neoplasia,
s
bu
and
BENIGN
normal
muaons,
ce.
neopasc
denng
malgnan
sared
cancer. ”
from
nsances,
oundng
genec
are
growth)
acquisition
a
genecay
a
grow
new
“escaped”
paogenc
o
aberran
or
of
vruay
o
e
and
NEOPLASIA
(literally,
have
e
a
aboraor y
OF
w
bengn
o
eaures
“amarks
manesaons
begns
o
o
“sudy
acqured
muaons
Incdence
5.1
neoplasa
caracerscs
(Immortality),
80
Inflammation
Staging
umors
pysoogc
Fg.
and
propery
ed,
n
of
Effects
reerred
afeced
presened
79
Surveillance,
as
75
73
neoplasia,
mon
Instability
74
Signals,
77
Potential
Metastasis,
Immune
Diagnosis,
daa or e mos common orms o cancer, w e major kers den-
are
and
Aspects
Grading
72
children
progress
cause
71
Cancer,
Death,
Malignancy,
Clinical
Mutations,
dagnoss
as
of
Clinical
Directed
70
in
Cell
Metabolism,
Angiogenesis,
of
Signals,
Growth-Inhibitory
Tumor-Promoting
70
Process
form
in
69
73
Growth
Replicative
Sustained
Mutations,
Passenger
er
dsease
of
Limitless
Genomic
Cancer,
Agents
Approxmaey
600,000
in
Evolution,
most
n
66
66
Mutations,
Multistep
consderabe
and
vascuar
Evasion
Neoplasms,
69
“Driver”
Carcinogenic
cause
Despe
pasms
A
Infectious
the
leading
64
to
in
Cellular
Invasion
Alterations
Significance
Cancer,
Tumors,
Malignant
Neoplasms,
and
Darwinian
Origin
Altered
68
Carcinogenesis:
by
and
64
Evasion
Genes
Epigenetic
Tumors,
68
Basis
Cancer,
Insensitivity
of
Characteristics
of
Self-Sufficiency
64
Nomenclature
Local
63
magnan
proeraon
probabe
reman
Afeced
based
cnca
ocazed
paens
on
e
(descrbed
gross
aer),
beavor.
and
s
amenabe
generay
sur vve,
bu even “bengn” umors may occasonay cause serous morbdy
63
64
CHAPTER
A
2019
ESTIMATED
Men
Melanoma
of
the
Neoplasia
5
CANCER
INCIDENCE
870,970
Women
BY
SITE
AND
B
SEX*
2019
891,480
7%
5%
Men
CANCER
321,670
DEATHS
Women
BY
SITE
4%
the
Brain
skin
4%
Thyroid
13%
Lung
and
24%
bronchus Lung
23% Esophagus Lung
and
13%
bronchus
and
bile
Pancreas
30%
3%
Breast
3%
Kidney
3% Colon
7%
bronchus
5%
and
and
4%
and Liver
bronchus
Kidney
SEX
282,210
3% of
cavity
AND
Melanoma
skin
Lung
Oral
ESTIMATED
Kidney
3%
Pancreas
7%
Colon
Pancreas
15%
Breast
4%
Liver
8%
Pancreas
8%
Colon
duct
and
9%
9%
and
rectum 7%
rectum
Colon
rectum
and
Urinary
rectum Urinary
4%
7%
4%
Uterine
5%
Ovary
corpus
bladder bladder
Prostate
20%
Leukemia
4%
Non-Hodgkin
5%
7%
Uterine
3%
Ovary
4%
Non-Hodgkin
other
Prostate
10%
Leukemia
4%
3%
Leukemia
Non-Hodgkin
4%
3%
Non-Hodgkin
lymphoma
lymphoma
lymphoma
All
corpus
sites
21%
23%
Fig.
cell
5.1
Estimated
and
Cancer
squamous
Facts
and
cancer
cell
incidence
skin
Figures
All
cancers
2019.
other
and
and
sites
death
in
American
situ
All
rates
by
site
carcinomas,
Cancer
other
Society.
lymphoma
sites
and
sex
except
24%
in
the
those
24%
United
of
States.
urinary
Excludes
bladder.
All
other
sites
basal
(Adapted
from
www.cancer.org/research/cancer-facts-statistics/
all-cancer-facts-figures/cancer-facts-figures-2019.html )
or
even
crca
•
moray,
organ
Mag nant
cen
n
de a .
cers
s
ssues
or
(e.g.,
appe d
and
exampe,
e
o
(der ve d
rom
ra ve
g row
ad ere
g y,
e
c aus es
pursue
a
de ad y
a s o
among
e
L a n
a
mos
a
oca
o
c urabe,
or
mass
efec
ono
b eav or.
s ome
e
o
and
des roy
u maey
reer re d
“crab”)
“g rab”
and
nvade
s es ,
co e c vey
word
crab’s
cours e
c an
d s an
are
em
o
a
o
umors
sm ar
cers
causng
n
a
5.2).
b e c aus e
nor ma
mos
desg na on
as
can-
er
n -
ssues
A oug
e
o
no
a
and
s
he
a
are
nens:
(1)
neopasc
connecve
cussed
n
depends
aso
on
uae”
ssue,
e
no
e
n
bengn
and
ces
bood
on
naure
order
o
o
and
(2)
vesses,
Hamarks
ony
magnan,
o
Cancer
nrnsc
e
sroma
er
composed
nonneopasc
and
e
avor
a
are
secon,
e
response,
grow
and
ces.
beavor
o
e
wc
wo
sroma,
nlammaor y
properes
o
bengn
made
As
o
w
a
umor
ces
poypod
s
used
or
grows,
bengn
umors,
parcuary
n
e
some
gu.
umors
up
be
Tabe
5.1),
umors
w
essenay
ceran
addons
oows
and
a
o
excepons:
S arcomas
er
subdvded
ose
•
o
ound
on
and
sod
ces.
Caper
he
ncude
o
ce
ype
or
are
nvove
ssues.
ssue
ces
ces
mos
are
gve
rse
nvove
smar
node
rom
bood
marrow
(ymp
resembe.
derved
o
o
desgnaed
cosey
neopasms
a
ssues
dferenaon.
o
Sarcomas
ey
preerenay
ympod
and
composed
magnan
progenor
Leukemas
grow
and
and
and
bood,
speen)
9).
resembe
neopasc
paerns
neopasms
ympomas
ransormed
usuay
on
mesencyma
norma
and
ympomas
(see
e
n
e
based
magnan
emaopoec
mmune
“manp-
are
Leukemas
e
bu
sur vva.
(see
Tumors
magnan
•
ds-
ces
Malignant
o
Carcnomas are magnan neopasms o epea ces, and are ur-
neopasm
neopasc
commony
as
•
re d
compo-
of
nomencaure
based
umors,
erm
begn
Nomenclature
c an-
ag g ress ve
mag nant
s
umors
adj a -
resu ng
ag .
A
Aoug
magnan
esons
me as asze
Ma g nan
by
bran).
e
ces
ces
n
ces
oow
peomorpc
a
o
a
neopasm,
snge
more
adenoma
an
o
weer
neage.
one
e
In
ne
bengn
some
o
savar y
or
magnan,
umors,
owever,
dferenaon.
gand,
a
cassc
hese
mxed
NOMENCLATURE tumor,
The
nomenclature
each
are
name
related
of
carries
to
the
various
with
it
biology
neoplasms
certain
of
the
is
associated
neoplasm
important
because
characteristics
and
its
likely
that
clinical
behavior.
of
Benign
Tumors
Mos bengn umors are desgnaed by aacng e suix “
ype
rom
wc
e
umor
arses
(Tabe
5.1).
Oers
oma” o e
ave
names
a relec er grow paerns. A papoma s a bengn epea neo-
pasm
growng
nger-ke
surace,
as
conss
o
on
a
surace
projecons.
n
e
gu,
A
o
a
poyp
orm
produces
s
a
a
mass
mcroscopc
a
projecs
macroscopcay
or
macroscopc
above
vsbe
a
mucosa
srucure
(Fg.
(aoug
magnan
nosarcomas,
wc
componens.
Nomenclature
ce
wc
cona)
s
comprsed
o
neopasc
epea
and mesencyma eemens (Fg. 5.3). Uncommony, magnan umors
o
rom
opoena
ce
bng
dferenaon
ype
many
Some
above
oma,
and
dferen
garng
may
be
anoer
ces
a
conan
dferen
bo
ype
ave
neages,
suc
mesencyma
o
umor
eFg.
e
5.1).
a
and
o
arranged
as
carc-
epea
sows
Teraomas
capacy
apazardy
mupe
orgnae
dferenae
eemens
no
resem-
ssues.
nconssences
noed
meanoma,
neopasms.
s
o
(Suppemena
germ
may
rom
composed
Teratoma
nes
any
eemens
are
n
and
Tabe
n
5.1.
semnoma
e
For
namng
exampe,
“sound”
convenons
ympoma,
bengn
bu
are
a
ad
ou
mesoe-
magnan
CHAPTER
A
5
Neoplasia
B
Supplemental
of
hair,
glands,
eFig.
sebaceous
fat
cells,
5.1
(A)
material,
and
a
tract
Gross
and
of
appearance
tooth.
neural
(B)
tissue
A
of
an
opened
microscopic
(arrow).
cystic
view
of
teratoma
a
similar
of
the
ovary.
tumor
Note
shows
the
skin,
presence
sebaceous
64.e1
CHAPTER
Table
5.1
Tissue
of
Nomenclature
Connective
of
One
tissue
Parenchymal
and
Cell
Benign
Malignant
Lipoma
Liposarcoma
Type
derivatives
vessels
Chondroma
Chondrosarcoma
Osteoma
Osteosarcoma
Hemangioma
Angiosarcoma
Mesothelium
Brain
Mesothelioma
coverings
Meningioma
Hematolymphoid
Smooth
Epithelial
of
Leiomyoma
skin
lining
of
or
meningioma
Leukemias,
squamous
cells
Invasive
cells
muscle
Stratified
Basal
65
Tumors
Origin
Composed
Blood
of
Neoplasia
5
Squamous
cell
papilloma
Squamous
adnexa
glands
or
Basal
ducts
lymphomas
Leiomyosarcoma
Adenoma
cell
cell
carcinoma
carcinoma
Adenocarcinoma
Papilloma
Cystadenoma
Liver
cells
Urinary
Hepatic
tract
Placental
epithelium
(transitional)
epithelium
Testicular
epithelium
adenoma
Urothelial
Hydatidiform
(germ
Hepatocellular
papilloma
Urothelial
mole
Choriocarcinoma
cells)
Seminoma
Embryonal
Tumors
of
melanocytes
Composed
Salivary
of
More
Nevus
Than
carcinoma
carcinoma
One
Neoplastic
gland
Cell
Malignant
Type:
Mixed
Pleomorphic
Tumors,
adenoma
(mixed
Usually
tumor
of
Derived
salivary
from
gland)
One
carcinoma
melanoma
Germ
Malignant
Cell
mixed
Layer
tumor
of
salivary
gland
Renal
anlage
More
T otipotential
Fig.
5.2
colonic
Wilms
Than
One
cells
Colonic
lumen
in
Neoplastic
gonads
polyp.
and
is
This
or
in
Cell
embryonic
glandular
attached
to
Type
the
tumor
Derived
rests
Mature
(adenoma)
mucosa
by
a
from
More
teratoma,
projects
distinct
stalk.
into
Than
One
dermoid
the
Germ
Cell
Layer:
cyst
Immature
Fig.
5.3
and
myxoid
present
tumor
Teratogenous
Mixed
in
Brigham
tumor
stroma
this
and
field.
of
the
forming
parotid
(Courtesy
Women’s
gland.
cartilage
of
Hospital,
Dr.
and
Vicky
Boston.)
teratoma,
Small
bone
Jo,
teratocarcinoma
nests
(an
of
epithelial
unusual
Department
cells
feature)
of
are
Pathology,
66
CHAPTER
Neoplasia
5
Endometrium
Fallopian
tube
T umor
Vein Ovar y
BENIGN
MALIGNANT
(Leiomyoma)
(Leiomyosarcoma)
Small
Noninvasive
Large
Well
Nonmetastatic
Poorly
Well
Rapidly
demarcated
Slow
growing
differentiated
Locally
demarcated
growing
hemorrhage
Fig.
5.4
similar
Comparison
origin
CHARACTERISTICS
OF
between
a
benign
tumor
of
the
myometrium
with
and
(leiomyoma)
invasive
Metastatic
Poorly
differentiated
necrosis
and
a
malignant
tumor
of
(leiomyosarcoma).
BENIGN
AND
MALIGNANT
NEOPLASMS
Most
on
benign
the
invasion,
In
s
and
evaluation
and
mos
made
nsances,
w
e
remarkabe
crera.
o
bengn
and
as
an
he
tumors
features:
can
be
degree
are
of
usng
a
of
distinguished
based
differentiation,
n
o
usng
Fg.
bengn
versus
ong-esabsed
usuay
neopasms,
summarzed
Differentiation
Differentiation
deermnaon
accuracy
eaures
magnan
exampe,
their
three
local
metastasis.
anaomc
ble
malignant
of
5.4
perm
umors
and
e
o
magnan
cnca
and
dferenaon
e
descrbed
myomerum
n
dea
nex.
Neoplasms
refers
to
parenchymal
the
cells
extent
of
to
origin,
which
both
tumor
cells
resem-
morphologically
and Fig.
5.5
Pleomorphic
malignant
tumor
(poorly
differentiated
sarcoma).
functionally. Note
In
ces
genera,
a
bengn
cosey
magnan
neopasms
magnan
naure.
o
be
neopasms
resembe
anapasc,
er
exb
Tumors
a
are
a
s
a
o
we-dferenaed
counerpars.
morpoogc
composed
eaure
composed
norma
o
By
aeraons
conras,
a
undferenaed
reabe
ndcaor
o
beray
ces
mos
er
are
the
nuclei,
rell,
ical
marked
and
the
magnancy.
•
Nucear
mupe
dferenaed
oowng
•
e
ces.
exampes
or
and
Anapasc
uncona
ces
oten
caracerscs
dspay
one
or
o
norma
more
o
szes
(varaon
ncude
negbors,
severa
umor
w
nuce.
n
ce
gan
eac
sze
ces
and
a
possessng
sape;
are
Fg.
5.5).
consderaby
eer
one
Exreme
arger
enormous
n
nucear
nuclear
giant
sizes,
cells.
University
nuceo.
ncudng
sze
•
a
approac
of
the
hyperchromatic
(Courtesy
Texas
Dr.
Trace
Southwestern
Wor-
Med-
ar
nuceus
•
e
ypercromasm
sape,
rao,
o
unusuay
nuce
and
dameer
or
o
may
nuceo
norma
(dark-sanng),
promnen
resu
may
n
an
aan
snge
or
ncreased
asoundng
ympocyes.
Atypca mtoses, wc may be numerous. Abnorma separaon o
cromads
an
and
Enargemen
nucear-o-cyopasmc
e
eaures:
Peomor psm
er
srucura
and
tumor
Pathology,
abnormates,
aon,
o
of
cell
Dallas.)
varaon
oss
of
in
sad
Anapasa eray means “backward ormaon, ” mpyng dedferen-
or
presence
Department
School,
variation
moc
L oss
of
durng
gures
poar ty,
p aer ns
o
ce
(Fg.
suc
dvson
may
produce
rpoar
or
quadrpo-
5.6).
a
or en a on
g roups
o
one
o
ne op as c
ano e r.
In
ce s
e
ack
mos
nor ma
anap as c
CHAPTER
umors,
nze d
ce s
g row
s r uc ures
n
Neoplasia
5
d s organ ze d
suc
as
g ands
se es,
or
w
s ra e d
67
o a
oss
s qu amous
o
orga -
arce c -
ure.
We - d e re n ae d
ona
c ap ab e s
p as c
u mor
re g ard ng
c e s
u mor
e
In
and
o
and
5.6
High-power
nuclear
field
has
an
variation
detail
in
abnormal
view
size
of
and
tripolar
anaplastic
shape.
The
tumor
cells
prominent
shows
cell
in
nsu n ,
cellular
the
( AC T H ) ,
g u c agon ,
p ar ane op as c
center
Dysplasia
spindle.
mal
but
is
not
o
c e
s y nd rome s
disordered
do
re a n
e r
c e
ana -
ae r,
ne op as ms
re qu e n y
o
c aus e
or g n .
pro du c e
e me rge.
s g ns
su c
as
s
s a d
S m ary,
ke r a n
(F g .
s e c re e
Mo s
and
and
e ab o -
b e.
no aby,
s y mpoms
by
a d re no c or c o rop c
or mone - re ae d
More
u nc -
( d s c uss e d
c arc nomas
u nc ons
may
so
e
w e re as
b engn
c arc nomas
or mone s ,
o e rs .
o
g ands
e p ao c e u ar
p ar a y ro d
and
o
e x amp e,
or g n
e c op c
key
c ou ne r p ar s ,
e nd o c r ne
u nan c p ae d
none nd o c r ne
are
key
car a c e r s c
s o-caed
or mone
Fig.
For
s qu amous
ns anc e s ,
s e c re ng
e ss
o
we - d e re n ae d
o e r
c anc e rs
mu c
c anc e rs
or mone s
c e s
nor ma
g r a d ng ) .
we - d e re n ae d
5.7)
e r
are
we - d e re n ae d
r ae
u mor
o
proe n
ab ou
e s e
( P Tr P ) ,
s o-caed
ae r.
growth
of
epithelial
cells
that
are
abnor-
malignant.
Dyspasa s mporan o recognze because s a we-documened
precursor
rum,
pasa
•
o
and
ncude
Ceuar
may
•
carcnoma
e
and
arge,
•
ey
e
tumor
with
cells
are
intercellular
strikingly
bridges
similar
and
to
nests
normal
of
of
squamous
keratin
the
skin.
epithelial
superca
no
e
are
ypcay
n
o
sraed
5.8
Carcinoma
dysplastic
cells
subepithelial
nuclear
and
in
situ.
lacking
stroma.
cellular
(A)
orderly
(B)
Low-power
view
differentiation.
High-power
pleomorphism,
view
and
of
shows
The
usua
progressve
canges
e
are
sage
prog resson
a
cancer
as
and
the
region
mitotic
endome-
assess
dys-
orm
o
abnor-
epeum,
b eng
a
n
e
sraed
badder,
basa-appearng
nvove
o
compeey,
as
ces
n
o
as
e
entire
thickness
membrane
shows
figures
is
of
intact
a
cancer
s
no
p ar c u ary
genera
ncre as e d
failure
of
extending
the
and
normal
toward
ces.
enre
carcnoma
squamous
resung
Wen
ckness
n
su,
a
n
a
dys-
o
e
prenva-
5.8).
dyspasa
Ne ver eess,
ssue
dark
reerred
(Fg.
o
reg ress
s
o
epeum
o
severe
eson
he
may
o
mauraon
ransona
sve
basement
another
numerous
that
e
squamous
r u e,
r sk
e
or
ne v abe,
nc ng
pres ence
de veopng
B
Fig.
o
seen
cancer.
A
cer vx,
used
nuce
ayers
normay
odgepodge
marks
cells,
(arrow).
n
dsordered
remove d
The
peomor psm,
or
pasas
carcinoma
nucear
are
epeum,
cell
as
a
oowng:
epeum
pasc
squamous
suc
Feaures
Arctectura dsarray. Exampes ncude e para or compee oss
o
Well-differentiated
ssues,
rac.
ypercromac
moses
were
5.7
many
Abnorma mtotc actvty, ncudng more numerous moc gures
and
Fig.
n
gasronesna
epithelium
there
is
no
consists
tumor
differentiation,
the
surface.
in
of
the
marked
and
dys-
caus es
o
are
dyspasa
an
nvasve
68
CHAPTER
Neoplasia
5
A
B
Fig.
5.9
from
Fibroadenoma
the
tumor
Texas
whiter
from
the
of
breast
the
tissue.
surrounding
Southwestern
breast.
(B)
The
tan-colored,
Microscopic
tissue.
Medical
(A)
(B,
School,
encapsulated
appearance.
Courtesy
Dr.
Trace
The
fibrous
Worrell,
5.10
causing
breast
ogy,
that
As
son
on
and
University
ductal
carcinoma
retraction,
of
umors
umors
bross,
may
a
by
are
Invasve
fat
by
Texas
and
sowy
grow
(Fg.
sroma
dscree,
can
sowy
and
nests
is
of
the
breast.
stony-hard
and
cords
Southwestern
of
on
tumor
Medical
(A)
The
lesion
palpation.
cells.
School,
(B,
(B)
infiltrates
Courtesy
demarcated
sharply
delimits
of
Pathology,
the
University
of
Dr.
surrounding
view
Trace
breast
illustrates
Worrell,
the
substance,
invasion
Department
of
of
Pathol-
Dallas.)
be
cancers
and
5.9).
ces,
a
s
sroma
a
usuay
on
o
depo-
encap-
easy
o
assocaed
gross
nspec-
he
bood
vesses,
unes
newy
an
or
sma
hs
nrave
an
ssue
umors
surgca
excson
dsngusng
eaures
emangomas)
ack
are
o
no
capsues
a
magnan
absoue:
and
are
no
umor
Some
s
aemped.
bengn
dscreey
umors
dened.
hese
(e.g.,
spread
occu
cancers,
asze
o
measac
the
tumor
cancer
as
may
ner vous
hus,
poena.
be
ce
e
tumor
perms
and
body
umors
evden
are
a
more
em
sites
and
that
the
are
ability
key
assocaed
sysem,
o
me
are
w
o
o
s
o
cancers
and
an
and
aways
In
bu
dsease.
mos
aggressve
no
w
oer
addona
dagnoss.
measasze,
skn
no
oppor-
paens
skn
measac
e
ocay
nvade
o
penerae
provdng
30%
measases,
e
o
caves,
(excudng
carcnoma
aby
to
tumor
malignant.
measases
cancers
a
Approxmaey
sod
cncay
basa
cenra
rarey.
as
of
primary
ces
5.11).
(dden)
umors
the
cannes,
(Fg.
ave
spread
with
magnan
suc
e
ony
a
o
anapasc
prmar y
grow necessaes remova o a wde margn o surroundng “norma”
by
ympac
meanomas)
nrae,
5.10).
marks
dagnosed
arge,
(Fg.
dened
nvasveness
era,
ssues
is
discontinuous
metastasize
appear o be crcumscrbed, ack rue capsues and progressvey nvade,
surroundng
ose
to
ave
desroy
even
Metastasis
physically
rm
by
Bengn
response
cancers,
feature
tumors.
deveop
and
umors
However,
the
ormed
brobass.
magnan
encapsuaed.
mos
capsue
as
is
benign
(nonxed),
nduce
growng
from
expand,
he
suc
movabe
aso
invasiveness
20%
wen
the
Microscopic
a
and
o
metastases,
capsue
cancers
appear
of
distinguishes
caed
coagen
sharply
Metastasis
reliably
ssue
o
excse.
stroma
development
bengn
suaed
w
the
most
brous
Invasive
tissue
Invasion
to
Department
is
(right)
B
Fig.
Next
tumor
capsule
Dallas.)
A
Local
small
gen-
even
Cer-
prmar y
bu
meas-
predcve
o
CHAPTER
MOLECULAR
BASIS
Cancer
and
All
of
Genes
forms
genes
cer
s
o
ave
consder
liver
studded
with
metastatic
even
a
caed
ways.
cancer.
or
cancer
number
or
cancer
are
a
e
ce
cells.
genec
dsease.
Genes
hey
are
a
One
a
our
Mos
suicen
genes
o
n
as can-
numerous
dicu
compexy
uncona
or
recur-
o
are
s
casses:
muaed
ranscrpon
progrow
because
produce
pro-
counerpars
encode
parcpae
function
are
ony
ceuar
oncogenes
a
a
a
smpy
norma
domnan
s
no
names
major
the
reerred
overexpressed
her
moecues
o
be
are
or
way
no
can
and
acronyms
grow.
aee
ces
undreds
consdered
snge
cancer
wen
protooncogenes.
alter
normal
exper.
a
that
of
n
genes
genes
sgnang
nvovng
s
n
e
mutations
behavior
dysreguaed
ncreased
acors
the
Mutations
from
unpronounceabe
O ncogenes
are
A
or
hese
oten
moe
5.11
essence,
remember,
•
Fig.
regulate
muaed
genes.
bu
o
n
stem
69
NEOPLASIA
“Driver”
neoplasia
that
hus,
reny
of
OF
Neoplasia
5
a
a
pa-
muaon
prooncogenc
efec.
Magnances
ca
a
o
crcumsance:
crcuae
hereore,
e
roug
w
dssemnaed
bood
hese
ony
e
are
excepons,
a
and
derved
boodsream
rare
dseases
(eukemas
umors
dagnoss
ympomas)
rom
and
spe-
ces
mgrae
eukemas
and
a
bood-ormng
are
o
and
aways
are
dsan
ympomas
consdered
S eedng
wtn
cuary
and
peronea
sysem
e
orms
he
e
dranage.
o
A
cancer
•
e
and
ree
mode
o
ceran
neopasms
e
adjacen
s
oten
o
e
ependymoma)
roug
suraces
wc
e
bran
may
e
Aoug
may
“sentne”
ymp
node
wc
a
or
cause
w
n
y mp
o
afeced
node
s
a
are
may
e
by
node
bopsy
rs
o
o
aso
tat
are
cers.
e
o
on
regona
gauge
Lymp
e
reacons
enargemen
and
ymp
umor
reamen.
spread
node
umor
can
ony
sopaoogc
o
node
resus
o
deer-
encode
are
•
ar eres
ces
and
are
are
oten
e
sysem
o
e
o
w
exampe,
e
b ones.
are
o
o cazaon
w oy
and
g
carcnomas
omc
no
e
e
expan
ung
bran,
C onvers ey,
rarey
ses
o
near
e
a
e
o
yrod
vae
•
an
Large
•
ends
and
umor
roug
s
Cromosome
(Fg.
s
o
spre ad
oten
mus ces,
measas es.
o
e
spreads
aoug
proen.
an
n
cnomas,
as
due
o
a
umor
o en
suppressor
grow.
ac
by
en ancng
p er
s e.
overex press e d
ap opo ss
end
o
n
be
ce
G enes
c anc er
und erex-
tumor
genes
os
a
Mos
a
and
n
enance
mmune
or
drver
encode
ces
aered
ost
ces
ceran
or
can-
nb
e
sysem.
progresson
muaons
reguaor y
o
cancers
afec
RNAs,
genes
suc
as
and
ncude:
and
sma
nsertons
and
deetons.
as
a
g ands
s
In
a
requeny
umor
suppressor
remove
an
oer
one
oncogene,
nsances,
or
proen.
more
cancers
o
and
orm
e
genes
o
w
oncogenes,
o
(eer
rear-
promoer
o
gene
a
composed
o
may
s
creaed
porons
rearrangemens
bu
a
sruc-
e
overexpresson
cmerc
sarcomas,
cromosome
cromosome
eemen
eadng
a
proen
ypes
e
n
nvovng
reguaor y
uson
hese
n
canges
nsances
srong
near
In
(oten
gross
some
a
bood
represen
anoer
acvy
an
abnorma
meapase
or
may
DNA
be
ncrease
he
genec
s
w
wn
p or ons
speca
ab erraon
dened
e
as
ereo
eve
amped
ragmens
presen
cromosome
wc
arge
o
5.13).
omogeneous-sanng
common
aneupody,
somes
or
way
(Fg.
exracromosoma
Anoer
and
nacvae
are
be
o
a
wo
parcuary
ound
n
car-
Gene ampcatons produce exra copes o one or more oncogenes
oncogenc
For
or
we.
cromosomes,
capar es,
uncon-
neopasms
pro era on
deveopmen
genes
oncogenc
n
n
preven
n
uncon.
proens.
can-
ver
e
produce
enancer)
ana-
e
ce
between
e
mutatons.
wc
paces
common
and
paens
adrena
os
unconay
are
by
substtutons
5.12).
e
o
r c
•
proba-
me as as es.
or
rearrangements
dranage
Howe ver,
venous
o
n
rs
oten
an
dferen
p or a
coumn
dverse
suppressor
encodes
umor
e
ces
bu
oncoproen
norma
encouner :
pa way
me as as es
pros ae.
and
we.
me as asze
ver ebra
dsrbuon
neurobasoma
skeea
e
e y
are
nteractons
promoe
ransocaons)
ck-waed
Bo o d-b orne
oten
pexus;
as
aees
pr mar y
promoe
muaed
drver
deetons,
umor
examnaon
cours e,
an
b ed
spread
ver ebra
neopasm
sysemc
spread.
cancers
paraver ebra
carcnoma
and
oer
s
easy
capar y
requeny
requenc y
o
o
rs
arsng
oow
more
avenue
e
w ereas
C ancers
roug
expans
n
cancers
ver,
ungs.
emb oze
by
e
usua
arresed
Gasronesna
carcnomas
as
srucuray
or
bu
p eneraed
bo
s mu a ng
mporan
Snge-nuceotde
ure
are
by
a
umor
proens,
paway
vens
s
Dependng on er precse ocaon and ype, ese may eer ac-
nodes.
sarcomas,
o
a
rangemen
or
o
unreguaed
ap oposs
os e
reguate
o
Hematogenous spread. Spread roug bo o d vess es s e avored
hn-waed
normay
genes
mcroRNAs, aso can be afeced by drver muaons. Drver muaons
angens.
be
a
suc
apoptos s
agans
Parcuary
reerred
a
va
spread
aow
an
recurreny
Muaons
are
enarge-
measac
o
se
ympac
he
sem
rom
e
oca
umor.
cannes.
uncon
o
reg uate
w ere as
Genes
carcnomas,
ympac
depends
prmar y
mmunoogc
ymp
ypca
paways
used
gudes
umor
cerany
mos
roug
naura
rom
urn
rom
s
nvovemen
e
bopsy
prmar y
ces
and
low
node
s
dssemnae
genes
o
press e d.
•
lud,
or
are
uncon
e
os
ra er
proe c
ce s,
cenra
a
cerebrospna
o
a
par-
spread
be
tat
sur v va ,
dssemnaon
genes
e
nsances,
mus
G enes
paways:
carcnomas,
rave
menngea
ymp
ymp
near
mned
o
hs
o
meduobasoma,
neopasm
ympacs,
hus,
one
ovaran
venrces,
cancer
receves
senne
o
o
suraces,
spread.
o
prmar y
men
gene
recognon
paern
a
mos
be
cord.
Ly mpatc
a
on
by
cavtes.
(e.g.,
cerebra
mpan
spna
•
body
spread
caracersc
ner vous
ener
neopasms
grow;
o dsrupve muaons or epgenec sencng (gene represson). In
are
o
suppressor
roed
•
Magnan
aong
Tumor
ssues.
magnan.
•
•
gans
(s ee
known
a
o
genes
a
proen
may
as
doube
cromosome
regon,
be
deeced
mnue
and
by
w
carred
appear
sanng
dyes.
a
or
s
ound
osses
Caper
o
6).
n
cancer
woe
How
ces
cromo-
s
causes
70
CHAPTER
Neoplasia
5
CHRONIC
NORMAL
MYELOID
CHROMOSOMES
LEUKEMIA
9
22
9
22
HSR
BCR BCR
NMYC
locus
ABL-BCR
locus
hybrid
gene
ABL
oncogene
Tyrosine Tyrosine kinase kinase inhibitor
ABL Activation
of
oncogene growth
factor
signaling
Double pathways
minutes
NORMAL
BURKITT
CHROMOSOMES
LYMPHOMA
8
14
8
14 Fig.
5.13
The
Amplification
NMYC
fied
and
is
gene,
seen
chromosomally
chromosome
other
to
Brodeur
MYC
oncogene
the
as
than
and
activation
gene
in
human
chromosome
chromosome
is
an
Sather
becomes
minutes
region,
NMYC
oncogenic
RC,
human
2.
neuroblastoma.
2p,
double
homogeneous-staining
Seeger
in
on
extrachromosomal
also
GM,
NMYC
normally
integrated
fied
of IG
IG
either
structure
from
of
present
is
et
al:
neuroblastomas.
on
related
factor.
Clinical
Cancer
as
usually
closely
transcription
H,
ampli-
or
a
a
in
(Modi-
implications
58:541,
1986.
gene Reprinted
Increased
by
permission
of
Wiley-Liss,
Inc.,
a
subsidiary
of
John
Wiley
gene MYC
&
Sons,
Inc.)
protein MYC
oncogene
MYC
oncogene
Carcinogenesis:
A
Multistep
Process
Directed
Increased
expression
pro-growth
of
by
Darwinian
genes
Cancers Fig.
5.12
Chromosomal
translocations
and
associated
oncogenes.
are
myeloid
leukemia,
a
balanced
translocation
involving
9
and
22
creates
a
chimeric
gene
containing
pieces
the
BCR
protein
of
with
genes
Even and
ABL
genes
that
encode
a
chimeric
BCR-ABL
fusion
ng constitutively
anced
translocation
sequence
in
the
MYC,
active
for
the
tyrosine
involving
MYC
immunoglobulin
an
oncogenic
kinase
activity.
In
chromosomes
gene
adjacent
heavy-chain
transcription
to
gene,
8
Burkitt
and
strong
leading
14
lymphoma,
places
the
regulatory
to
a
ce,
coding
elements
overexpression
of
factor.
a
A
s
ncompeey
n
mosoma
e
underso o d,
expresson
o
cancer
bu
s
a
b eeved
resde
n
o
nvove
afeced
cro-
oug
ereby
Epigenetic
sion
of
a
Gene
changes
gene
that
expresson
are
Cancer
dened
occur
s
in
as
without
akn
seecve
reguaed
orgn
heritable
mutation
by
changes
of
the
in
the
expres
gene.
posransaona
cancer
pars.
s
How
poory
rom
ces
e
wen
ese
aeraons
undersood,
aered
compared
bu
are
expresson
n
w
e
key
o
er
norma
modcaons
epgenome
n
cancer
mos,
genes.
ceuar
conrbue
no
a,
o
that
by
the
disrupt
stepwise
sets
o
couner-
neopasa
nsances
o
prooncogenic
of
can-
o
s
evove
functions.
naed
rom
genecay
a
(Fg.
snge
5.14),
a
ound-
process
sem
a
o
o
umor
a
ese
prmar y
and
muaons
e
Dar wnan
or
a
seecon,
ypcay
ses
o
genecay
more
come
o
o
umors
n
a
es).
a
B ecause
were
a
e
rom
o
can-
cancer
grow,
resung
e
eerogeneous
resu
dferen
uncon
adep
a
progresson.
o
domnae
measass.
magnan
umor
e
evason,
(sur vva
may
as
beeved
aer
ces
mmune
evouon
o
s
ndependeny
may
afeced
or
subcones
se
reerred
progresson
accumuae
measass,
advanage,
are
penomenon
n
Due
o
umor,
o
sur-
progres-
s
eer
connung
monocona
me
o
n
cnca
presenaon.
Genetic
heterogeneity
gression
but
Wen
sones and by DNA meyaon, bo o wc are requeny aered
n
progress
aberrations
ormaon
eve,
makng
nvason,
e
o
muaons
S ome
muaon
Alterations
umor
connue
moecuar
ces.
son
a
regons.
Epigenetic
subsequently
genetic
complementary
cancers
addona
cer
genes
with
conrbues
e
vva,
canges
and
multiple
bal-
genes,
cancer
of
chromo-
cer somes
initiated
In
acquisition chronic
Evolution
amos
umors
aways
ressance
(or
also
evouon
has
the
recur
ressan
sems
epgenec
for
rom
ater
o
e
by
to
not
orgna
a
dar wnan
only
for
cancer
pro-
therapy.
cemoerapy,
e
ougrow
aeraons)
orged
implications
response
o
mpar
drug
e
subcones
drug
seecon
recurren
regmen.
a
ave
ressance.
can
expan
umor
hs
muaons
hus,
e
s
acqured
genec
wo
mos
CHAPTER
Accumulation
passenger
Carcinogen-induced
Additional
mutation
of
driver
Neoplasia
5
71
and
mutations
driver
Additional
mutations
Emergence
mutations,
of
subclones
Diagnosis
Nor mal
Initiated
cell
stem
precursor
cell-like
with
Founding
proper ties
cancer
cell
Genetically
heterogeneous
cancer
Acquisition Initiating
5.14
order
perncous
properes
become
more
Origin
of
o
in
Development
which
cancers:
aggressve
Further
and
various
e
ess
of
cancer
driver
endency
responsve
through
mutations
or
o
hallmarks
stepwise
occur
cancers
evolution
over
is
accumulation
usually
me
unknown
o
o
erapy.
of
and
an
Carcinogenic
mutations
monly
acquired
Facors
muaons
•
Age.
a
a
In
mos
ors
and
Exposure
w
erapy
par
Some
ca
s
age
an
s
bu
resu
o
(many
cancer
mporan
carcnogens
DNA,
causng
agens
(e.g.,
Some
rsk
o
a
muaons.
e
•
com-
55
arge
somac
w
and
and
par
are
muaona
75.
by
he
e
w
rsng
by
noma
ac-
assocaed
reacons,
resdues
suc
o
damage
agens
hese
cancers,
DNA),
varey
o
are
a
do
DNA
ssues.
as
poen
creae
wo
no
are
•
assoc-
ndvduas),
cemo-
array
o
(oten
n
T abe
groups
casses:
requre
gven
ors)
cemcas.
Major
Carcinogens
and
Associated
Agent
Associated
Tobacco
Lung,
renal
Ultraviolet
light
Skin
e
cancer
Lung,
head
cell
esophageal,
Ionizing
chemotherapy
agents
radiation
Aflatoxin
B
Many
Liver
1
Nitrosamine
Acute
and
nitrosamides
myeloid
and
(n
Cronc
o
o
o
women
as
e
paways.
cyocrome
converson
are
par
cronc
exposed
key
wc
e
o
s
paogeness
drec-acng
occur
may
repar
ncdence
ormones
n
o
be
process.
o
carc-
dsorders
aso
s
asso-
ormone-responsve
g
eves
endomera
o
esrogen
epeum)
Another
con-
ited)
DNA
can
case
o
and
breakage
genes
B
ces)
o
oncogenes
B-ce
important
and
source
reguaed
and
T-ce
of
B
rejonng
o
(mmunogobun
mmunogobuns
creae
mutageness.
and
and
and
angens.
are
mporan
ympo-
T-ce
muageness
or
T
assembe
Errors
o
n
a
vas
recep-
mprove
ese
conrbuors
pro-
o
e
umors.
driver
mutations
is
germline
(inher-
aberrations.
hese
pacng
nered
e
Cancers
neck,
afeced
muaons
are
ndvdua
a
presen
a
g
n
rsk
ever y
or
ce
n
deveopng
e
body,
cancer.
Mechanism
pancreatic,
and
DNA
in
squamous
cell
carci-
damage
tobacco
DNA
caused
smoke
by
carcinogens
(e.g.,
and
procarcinogens
benzo[ a]pyrene)
damage
carcinoma)
gastric,
and
colon
esophageal
carcinoma;
Uncertain.
Activates
inflammation.
leukemia
cancer
(a
over
Cancers
and
o
assocaed
nlammaor y
mogenc
and
o
ncreased
carcnoma
mammar y
more
dvson,
nlammaon
as
e
many
rearrangement
e
o
damage
cancer
cancer,
ceuar
par,
rsk
angen-recepor
a
cancers
Gastric
DNA
cesses
mesothelioma
Alkylating
or
n
aerng
Muaons
and
exposure
eevaed
exampe,
Cem-
(melanoma,
basal
an
reguaed
ainy
carcinomas
noma,
Asbestos
Human
bladder,
seng
Increased
5.2.
meaboc
e
by
suc
carcnogens.
proeraon
eas
meaboc
enzymes
carcnoma.
Reguated
use
zo(a)pyrene, azo dyes, alaoxn), wc are no acve un convered
5.2
For
n
acve
acors.
ceuar
mogen
cyes
radaon
severa
a
endogenous
susaned perods o me ave an ncreased rsk o breas and endo-
verson o become carcnogenc, and ndrec-acng agens (e.g., ben-
Table
w
obacco
envronmena
sed
no
5.3).
caed
ncudng
eecrope
wc
(Tabe
o
proferaton.
expan,
seen
mera
damage
pgmened
reacve
agens),
o
may
by
The
tumor.
endogenous
repcaon
ncreased
hs
o
mutations.
to
carcnogeness
agens
ceuar
by
driver
tumor
carcnogen
nluence
DNA
ncreased
accumu-
expaned
burden
cemca
a
varey
a
may
Increased
w
age,
from
poymorpsms
durng
oowng:
mey-cyosne
gy
wc
gy
akyang
e
most
oncogenc
ncreases
muaons
Agens
carcnogenc
ave
o
ages
n
are
inherited.
respecvey.
o
(n
erapy),
o
and
agents.
g
ncude
cancer
sponaneous
cyosne
ncreased
e
o
expaned
resdues,
function
be
beween
mos
o
also
occurrence
durng
key
mutagenc
drugs
e
occurrng
uravoe
o
o
vary
ndrec-acng
gene
may
requency
beow,
e
cancer
but
muaons.
ymne
to
smokng,
as
w
deamnaon
aed
e
somac
agng
urac
•
o
life
acqured
deas
descrbed
w
e
are
genera,
ncdence
alter
during
conrbue
cancer
aon
that
Mutations
complementary
may
umae
Hence,
P-450
Driver
genetic
mutation cancer
Fig.
of
DNA
damage
DNA
damage
DNA
damage
DNA
damage
the
inflammasome,
leading
to
local
In
72
CHAPTER
Table
5.3
Chronic
Pathologic
Inflammatory
Disorders
Condition
Asbestosis,
and
Cancer
Associated
silicosis
Inflammatory
Lichen
Neoplasia
5
bowel
disease
Colorectal
sclerosis
Vulvar
squamous
Pancreatic
Chronic
Gallbladder
cholecystitis
esophagus
Sjögren
Opisthorchis,
Hashimoto
thyroiditis
Extranodal
cholangitis
Hepatocellular
Osteomyelitis
Carcinoma
ames
ma
w
more
sor
a
gene
afeced
some
ra.
ndvduas
nsances,
cancer
a
preven
provde
Tumor
he
encodng
a
ypcay
LM:
muaons,
nered
acves
genes
us,
n
n
Coussens
mupe
rsk
cause
umor
ceuar
adequae
are
stroma
cancers
mos
acs
suppressor,
a
norma
arse),
e
draining
cancer
an
s
a
n
carcinoma
MALT
a
compeey
emnaes
e
uncon
o
e
w
mutations
pylori
B
and/or
C
virus
infection
Schistosomiasis
a
Ann
Rev
arose
durng
Pathol
n
eary
e
Mech
Dis
germ
1:119,
ces
o
2006.
e
parens
or
occurred
n
e
eus
embr yogeness.
one
Role
suppres-
he
germline
stones
flukes
Helicobacter
Bacterial
development.
auoso-
arses
e.
umor
particles
acid
Hepatitis
of
Infectious
sae;
Infectious
(and,
of
rans-
this,
agents
some
causative
ormed ces ypcay conan a second, sporadc muaon n e norma
aee
Liver
lymphoma
sinuses
germne
T umor
cancer
eary
colon
carcinoma
eerozygous
un
oten
of
proen
ransormaon.
n
in
ke
nsances
silica
lymphoma
carcinoma
regulation
usuay
n
uncon
perecy
and
Gastric
zone
adenocarcinoma,
Bladder
TD,
ese
domnan
muaon
or
Tlsty
Alcoholism,
Gallbladder
Cholangiocarcinoma,
cystitis
fibers,
carcinoma
carcinoma
Hepatitis
from
cell
marginal
Gastric
Chronic
Agent
Asbestos
cancer
Gastritis/ulcers
Adapted
Etiologic
carcinoma
carcinoma
Esophageal
syndrome,
lung
carcinoma
Pancreatitis
Barrett
Neoplasm(s)
Mesothelioma,
cancers
agents
number
o
and
necous
up
can
or by
Epdemoogc
suppressor.
Agents
cause
in
to
be
Cancer
25%
effective
cancers
n
e
worldwide;
through
treatment
mecansc
agens
of
prevented
sudes
eoog y
of
established
ave
o
because
vaccination
rmy
varous
against
infections.
mpcaed
cancers
a
(Tabe
he need or a second (e two-t ypotess) o creae a “procancer”
5.5). Inecous agens appear o ncrease e rsk o cancer roug wo
penoype
major
one
and
suc
as
was
cancer
argey
Imporan
cancers
are
reveaed
caed
ou
borne
g
5.4
e
ou
n
by
Tabe
o
subsequen
5.4.
Presumaby,
Inherited
genes,
many
o
Predisposition
o
n
ese
to
cdren
n
are
are
cdren
new
Disorder
syndrome
(various
tumors)
Melanoma
Familial
adenomatous
polyposis/colon
Neurofibromatosis
1
Breast
tumors
and
Hereditary
Nevoid
ovarian
and
nonpolyposis
basal
cell
pes
aso
ncude
nduce
asso-
ceuar
w-
epas
cronc
ver
carcnoma
2
syndrome
pigmentosum
(ver
and
and
cancer),
epas
are
srongy
C
vrus,
and Hecobacter
Bloom
syndrome
Fanconi
anemia
o
w
pyor, a
wc
epao-
bacerum
a coonzes and damages e gasrc mucosa, wc as been nked
muaons
o e deveopmen o gasrc carcnoma and gasrc ympoma.
Dominant
Cancer
Syndromes
Functional
Defect
TP53
Increased
p16-INK4A
Loss
APC
Increased
signaling
Increased
progrowth
Increased
genomic
instability
Increased
genomic
instability
Increased
signaling
in
Increased
genomic
instability
Increased
genomic
instability
Increased
genomic
instability
Increased
genomic
instability
NF2
MSH2,
BRCA2
MLH1,
MSH6
PTCH1
Recessive
Diverse
genes
Syndromes
involved
in
of
Defective
nucleotide
DNA
excision
of
of
cell
cycle
control
genomic
cell
cycle
instability
control
in
the
Wnt
ATM
BLM
Diverse
links
genes
involved
in
repair
of
DNA
cross-
pathway
signaling
the
Hedgehog
Repair
repair
Ataxia-telangiectasia
bo
assocaed
Loss
BRCA1,
cancer
vrus
RB
NF1,
colon
carcinoma
cancer
B
damage
Cancer
Autosomal
Xeroderma
and
Gene(s)
Retinoblastoma
Li-Fraumeni
mecansms:
By nducng cronc nlammaton and tssue repar, ereby ncreasng
e rae o acquson o drver muaons, as descrbed earer. Exam-
as
Autosomal
Inherited
•
aer),
genes
genomes
even
o
sudes.
assocaed
occurrng
cancer
nerance
(descrbed
moecuar
and
Sequencng
cancers
n
domnan
renobasoma
syndromes
muaons
sor y.
auosoma
ama
cancer
racon
germne
amy
Table
been
ama
a
rom
syndrome,
summarzed
a
w
any
predced
pathway
CHAPTER
Table
5.5
Infectious
Agents
Agent
DNA
Linked
to
73
Cancer
Cancers
Mechanism
Viruses
Human
papillomavirus
(HPV)
Squamous
tonsil,
Epstein-Barr
virus
(EBV)
B
cell
cell
carcinomas
vulva,
and
lymphomas,
of
the
cervix,
Virus
Human
herpesvirus
8
Kaposi
encodes
oncoproteins
that
inactivate
p53
and
RB
penis
nasopharyngeal
Uncertain.
carcinoma
Virus
encodes
proteins
that
activate
oncogenic
signaling
encodes
proteins
that
activate
oncogenic
signaling
pathways
sarcoma,
B
cell
lymphomas
Uncertain.
(HHV8)
Virus
pathways
Hepatitis
RNA
Neoplasia
5
B
virus
Hepatocellular
carcinoma
Uncertain.
Causes
chronic
liver
inflammation
and
associated
repair
Hepatocellular
carcinoma
Uncertain.
Causes
chronic
liver
inflammation
and
associated
repair
Uncertain.
Virus
Viruses
Hepatitis
C
virus
Retroviruses
Human
virus
T-cell
1
lymphotrophic
Adult
T-cell
leukemia
(HTL V1)
T
encodes
proteins
that
causes
expansion
of
infected
cells
Bacteria
Helicobacter
pylori
Gastric
carcinoma,
gastric
B
cell
lymphoma
Uncertain.
lates
a
Causes
chronic
chronic
immune
gastritis
and
associated
repair
and
stimu-
response.
Parasites
Schistosoma
Liver
•
By
haematobium
sood
many
s
e
cases
dscussed
and
te
functon
ceuar
exampe
wc
o
p53
s
ead
aer,
and
Significance
wo
RB,
of
agen
and
HPV
Uncertain.
he
n
neck
e
by
uman
cases
wo
mos
cancer
genes
mporan
squamous
Passenger
inuence
s
mos
encodes
o
made
mos
Uncertain.
and
or
by
bes
papomavrus
o
cer vca
ce
mporan
E6
and
umor
stm-
As
E7,
create
host
response
that
to
the
do
not
cystitis
bile
Avoiding
and
duct
associated
inflammation
immune
Evading
destruction
repair
and
associated
repair
growth
suppressors
w
a
Enabling
replicative
signaling
immor tality
be
bnd
suppressor
alter growth
Sustaining
proliferative
and
pro-
Deregulating
T umor-
cellular
promoting
energetics
inflammation
Mutations
variants
chronic
chronic
(HPV),
carcnoma
carcnoma.
proens,
Causes
Causes
under-
respecvey.
Passenger mutations
but
protens
mecansm
eoogc
o
of
proferaton.
nacvae
ens,
carcinoma
Cholangiocarcinoma
aterng
uatng
erties
Bladder
flukes
prop-
tumor.
Activating
hey
greay
ounumber
drver
muaons,
parcuary
n
cancers
Resisting invasion
caused
by
exposure
o
muagens,
suc
as
mos
meanomas
and
cell
smok-
and
death metastasis
ng-reaed
passenger
•
ung
Passenger
tance
rare
cancer.
muaons
to
are
mutatons
terapeutc
ces
evenuay
o
may
er
n
create
agents.
arborng
come
Despe
mporan
genetc
Under
ressance
domnae
appareny
severa
e
seecve
umor
naure,
ce
tat
confer
pressure
gan
an
o
erapy,
advanage
and
Fig.
5.15
instability
acquire
popuaon.
Passenger
mutatons
may
create
tumor
neoantgens
(mutator
angiogenesis
ress-
Eight
and
these
mutations
•
Genomic
Inducing
varants
muaons
e
nnocuous
ways:
in
cancer
hallmarks
tumor-promoting
properties
critical
during
genes.
and
enabling
inflammation).
their
(From
two
instability
phenotype)
development,
Hanahan
D,
factors
Most
typically
Weinberg
(genomic
cancer
RA:
cells
owing
to
Hallmarks
(proen
of
cancer:
the
next
generation.
Cell
144:646,
2011.)
sequences a dfer rom ose o norma ces). Suc angens may
be
seen
ng
w
o
a
be
as
“oregn”
os
dscussed
HALLMARKS
All
cancers
are
As
e
as
ypc
5.15
can
properes
and
OF
the
aready
undreds
conss
ces
o
e
response.
mmune
sysem,
Neoangens
poenay
and
os
ead-
mmuny
•
S e-suicency n grow sgnas
•
Insensvy o grow-nbor y sgnas
•
Aered ceuar meabosm
•
Evason o ce dea
•
L mess repcave poena (mmoray)
•
Susaned angogeness
n
•
Invason and measass
peno-
•
Evason o mmune sur veance
aer.
display
considered
by
anumor
CANCER
fundamental
hallmarks
been
be
of
changes
o
cancer
o
e
ces.
n
cancer
e
hese
oowng:
cell
physiology,
which
cancer.
menoned,
consdered
in
genes
conex
numberng
o
properes
e
are
a
common
eas
usraed
n
Fg.
In
a
addon,
coner
e
ese
acquson
properes
o
may
e
be
genec
and
acceeraed
epgenec
by
aeraons
cancer-promong
74
CHAPTER
Table
5.6
Cancer
Important
Gene
Gene
TP53
Neoplasia
5
Cancer
Genes
Class
Tumor
Function
suppres-
Sensor
sor
Effect
of
cell
stress,
DNA
Loss
repair
of
of
Mutations
function
instability,
Associated
leads
to
resistance
genomic
to
Diverse
Cancers
cancers
proapoptotic
stresses
RB
Tumor
suppres-
Negative
sor
regulator
of
cell
Loss
cycle
of
function
growth,
leads
failure
to
to
increased
Mutated
differentiate
in
retinoblastoma,
sarcoma;
dysregulated
osteo-
in
diverse
cancers
HER2
Oncogene
Growth
factor
receptor
Gain
of
function
leads
to
factor–independent
ABL
Oncogene
Nonreceptor
tyrosine
kinase
Gain
of
function
leads
to
factor–independent
RAS
Oncogene
Signaling
molecule
Gain
of
function
Oncogene
Signaling
molecule
Gain
of
leads
function
D
Oncogene
Cell
cycle
regulator
Gain
of
RB,
leads
function
leads
to
growth
to
in
cancers
Activated
by
several
growth
Diverse
NMYC
Oncogene
Transcription
factors
ming
of
IDH2
Oncogene
Metabolic
enzyme
Mutation
that
to
growth
opposes
Commonly
the
action
of
leads
leads
to
to
mutated
tion
or
in
reprogram-
breast
Translocated
enzyme
activity
Acute
oncometabolite
due
in
melanoma
to
amplification
amplified
new
an
breast
translocations
Overexpressed
proliferation
metabolism
produces
of
carcinomas
cancers
in
in
regulated
IDH1,
other
signaling
increased
Overexpression
subset
leukemias
phoma,
MYC,
a
and
signaling
factor–independent
Cyclin
Amplified
signaling
factor–independent
BRAF
growth
signaling
transloca-
in
lym-
cancer
Burkitt
lymphoma,
neuroblastoma;
in
diverse
myeloid
leukemia,
chondrosarcoma,
dys-
cancers
glioma,
cholangiocar-
cinoma
BCL2
Anti-apoptosis
Opposes
the
activity
proapoptotic
of
Overexpression
factors
leads
to
resistance
to
Translocated
apoptosis
phoma;
in
follicular
dysregulated
lym-
in
diverse
cancers
PDL1,
PDL2
Host/cancer
cell
Activates
interactions
immune
pathways
in
T
checkpoint
Overexpression
cells
leads
to
immunoeva-
Amplified
sion
in
Hodgkin
overexpressed
in
lymphoma,
diverse
cancers
nlammaon
erscs
umor
seen
n
oowng
we
by
ey
genomc
promoe
nsaby,
ceuar
wc
are
enabng
ransormaon
and
carac-
w
dened
cusson
•
genes
ever y
(by
o
dscuss
roes
n
a
cancer ;
dscusson
aso
producs
n
a
cancer
no
(e.g.,
reguae
some
accordngy,
e
o
gene
RB
n
and
RB
o
genes
are
o
ras
Tabe
symbos
gene
a
orgns
cancer
(summarzed
or
ese
moecuar
subse
convenon)
are
ceuar
subsequen
progresson.
Muaons
are
and
because
ese
orm
ceuar
e
cancer,
w
5.6).
bass
durng
requen
and
o
er
e
Progresson
of
a
Self-Sufficiency
often
that
stems
reduce
hese
encode
grow
ow
from
or
even
oncogenes
Bndng
ds-
den
proen).
drve
acve
n
a
factor
proens
e
absence
can
be
to
ts
signaling
no
(oncoproens)
o
ce
resoved
factor
in
cells
most
proteins
dependency.
proooncogenes
napproprae
growt
mutations
cancer
grow
grow,
no
e
specc
a
acors.
on
wc
ransm
To
a
oowng
receptor
sep
on
and
proens,
RAS.
S ome
pro-
apprecae
grow
ac-
seps:
e
•
protens
n
the
mem-
vaes
vaed.
by
second
messengers
proens
or
a
cascade
o
sgna
cytoso
to
te
nuceus
ransducon
moe-
cues
•
of
genes
reguae
a
transcrpton
DNA
factors
a
repcaon
ncrease
and
e
e
a
s
and
oppose
descrbed
suscepbe
cyce,
resung
dauger
ces;
and
umaey
s
process
ces
same
(grow
n
s
(RB,
p53,
corrupon
a
varous
sgnang
proens
grow
and
acor
knase
cycn-depen-
aer)
o
are
acors,
cycn/cycn-dependen
oncoproens
ceran
ese
expresson
bosyness
mutaton
to
o
o
oer
and
w
ave
delver
o
c auses
are
n
cancer
mpar
grow
acors
a
arges
growth
mtogenc
growth
cause
ow.
smuaes
yrosne
e
o
ces.
grow
acor
ac
he
acor
recepors,
downsream
efecve
One
actor
sgnals
actor.
eer
e
o
o
an
acvy
smuae
muaons
creae
a
occur
exampe
convered
o
to
Many
o
erapeuc
common
re ceptors
cells
or
typ e
acor
o
relate d
contnuously,
grow
o
a
sgnang
are
e
nvovng
consuvey
overexpresson
sgnang
An
downsream
knase
capacy
Oncogenc
proens
ng
Actvaton
ce
wo
progresson
moecues,
cancer
absence
acors
Transmsson
te
componens,
e ven
recepors
ave an nrnsc yrosne knase acvy a s acvaed by grow
ce
•
across
o
oncogenc
s
sgna
te
o
Grow t factor receptors and reated protens.
Transent actvaton of te growt factor receptor, wc n urn ac-
transduced
cyce
muaed
RAS
•
te
troug
ose
above
ndependence
ens
of
membrane
dvson
“br”
nbors,
requeny
brane
sgna-ransducng
organees,
ce
drugs.
oncogenes,
reca
ce
and
knase
E ac
characterizes
ce
e
sgnang
compexes)
proen
Signals
that
growth
conver
sgnang
of
growth
eliminate
consuvey
sgnas
Growth
in
gain-of-function
muaons
or–nduced
•
in
self-sufciency
te
and
promoe
recepors,
mos
The
dvson
(e.g.,
or
normay reguaed on mupe eves by a baance beween proens
we-
e
needed
ce
wc
or
hrougou
taczed
ras
componens
rbosomes)
o
e
even
wen
by
cascades.
surace
same
genes
cromosoma
a
encode
suc
eves
knase
bu
ac-
knase
recepors,
acor
yrosne
pro-
wen
yrosne
norma
grow
Oer
recepors
paways
acvaed
srucuray
nonrecepor
oncogene
no
are
gene
ransocaons
or
aow-
ver y
a
s
s
ABL,
CHAPTER
RAS Growth
as
an
nrnsc
Neoplasia
5
guanosne
rpospaase
75
(GTPase)
acvy
factor
a Growth
factor
ydroyzes
o
GDP ,
reurnng
e
proen
o
s
quescen
receptor
GDP-bound
pon Far nesyl
membrane
e
bound
•
Inactive
In
cancers,
eadng
o
on
by
es e
acvy :
and
sgnas
fac tors
Ac vae d
RAS
Activation
GTPase
orm
S g nang
Active
RAS
sae.
muaons,
s
saeguard
amno
acd
s
oten
abrogaed
subsuons
a
by
nerere
anchor
w
Bridging
GTP
R AS
and
RAS
us
ac ors
fac tors
dow ns re am
nercon ne c e d
dow ns re am
rapped
trans c r pton
s mu aes
s e vera
s
n
s
acvaed,
GTP-
ncessany.
dow nstream
regu aors
p a ways.
mmcs
e
o
Mu a on
of
R AS.
proera-
o
s ome
g row -promo ng
o
e e c s
protein GDP
GTP
o
ac vae d
o
PI3-k nas e
R AS
(e. g . ,
mu a ons
o
BR A F
n
me anomas
and
Activates
Inactivation
of
nuceus
umors).
Tes e
sg na s
converge
and
upregu ae
e
express on
o
genes
a
on
supp or
NF1
GTP
ce
g row ,
ncud ng
prog resson,
Active
mu pe
by
e hydrolysis
n
e e c s
RAS
are PI3K
RAF
on
and
anab oc
ds c uss e d
c ycn
M YC ,
a
D,
a
ac or
rans cr p on
me ab osm
and
re qure d
ac or
ce
or
w
g row ,
c e
c yc e
w de-rang ng
b o
o
w c
aer.
PTEN
Insensitivity
to
Growth-Inhibitory
Signals
Pro-growth MAPK
Mutation
of
oncogenes
is
not
sufcient
to
produce
the
unbridled
metabolism
MYC
proliferation Increased
that
is
characteristic
of
cancer cells;
excessive
growth
protein
also
requires
complementary
mutations
that
inhibit
the
function
synthesis
Activation
of
of
tumor
to
cellular
suppressor
Many D
cyclins
Cell
umor
ce
cycle
cyce,
ces.
As
crca CELL
Fig. 5.16
ulated
normal
cells
apply
“brakes”
and
activity
(a
a
growth
so-called
activated
to
a
factor
receptor
receptor
tyrosine
GTP-bound
state.
with
kinase),
intrinsic
inactive
Activated
a
umor
RAS
tyrosine
kinase
(GDP-bound)
transduces
RAS
RB:
RB
to
the
nucleus
along
two
kinase
pathway
and
the
pathways:
PI3
the
the
expression
of
D
cyclins
pass
kinase/AKT
and
MYC.
pathway,
The
held
in
check
by
GAPs
(GTPase-activating
of
eps
a
or
g
been
descrbed,
RB,
manan
racon
ndrecy
Cellular
the
beore
key
e
o
dsrup
a
bu
wo
reguaor
are
genomc
cancers
e
e
negry
conan
uncon
o
o
o
genec
ese
wo
G1/S
DNA
Proliferation
checkpont,
replcaton
the
portal
through
whch
cells
commences.
activity
members
o
proeraon
e
and
renobasoma
dferenaon
(RB)
amy
o
are
orcesraed
proens,
reerred
which
of
proteins)
ceuar
RAF/
ere
smpy
as
RB.
RB
was
e
rs
umor
suppressor
gene
o
be
RAS
dscovered normally
ave
prolifer-
so-called
o upregulate
wc
beow,
drecy
Governor
must
by ERK/MAP
genes
carcnogeness:
suppressors.
regulates
Norma
signals
TP53,
n
GROWTH
Oncogenic growth factor signaling. When a normal cell is stim-
through
suppressor
mporan
dscussed
aeraons
is
in
p16
progression
ative
which
proliferation.
parcuary
is
genes,
transcription
such
and
s
a
prooypca
represenave.
Approxmaey
40%
o
as
renobasomas are ama, w e predsposon o deveop umors NF1,
whereas
the
activity
of
PI3
kinase
is
antagonized
by
PTEN.
Factors
beng shown
in
green
mutations
in
suppressors
GDP ,
are
oncoproteins
various
that
Guanosine
gen-activated
cancers,
are
often
missing
diphosphate;
protein;
that
PI3K,
are
whereas
GTP ,
activated
factors
due
to
by
shown
red
loss-of-function
guanosine
triphosphate;
phosphatidylinositol-3
are
tumor
mutations.
MAP ,
e
afeced
mito-
kinase.
presence
ed
e
s
n
RAS.
n
encodes
breas
same:
acors
•
rearranged
wc
cancer.
a
ceran
he
overacvaon
downsream
RAS
genes
o
are
eukemas.
recepor
ne
o
a
yrosne
efec
o
sgnang
In
conras,
knase,
bo
ypes
cascade
s
o
e
oten
HER2
amp-
aeraons
nvovng
RAS
s
and
s
commonly
mutated
oncogenes
n
muc
acqure
oer
ndrecy.
acqured
requred.
DNA;
ces
ener
a
bnd
and
guanosne
and
or
sae
and
grow
by
guanosne
a
hs
an
quescen
muaon
and
dpospae
beween
acor
o
e
[GDP]).
exced
(eer
recepor)
amy
by
Normay,
eads
sae
o
e
canges
sae
(Fg.
grow
s
G
proens
RAS
5.16).
excange
or,
lps
back
o
Acvaon
as
sor
n
GDP
generae
normay
[GTP]
sgna-ransmng
acors
a
o
rpospae
(GTP-bound)
conormaona
sgna-emng
a
(guanosne
(GDP-bound)
recepors
subsequen
exced
nuceodes
o
or
acve
ved
o
cancers,
GTP
RAS.
because
1
,
a
a
pase
copy
domnan
o
e
ama
o
2
specrum
suc
resu,
a
o
by
RB
ra
gene
a
n
s
e
or
sporadc,
caused
by
germne
aways
a
ead
1
.
ree
(and
o
pases
eng;
pase
o
ses
cancers,
RB
a
a
o
sow
com-
one
RB
and
deecve
muaons
many
a
cancers
(CDKs),
o
proens
e
pase
o
revew
ce
varabe
cyce
durng
eng;
o
n
specc
cycns;
and
one
ces
e
wc
ces
M,
wo
roug
cycns,
enzymac
CDK
ce
ave
on
or
RB
more
ces
wc
dauger
e
s
are
repcae
durng
proens
ce
ces
cyce
wose
s
eves
cycn-depen-
acves
nbors
cyce
growng
and
generang
acors:
wose
cancers
mpnge
ave
copy
occur
uncon.
moss,
o
a)
bre
o
S,
o
ner
aee.
modcaons,
progresson
major
wo
oer
peraps
oss
compee
he
e
dferen
uncon,
second
G
o
o
epgenec
mos
RB
and
ndvduas
and down dependng on e ce cyce pase;
knases
bndng
as
varabe
,
no
oscae up
e
a
n
muaon
successve
G
reurn
conroed
den
a
he
er
members
n
deecs
G
are
key
undersand
muaons.
proens
auosoma
weer
somac
As
human tumors. Approxmaey 30% o a uman umors ave RAS
RAS
more
a
aeraons,
To
most
an
deecve
ndvduas.
sporadcay
RAS.
the
as
one
Renobasomas,
and
gene,
o
pee oss o RB uncon due o nacvaon o bo RB aees, an even
a
wc
ransmed
gain-of-function
in
depend
(CDKIs),
on
proens
a ac as negave reguaors o cycn/CDK compexes (Fg. 5.17). he
ranson
rom
e
G
1
pase
o
e
S
pase
consues
an
mporan
CHAPTER
Neoplasia
5
inhibito
K CD
rs
C
p21
in
h
ib
o it
family
rs
in
K y il m fa
C
h ib
it o r
p 2 1
E
D
D K
Cyclin
s
fa m
il y
6 1 p
CDK2
Cyclin
D
D
CDK4
CDK6
Cyclin
C
Cyclin
K
A
D
76
ih ib
2 1
o s
f a A
m li y
Cyclin P
RB
i n
CDK2
RB
CDK1
S
G
1
G
2
M
Cyclin
B
CDK1
i
l
m a f
1 2 p
r
t i
o
i n i
K D
Fig.
5.17
which
CDK6
is
Cell
inhibited
complexes.
complexes,
throughout
ce
cyce
ceckpon,
commed
“governs”
•
E ary
and
o
G
1
n
G
1
Sgnas
ors
RB
a
RB
needed
orm
RB
o
s
are
a
e
and
or
as
a
E2F
enr y
M
e
once
ce
ces
as
This
move
D
(Fg.
or
the
p16
of
e
S
by
family
the
pase
he
p21
acve
ey
acvy
orm
amy,
acvaed
o
wc
a
proliferation
phosphorylation
family
another
are
vruses
e
no
S
recep-
a
e
are
express
RB.
genes
hs
a
TP53:
D/CDK4
resu
n
he
was
compexes,
exampes
o
consuve
mporance
recognzed
n
suc
ces
e
e
move
abnormaes
eadng
RB
par
o
aernave
acvaon
o
n
o
e
roug
pospae
groups
ypopospor yaed
back
no
ncrease
nacvaon
mecansms
grow
conro
e
S
phase
D/CDK4
inhibiting
transition,
and
cyclin
cyclin
cyclin/CDK
D/
D/CDK4
complexes
encode
bnds
nbon.
over
and
e
sow
e
deveopmen
suscepbe
o
HPV
a
nacvae
ypopospor yaed
Perssen
years
e
oncoproens
o
vra
necon
seeds
o
or
(e.g.,
e
ce
In
o
o
and
and
yper-
addona
carcnomas
cer vx
HPV ,
RB
susaned
acquson
squamous
necon
and
RB.
orm
e
a
ses
cr yps
o
onss).
Guardian
of
the
Genome
The TP53 tumor suppressor gene, the most commonly mutated gene in
e
G
1
pase.
I
p53,
RB
can
acor
o
ce
dscover y
e
o
are
acvaon
RB.
mos
muaons
recepors
grow
a
he
or
and
ceran
o
a
ces,
a
s
o
acor,
as
sabze
genes.
a
a
sressed
a
s
exerna
cenra
efecs
conro
RAS
due
p53
o
undergong
o
or
DNA
s
grow
magnan
and
and
ce
o
s
desrucon.
o
In
drve
ransormaon.
nonsressed,
w
ran-
expres-
a
smu
eay
MDM2,
wen
proens
preven
TP53,
a
Sresses
e
mody
ranscrpon
o
s
progrow
conras,
e
ac
by
ncreased
assocaon
In
p53
sur vva.
“sensor”
genes
encoded
sress.
roug
ypoxa.
damage),
arge
proen
nerna
napproprae
because
aby
ese
e
o
medaed
damage,
a-e
enancng
producs
are
acvy),
sor
sgnas,
monor
ce
DNA
arges
(e.g.,
p53,
he
and
a
o
as
ncude
unbrded
proen
rom
“sensor”
vewed
p53
p53
n
oncogenc
a
genes
RAS.
cancer
s
be
scrpon
(e.g.,
common
by
to
1
human cancers, functions to protect cells from stress-induced damage.
remove
cells show dysregulation of the G1-S check point.
cycn
G
cyclin
multiple
HPV)
oropar yngea
cer
ese
the
control
proen
E2F
muaons
acvae
par,
E7
proeraon
son
mos
of
is
by
compexes
nacvae
o
pase.
acor
orm
e
RB phosphorylation are commonly found; as a result, virtually all can-
e
RB
regulate
(e.g.,
HPV
In cancers with normal RB genes, mutations in other genes that control
For
of
level
negatively
RB
bnds
prevenng
grow
and
ces
regenerang
dvded
cellular
provide
pase.
pase,
of
prevens
progresson
permng
released
5.18):
E2F
cycns,
pospaases
newy
of
is
determinant
phases.
no
pospor yae
acors,
S
o
by
block
dvdng.
e
requred
creaed
a
o
key
inhibitors
cycle
and
oows
The
inhibitors
CDK
cell
cyce
acors
are
no
ceuar
CDK
whereas
expresson
CDK6
rom
RB.
ypopospor yaed
normay
durng
RB
n
regulation.
by
various
ranson
genes
Subsequeny,
rom
e
ranscrpon
o
CDK4
reeases
are
,
upreguae
w
•
pase
nbs
expresson
•
because
compeng
-S
cycle
o
ce
and
arge
sressed
ces
CHAPTER
he
GROWTH
INHIBITORS
GROWTH
acors
a
deermne
Neoplasia
5
weer
a
ce
repars
77
s
DNA,
becomes
FACTORS
senescen, or undergoes apoposs are unceran; bo e duraon and p53
(EGF,
PDGF)
e
o
eve
be
o
p53
earned
acvaon
abou
e
may
be
nuances
decdng
o
p53
acors.
here
s
s
muc
uncon.
Stimulate
he
e
CDK
Inhibitors
•
Activate
p16
and
mporance
oowng
More
o
TP53
dysreguaon
n
cancer
s
gged
by
consderaons:
tan
70%
of
uman
cancers
ave
defects
n
TP53,
and
oer
p21
cancers
oten
ave
deecs
n
genes
upsream
or
downsream
o
TP53. Baec abnormaes o e TP53 gene are ound n vruay
Inactivate
ever y
ype
breas,
Cyclins
D/CDK4,6
• Cyclins
Cyclin
e
ertabe
he
Hypophosphorylated
RB
a
25-od
mos
e
•
P
e
P
Cell
p53
to
S
site
E2F
phase
S
site
genes
of
G
o
a
binds
are
to
phase
DNA
required
by
the
for
the
transition
RB
and
cyclin
he
few
Wn
E2F ,
phosphorylation
which
of
s
a
S
in
complex
inhibits
phase
D–CDK4
through
E2F
with
the
transcription
of
the
and
cell
cyclin
tran-
of
E2F
genes
cycle.
When
D–CDK6
o
–S
1
o
syndrome
o
Paens
w
deveopng
compared
cancers
w
seen
eukemas
activates
RB
is
transcription
inhibited
complexes.
checkpoint
as
by
Virtually
a
age,
and
target
of
a
e
are
and
and
s
s
due
to
a
wde
syndrome
specrum
o
genera
popuaon.
sarcomas,
carcnomas
bran
many
vra
caracerzed
TP53,
cancer
ce
umors;
paens
ese
deveop
can-
mupe
o
oncoprotens.
by
e
ese
As
bndng
s
E6,
a
w
o
RB,
ceran
vra
nor-
DNA
oncoproen
carcnoma.
Tumor
which
other
Suppressor
are
tumor
Genes
commonly
suppressor
lost
genes
in
many
are
different
strongly
linked
types.
exampe
s
e
APC
paway.
s
o
yperacve.
of
S-phase
CDKIs
all
such
cancer
as
cells
gene,
APC
wc
promoe
s
e
acvaor,
a
encodes
cyopasmc
a
componen
degradaon
and
w
o
oss
proen
wose
β-caenn.
o
APC,
β-ca-
β-caenn
co
ner
(rom
one
result
of
a
mutation
in
at
coonc
o
genes,
deecve
wc
APC
epeum
β-caenn
suc
copy
akes
o
s
eads
as
(unke
o
cycn
APC
D
and
deveop
name),
a
mos
ncreased
ces
MYC.
oer
Indvduas
adenomatous
dsease
o
ranscrpon
poyposs
caracerzed
by
e
and
e
com-
o
undreds
o
coonc
poyps
by
eary
aduood
genes.
p16,
show
In
yperacvy
grow-promong
wo
o
coon
carcnoma
by
age
50.
hese
umors
ave
somac
which
or
muaons
a
emnae
e
uncon
o
e
remanng
dysreg-
norma G
aee.
nonuncona
ranscrpona
neages),
deeons cyclin–CDK
the
coon,
ypes.
te
sgnang
deveopmen
of
50
young
squamous
uncon
appearance
releases
a
s
bes
and
cassc
e
becomes
activation
–S
1
Hypophosphorylated
factors
phosphorylated
ulation
ung,
Transcriptional
block
inactivate
e
phase
genes
enn
regulation
a
rendered
cancers,
domnan
Transcriptional
s
RB
only
A E2F
The
L-Fraumen
TP53
cance
age
ypes
Lineage–Specific
human
it
one
ceran
dferen
proten
onsar
Unlike
plexes,
o
deas.
encoded by HPV , dscussed earer as an mporan cause o cer vca
and
products
and
occur
o
p53
vruses.
E2F
is
cancer
P
P
P
factors.
by
common
oten
ma
RB
syndrome
n
greaer
umors
breas,
umors P E2F
whose
o
RB
cers
transcription
carcnomas
causes
Hyperphosphorylated
o
scription
cancer
mutaton
magnan
RB
ncudng
eadng
D/CDK4,6
ave
5.18
cancer,
ree
E/CDK2
germne
Fig.
o
e
least
one
copy
o
APC.
Smar
baec
oss
o
APC
s
aso
seen
n
a
sub-
of
se o sporadc coon cancers. Oer exampes o neage-specc umor four
genes;
RB,
CDK4,
cyclin
D,
and/or
CDKN2A
[p16].
EGF ,
Epidermal
suppressor growth
factor;
PDGF ,
platelet-derived
growth
Altered
•
Trggerng
morda
G
1
RB
n
nduces
e
and
p21
s
By
o
s
ce
e
DNA
caused
cycng
p53-medaed
damage
many
and
o
by
cycn
successuy,
arress
o
cyce
5.19).
I
ce
s
arres
occurs
ces
n
e
DNA
repar
ae
p21
G
1
a
o
I
pr-
n
o
e
e
prevens
pase.
damage
genes).
aowed
s
expresson
compexes,
repar
damage
e
ce
p53-dependen
me
DNA
(Fg.
D–CDK4
ereby
provdes
expresson
repared
ce
arrest.
nbng
pospor yaon
pause
age
cyce
response
pase
CDKI
ce
genes
(and
oncogenes)
are
dscussed
n
aer
capers.
factor.
(p53
DNA
proceed
Even
aso
roug
cyce.
Cellular
the
distinctive
els
of
form
glucose
hs
aerobc
Metabolism
presence
of
via
of
and
the
penomenon,
gycoyss,
s
ample
cellular
uptake
(fermentation)
hs
dam-
in
a
oxygen,
cancer
metabolism
increased
glycolytic
caed
e
cells
demonstrate
characterized
conversion
of
by
high
glucose
to
a
lev-
lactose
pathway.
Warburg
caracersc
o
many
efect
and
rapdy
aso
known
proerang
as
ces,
ncudng ea ssue, acvaed ympocyes, and umor ces. he “gu-
cose
unger”
son
omograpy
o
umors
s
(PET)
used
o
scannng,
vsuaze
n
umors
wc
va
paens
posron
are
ems-
njeced
w
18
•
Inducng ceuar senescence. I e DNA damage canno be repared,
ces
w
acve
p53
may
undergo
senescence,
a
orm
o
perma-
nen ce cyce arres. he mecansms o senescence are uncear bu
seem
e
•
o
nvove
expresson
p21
o
and
genes
epgenec
a
are
canges
requred
or
a
permaneny
aer
oc
rreversbe
genes.
DNA
damage
by
upreguang
severa
up
e
no
umor
bone
ones
are
Wy
grow.
Kng stressed ces troug apoptoss. p53 nduces apoposs o ces
w
F-luorodeoxygucose, a gucose dervave a s preerenay aken
proapop-
wo
ces
marrow).
markedy
do
o
pospor yaon
we
as
norma,
umors
are
acvey
dvdng
PET-posve,
and
ssues
rapdy
suc
as
growng
so.
cancer
moecues
(as
Mos
ces
ATP
rey
per
(wc
on
neicen
moecue
generaes
up
o
o
gycoyss
gucose)
36
(wc
nsead
moecues
o
generaes
o
ATP
oxdave
per
mo-
ecue o gucose)? he answer s a aerobc gycoyss provdes rapdy
78
CHAPTER
Neoplasia
5
Ionizing
radiation
Carcinogens
Mutagens
Nor mal
(p53
cell
Cell
nor mal)
loss
Oncogenic
with
mutations
of
or
p53
Stress
DNA
Hypoxia
p53
damage
accumulates
binds
to
DNA
and
damage
p53-dependent
DNA
not
genes
activated
No No
DNA
cell repair,
T ranscription
dependent
and
cycle
no
arrest senescence
independent
effects
on
targets
Mutant
cells
Expansion
GADD45
p21
and
Senescence (CDK
(DNA
inhibitor)
repair)
additional BAX
mutations
(apoptosis
G1
arrest
Successful
Nor mal
Fig.
5.19
aging
The
agents
upregulation
repair
of
dvdng
e
umor
syness
o
ces
pospor yaon
cue
o
gucose
w
ceuar
does
or
and
In
combnes
p53
the
cells
with
genetically
Durng
w
O
to
to
loss
or
damaged
wereas
oxdave
cycle
kinase
with
a
are
H
2
O
and
inhibitor
the
cell
of
CO
2
,
in
G
fails
if
rise
or
moe-
wc
s
and
1
induction
damage
Beyond
cancer
and
(see
grow
yss
moees
(proens,
yeds
pds,
meaboc
needed
and
o
nucec
nermedaes
bud
e
acds).
a
In
are
ceuar
componens
conras,
useu
as
aerobc
ceuar
or
gyco-
e
bocks.
reprogramming
downstream
are
of
deregulated
genes
In
in
o
unc on.
sg na ng
5.20).
by
factor
mutations
produced
receptors,
in
by
the
oncogenes
signaling
same
and
cascades
pathways
tumor
that
suppressor
cancers.
c ancer
ac ons
growth
is
ce s,
ac ors
s
reprog rammng
oncoproens
mp or an
and
ce u ar
and
p ons
o
e
p ersss
oss
o
cross a k
me ab osm
ave
b e c aus e
umor
b e we en
b e en
o
er
own
1).
genes.
cycle
Successful
apoptosis
arrest
wo
or
oer
mporan
seen
severa
n
a
oss
o
n
a
o
or
DNA
nks
mer
beween
bre
prog row
a
ne
cancer
new
efec
afec
genes.
rggerng
promoe
o
meabosm
menon:
e
group
c yce.
o
auop-
S ome
o
n
expresson
or
s
In
o
and
eac
cause
acvy
keepng
o
n
a
w
suppressors.
aeraons
enzymes
muaons
oer
aogeer
muaons
umor
ese
sur vve
envron-
suggesng
In
oncogenc
muaons
wereas
acves
are
o
o
margna
deranged.
auopag y
consss
membranes
under
auopag y,
are
oncomeaboes.
e
and
grow
auopag y
uncon,
caed
proens,
oten
surprsng
Krebs
enzyme
been
a
A
e
acqure
e
wou
neopasms
a
ave
ces
nduce
genes
ceran
parcpae
osm
organees,
condons
enzymes
(Fg .
DNA-dam-
transcriptional
either
efec,
Tumor
suppress or
ds covere d
e
cell
by
by
neoplasms.
suiceny
Oncometabosm.
e
mu ae d
S e vera
•
induce
Warburg
are
paways
s,
Metabolic
triggers
tumor
p53
repair,
GADD45
p53
malignant
Caper
mena
budng
e
DNA
the
not
normal
Autopag y s a sae o severe nuren decency n wc ces can-
nbaze
carbon
to
of
“oncomeabosm. ”
any
e
of
fails,
does
eventually
ag y
and
repair
os roug respraon. hs yeds abundan ATP , bu does no yed
o
Activation
(p21)
DNA
and
•
Malignant
genome.
CDKN1A
DNA
giving
oxdave
a
the
cycle;
TP53,
needed
pospor yaon,
of
arrest
proliferate,
mocondra
produce
integrity
mutations
cells
Repair
Apoptosis
the
cell
proceed
nermedaes
o
2
leads
repair
cells
maintaining
cyclin-dependent
cells
meaboc
in
hypoxia
allows
componens,
no.
of
by
of
DNA
senescence.
repair,
role
gene)
cases
e
generae
o
afeced
producs
nsance,
canges
n
curreny
a
ead
appears
meab-
unknown
CHAPTER
QUIESCENT
CELL
GROWING
Glucose
CELL
(NORMAL
OR
Neoplasia
5
79
TUMOR)
Growth
Glucose
factor Glucose
Glucose
transpor ter
RTK
RTK
transpor ter
PI3K
Autophagy
Protein
Lipids Akt
Increased
synthesis
glycolytic
inter mediates Nucleotide, Lysosome Lipid
and amino
amino
acid
GROWTH
acid synthesis
catabolism Lactate
Krebs
Mitochondrial Lipogenesis
cycle
metabolites
Increased A TP
CO
2
glutamine
MYC
utilization
RTK
RTK
Glutamine
Growth
factor
Fig.
5.20
starved,
normal
thesis
Metabolism
autophagy
cells
of
Evasion
In
of
certain
Cell
markedly
and
Warburg
cell
growth.
(self-eating)
other
is
upregulate
nucleotides,
pathways
the
and
proteins,
key
induced
glucose
and
factors
Quiescent
as
provide
and
lipids.
such
to
In
cells
a
rely
source
glutamine
cancers,
MYC
the
of
uptake,
deregulate
these
mutations
that
the
fuel.
Krebs
When
provides
mutations
metabolic
cycle
for
stimulated
carbon
involving
ATP
by
sources
growth
pathways,
production;
growth
an
for
factor
alteration
if
factors,
the
syn-
signaling
known
as
effect.
accumulation
of
neoplastic
cells
overexpresson
o
w
o
provide
resistance
to
regulated
g
eves
BCL2,
and
expresson
many
o
oer
BCL2
or
cancers
oer
are
assocaed
anapopoc
mem-
results bers
from
on
which
oncogenic
Death
cancers,
mainly
cell
o
e
BCL2
amy.
death
•
Inactvaton of sensors and efectors o ce stress that woud normay
(apoptosis).
As
ces
dscussed
no
n
Caper
componen
1,
peces,
apoposs
a
process
s
e
a
ordery
may
be
dsmanng
rggered
by
trgger
apoptoss s
dea.
As
or
exrnsc
paway
a
umaey
acvaes
a
nvovng
caspases;
ese
n
urn
are
responsbe
or
o
e
ce.
he
sequence
o
evens
a
ead
paways
be
rggered
by
sress-nducng
ceuar
njures
or
o
(e
nrnsc
paway),
or
by
acvaon
o
members
recepor
amy
(e
exrnsc
O
ese
wo
e
paways
o
mocondra
ces
escape
efecor
sense
ce
sress.
Wen
acvaed,
p53
o
canges
p53
o
promoe
uncon
(due
o
apoposs
muaon
n
o
severey
TP53
or
sressed
p53
ces.
nacvaon
ndrec
ordnary
mecansms)
k
aows
ces
o
sur vve
sresses
a
em.
protein
expression
and
TP53
mutation
status
have
import-
paway).
apoposs,
s
e
nrnsc
paway
implications
paway)
a
s
mos
requeny
for
treatment
and
prognosis.
(aso Drugs
as
cancer
downsream
e
ant
known
wc
e
acor
o
BCL2 TNF
by
s
apoposs
grow
woud decency
a
expresson
o
roug can
p53
ordery Loss
dsassemby
mecansm
prevousy,
proeoyc gene
cascade
menoned
e severa
nrnsc
anoer
o
a
bnd
BCL2
and
bock
s
uncon
are
used
o
rea
can-
dsabed cers
assocaed
w
BCL2
overexpresson.
Conversey,
e
presence
n cancer (Fg. 5.21). A decae baance beween proapopoc and ano apopoc
members
no
undergoes
o
e
BCL2
proen
amy
deermnes
weer
TP53
muaons
s
assocaed
w
a
worse
oucome
n
vruay
a
or orms o cancer, key because oss o p53 makes ces ressan o orms
a
ce
apoposs.
he
reease
o
cyocrome
c
by
moo
condra
permeabzaon
promoes
apoposs
va
e
erapy
(e.g.,
radaon
erapy
and
ceran
ypes
o
cemoerapy)
proapopoc a
cause
DNA
damage,
a
poen
nducer
o
apoposs
n
ces
w
proens BAX and BAK, wc are ed n ceck by anapopoc memnac bers
o
e
amy
(e.g.,
BCL2).
A
rd
se
o
proens,
e
cause BH3-ony
oc
and
Wn
n
wc
proens,
appears
anapopoc
s
ramework,
apoposs
o
amy
st
baance
beween
e
DNA
ces
(Fg.
possbe
by
e
o
usrae
nrnsc
e
paway
mupe
damage
ese
ces
ypes
o
reamen
w
agens
are
key
o
be
deecve
n TP53
uncon,
a
because
ave
a
seecve
advanage
a
aows
em
o
sur vve
ese
s
erapes.
rusraed
by
of
BCL2
s
a
we
caracerzed
mecansm
of
Replicative
growth
Potential
umor
ces
rom
apoposs.
Approxmaey
85%
o
carr y
a
cromosoma
ransocaon
a
is
not
(Immortality)
enough
tumor
cells
also
must
for
develop
ocsenescence
ympomas
restraints
tumors
to
achieve
a immortality:
uar
oowng
5.21).
O verexpresson
proecs
recur
ways
Loss
•
a
proapop-
Limitless cancer
Cancers
members.
s
medaed
e
p53.
so-caed
drves
e
and
mitotic
catastrophe.
ways
to
avoid
cellular
80
CHAPTER
Neoplasia
5
Deficiency
ROS
growth
Radiation
and
Chemicals
Lke norma ssues, umors requre dever y o oxygen and nurens
of
and
factors
survival
o
signals
remova
1
o
sze
2
o
mm
wase
n
represens
and
wase
grow
can
beyond
wc
as
e
a
producs.
absence
rom
sze
sprou
dua
rom
dsance
ey
ony
across
ave
prevousy
on
are
angogeness,
preexsng
m,
efec
Tumors
o
maxma
dfuse
s
vesses
zaon
e
umor
wc
bood
o
abe
grow
exsng
a
sze
because
s
oxygen,
vesses.
smuae
grow:
o
presumaby
For
o
nurens,
neopasms
o
neoangogeness,
n
capares.
Peruson
Neovascuar-
suppes
needed
DNA
nurens
and
oxygen,
and
newy
ormed
endoea
ces
smuae
e
damage
grow
e Mutation
of
adjacen
resung
umor
umor
ces
by
vascuaure
s
secreng
efecve
grow
a
acors.
deverng
Aoug
nurens
and
p53
p53
Overexpression
of
o
removng wases, s no norma: he vesses are eaky and daed w
response
a
MDM2
Activation
apazard
penerae
of
Tumor
various
BAX/BAK
sensors
a
are
paern
ese
o
connecon.
vesses,
angogeness
pro duced
by
Invasve
conrbung
may
e
be
o
smuaed
umor
umor
ces
may
ready
proangogenc
ac ors
measass.
ces,
by
nlammaor y
ces
(e.g.,
mac-
BCL-2
ropages),
and
o er
resden
sroma
ces
(e.g.,
umor-ass o caed
BCL-XL
brobass).
Proe as es
eab oraed
by
e
umor
ces
or
by
s roma
MCL-1
Mitochondria
ces
may
as o
exraceuar
s
Cytochrome
c
•
APAF-1
ur er
o
In
renorced
by
vas c uar
ac or Caspase
p epdes
mar x.
c yokne.
IAP
ree as e
endo ea
Mos
(HIF),
u-bown
s e vera
angogenc
cancers,
o er
grow
no aby,
an
w
ssue
(VEGF),
yp oxa
rom
proangogenc
aera ons
ac or
oxygen-s ensve
e
ac vy
a
a
ke y
s abzes
rans cr p on
ncre as e
e
s ae
e ves
proangogenc
yp oxa-nduced
ac or
a
drec y
9
upreguaes
a Caspase
VEGF
smuaes
expresson.
e
hs
proeraon
o
cre aes
an
angogenc
endo ea
ces
and
g raden
gudes
e
3
grow
o
ne w
suppress ors
p53
vess es
oten
repress es
e
oward
e
e
baance
expresson
umor.
o
o
Mu a ons
avor
VEGF
nvovng
angogeness.
and
For
s muaes
umor
exampe,
e
expres-
Apoptosis son
Fig.
5.21
tumor
are
in
Intrinsic
cells
red
to
pathway
evade
and
cell
include:
of
apoptosis
death.
(1)
Loss
and
Evasion
of
p53,
mechanisms
mechanisms
leading
to
in
used
tumor
reduced
by
cells
function
o
anangogenc
provdes
a
more
ac or–recepor
moec ues.
p er mssve
sgnang
hus,
oss
envronmen
and
MYC
as o
o
or
p53
n
umor
angogeness.
s muae
e
ces
Grow
expresson
o
of
VEGF.
proapoptotic
factors
such
as
BAX.
(2)
Reduced
egress
of
cytochrome
Te c
from
mitochondria
as
a
result
of
upregulation
of
antiapoptotic
dep endence
erap eu c a y. such
as
BCL2,
BCL-XL,
and
MCL-1.
(3)
Loss
of
apoptotic
factor
1
(APAF1).
(4)
Upregulation
of
inhibitors
of
Te
umors
proo yp e
on
ang ogeness
an ang o genes s
c an
dr ug ,
be
ex poe d
b e vac zumab,
peptidase-acti-
s vating
o
factors
apoptosis
an
an b o dy
a
neu ra zes
VE GF
and
s
approve d
or
e
re a -
(IAP).
men
no
o
mu pe
b e en
as
c ancers .
e e c ve
as
Howe ver,
or g na y
ang o genes s
op e d;
n bors
presumaby,
ave
sub cones
o
As dscussed prevousy n e conex o ceuar agng (see Caper umor
1),
mos
norma
uman
ces
can
doube
60
o
70
mes,
ater
wc
ce s
w
g re aer
nvasve
c ap ac y
and
e
ab y
o
mg rae
e o
exs ng
bo o d
vess es
emerge,
ereby
s deseppng
e
ne e d
or
ces ose e aby o dvde and ener senescence. hs penomenon s ne o ang ogeness.
due o progressve sorenng o teomeres a e ends o cromosomes.
he
are
consequences
drasc.
Sor
o
eomere
eomeres
are
sorenng,
recognzed
as
wen
pronounced,
doube-sranded
Invasion
Invasion
breaks
by
e
ce’s
DNA
damage
“sensors, ”
eadng
o
c yce
arres
and
apoposs
or
senescence
Even
n
ces
w
cancer
aemps
o
repar
e
damage
roug
Metastasis
metastasis
oer
DNA
cells,
stromal
result
cells,
from
and
complex
the
interactions
extracellular
involv-
matrix.
TP53 Mos
muaons,
and
p53-medaed ing
ce
and
DNA
sudes
peran
o
carcnomas,
wc
are
our
ocus
ere.
For
repar e purpose o dscusson, nvason and measass can be broken down
paways
eads
o
cromosome
nsaby,
wc
evenuay
eads
o
eomerase
(a
no
ce
dea.
I,
specazed
pae
or
owever,
e
RNA-proen
addng
ce
reacvaes
compex
nuceodes
o
a
e
e
uses
ends
o
enzyme
s
own
RNA
cromosomes),
as
a
ce
em-
a
successve
Invasion
be
Teomerase
are
s
acve
n
norma
sem
ces
and
s
absen
rom,
wo
a
ver y
eomere
ow
eves
n,
manenance
mos
s
somac
due
o
ces.
In
upreguaon
85%
o
o
95%
o
eomerase.
nex.
no
Matrix
comparmens
remanng
umors
a
o
aternatve
express
eomerase
engtenng
of
and
teomeres
use
a
anoer
depends
and
a
o
manan
separaed
rom
ssue,
proeogycans
mus
e
sages
rs
(see
n
eac
composed
Caper
e
breac
nersa
crcuaon
eac
oer
membranes
o
coagens,
and
gycopro-
2).
measac
Tumor
ces
cascade
nerac
(Fg.
5.22).
w
A
e
carc-
e
underyng
connecve
ssue,
basemen
and
membrane,
umaey
gan
en
access
s
by
penerang
repeaed
n
reverse
e
vascuar
wen
umor
basemen
ces
membrane.
o
exravasae
a
hs
dsan
Angiogenesis
grow,
solid
tumors
develop
their
own
blood
supply
Invason
o
e
ECM
naes
e
measac
cascade
and
s
an
by acve
inducing
basemen
eomeres.
ses.
to
connecve
severa
ce
process
order
(ECM),
DNA
e
Sustained
marx
meca-
on
raverse
recombnaon
exraceuar
he
noma
ermed
o
can-
ECM
In
dscussed
or
ens,
nsm
Extracellular
organzed
ypes
nersa
cers,
evens,
avered. by
presen
the
o
dea Tssues
may
of
sequence
process
angiogenesis. oows:
a
can
be
resoved
no
severa
sequena
seps,
as
CHAPTER
metaoproteases
(MMPs)
Neoplasia
5
produced
by
umor
81
ces
or
sroma
ces
Transformed
(e.g.,
brobass
and
nlammaor y
ces)
reacng
o
e
umor.
he
cell PRIMARY Clonal
eves
expansion,
o
meaoproease
nbors
aso
are
reduced
n
carcnomas,
TUMOR growth,
diversification,
urer
ng
e
baance
oward
ssue
degradaon.
angiogenesis
•
Locomoton,
e
degraded
yss.
Metastatic
e
Suc
sep
basemen
movemen
ce–derved
subclone
na
o
nvason,
membranes
may
cemoknes.
be
In
propes
and
poenaed
addon,
umor
zones
o
and
ceavage
ces
roug
marx
proeo-
dreced
by
producs
o
umor
marx
Basement
componens
(e.g.,
cemoacc
acvy
coagen,
amnn)
and
some
grow
acors
ave
membrane Adhesion
invasion
of
to
and
or
umor
ces,
and
sroma
ces
aso
produce
basement
paracrne
efecors
o
ce
moy.
membrane
Vascular Passage
Dissemination
and
Homing
of
Tumor
Cells
through
extracellular
matrix
T umor
ces
requeny
escape
er
ses
o
orgn
and
ener
e
crcua-
on roug bood vesses or ympacs. Mons o umor ces are sed
day
Intravasation
rom
even
sma
cancers.
Severa
acors
seem
o
m
e
mea-
sac poena o crcuang umor ces: We n e crcuaon, umor
ces
are
vunerabe
o
desrucon
by
os
mmune
ces,
and
e
process
o adeson o vascuar beds and nvason o norma ssues may be more
Interaction
with
lymphoid
host
cells
dicu
an
e
na
nvason.
Even
oowng
exravasaon,
umor
ces a grow we n er prmary se may ack crca sroma suppor
or be suppressed by resden mmune ces. Despe ese mng acors, Host
negeced,
vruay
a
magnan
umors
w
evenuay
produce
mac-
lymphocyte
roscopc
The Platelets
Tumor
measases.
sites
of
metastases
are
related
to
two
factors:
the
anatomic
cell
location
embolus
and
the
and
vascular or lymphatic
tropism
of
particular
drainage
tumors
for
of
the
specic
primary
tumor,
tissues.
Extracellular
Mos measases arse n e rs capar y bed avaabe o e umor,
matrix
bu Adhesion
naura
paways
o
dranage
canno
woy
expan
e
dsrbu-
to
on
o
measases.
As
menoned
earer,
or
exampe,
ung
carcnoma
basement
as a g procvy or spread o e adrena gands and e bran, and
membrane
meanoma
ropsm
o
may
e
be
eye
amos
reaed
o
aways
e
spreads
expresson
o
o
e
ver.
Suc
ssue-seecve
organ
adeson
Extravasation
moecues,
or
wc
ces
Metastatic
deposit
a
eren
e
producon
umor
ces
suppor
ssues
e
o
specc
express
grow
avorabe
or
cemoknes
recepors,
o
umors.
unavorabe
and
A
“so”
e
o
n
ese
or
dferen
presence
o
acors
dferen
ssues
sroma
make
d-
umors.
Metastasis Angiogenesis
T umors
vary
greay
n
er
aby
o
measasze,
n
par
because
o
METASTATIC
neren
dferences
n
beavor.
In
genera,
arge
umors
are
more
key
TUMOR
o
measasze
an
sma
umors,
presumaby
because
arge
umors
are
Growth
ypcay presen n e paen or onger perods o me, provdng add-
ona cances or measass o occur. However, umor sze and ype can-
no
adequaey
open
o
muped
neren
Fig.
5.22
The
metastatic
hematogenous
spread
of
cascade:
a
The
sequential
steps
involved
in
of
nterceuar
host
connec tons
between
tumor
ce s.
of
ce s
are
nor ma y
suc
E-c ad er n.
ed
oge er
by
ad eson
evolve
E-c ad er n
unc on
s
o en
c arcnomas
due
o
e er
deeer ous
os
mu a ons
n
n
or
s encng
ass o c ae d
w
o
E-c ad er n
canges
n
expresson.
ce
sap e,
L oss
o
ncre as e d
upregu a on
(e.g .,
o
genes
brob ass).
a
Tes e
are
more
canges
ypc a
are
o
reer re d
rans on
Loca
degradaton
of
te
tssue
by
umor
o
s
s
cance
(relecng
umor).
or
is
capable
inhibit
of
destroying
immune
tumors,
but
can-
responses.
ces
can
be
recognzed
mmune
as
surveance
“oregn”
reers
o
and
e
emnaed
roe
o
e
by
e
mmune
n
consany
“scannng”
em.
e
body
Tumor-specc
T
or
ces
emergng
and
magnan
anbodes
are
ces
ound
many
paens,
s
oten
and
e
exen
correaed
w
and
e
quay
cnca
o
mmune
oucome
nraes
(e.g.,
coon
n
can-
mes ency ma
o
as
here
s
an
ncreased
ncdence
o
ceran
cancers
n
mmuno-
ep e-
saes.
Receny,
erapeuc
T-ce
responses
(descrbed
agens
a
ac
by
smuang
(EMT).
basement
membrane
and
proeoyc
enzymes,
os
nterstta
n connectve
deermnsc
rom
o
mo y,
aen
•
or
and
maer
Surveillance
system
evade
sysem;
decency a -mes ency ma
me)
poena
(a
E-c ad er n
ce
cer). ce s
to
desroyng
cancers and
and
cancers,
probabsc
E-c ad-
n s
ndvdua
s
me a -
and er n
number
measac
o
C ar-
sysem s a c
beavor
measass
proens,
mmune as
ce
n
Immune
immune
Tumor cnoma
umor
dferences
Evasion
cers
L oos enng
by
e
weer
the
tumor.
The
•
expan
queson
parcuary
matrx
some
advanced
cancers.
aer)
ave
sown
efecveness
82
CHAPTER
Because
nang
nvsbe
ny.
e
nascen
o
hs
mmune
cancers,
e
os
Neoplasia
5
sysem
cancer
mmune
undersandng
s
capabe
sur vva
sysem
as
ed
or
o
o
recognzng
requres
a
a
acvey
e
suppress
modern
and
umor
os
revouon
em-
ces
angens.
be
oucome
mmu-
n
rae
cancer
he
o
(e
oer
presence
many
o
mmunoscore)
kng
uncona
cancers,
and
as
mecansms
some
(e.g.,
CD8+
T
quancaon
predcve
macropages
ces
o
s
e
vaue.
and
predcve
mmune
he
o
ce
e
n-
sgncance
NK
ces)
s
by
being
o
uncear.
mmunoerapy.
Immune
Tumor
The
the
Antigens
major
antigens
products
of
MHC-binding
Because
are
seen
ens,
as
ger
and
o
oers
by
o
are
nove
os’s
T
immune
produce
responses
neoantigens
are
are
mmune
bu
presen
Lke
dspayed
Some
umor
expressed
ces
expressed
no
sysem.
and
are
Escape
cells
lymphoid
with
(e.g.,
eary
n
as
a
cyosoc
cass
angens
cancer
yrosnase
n
normay,
regulation
I
ave
pro-
•
of
are
no
a
muc
repressed
oten,
nens
o
•
Inbton
ess
and
because
presen
o
n
anumor
er
oer
recognon
norma
ces
angens
by
and
ave
been
anbodes,
ey
are
bu
neer
dened
mos
o
nducers
n
ese
nor
umors
are
aso
arges
engage
o
agans
he
mos
Mechanisms
mporan
of
Tumor
mecansm
Destruction
o
umor
o
of
T
T
a
er
nbed.
mmuny.
o
ose
CTLA-4.
CD8+
Immune
o
system
either
inhibitory
mmune
(Fg.
pathways
invisible
designed
evason
ave
been
descrbed
emnaon
s
e
kng
o
e
angens
expresson
ces
usng
Wen
gands,
ces.
are
cass
I
arges
MHC
paways,
ceckpont
o
os
mmuny
moecues
prevenng
e
and
and
s
e
o
or
rae.
n
wo
uncon
preven
umors
by
bes-known
on
o
ese
mmune
umor
because
are
CD8+
ces
umor
o
PDL-1
Bockng
o
and
eer
PDL-2
PD-1
or
on
oer
CTLA-4
ces
w
n
e
T umor
peptide-MHC
Primed
of
CTL
killing
capable
tumor
TCR CD28
B7 B7
CTLA-4
CTLA-4
CD8+
CD8+
cell
T
Anti-
CTL
cell
CTLA-4
NO
COSTIMULA TION
COSTIMULA TION
Activated
Inhibited
Cytotoxic
CD8+
CD8+
granules
CTL
CTL
CTL
CTL
TCR
TCR
Peptide-MHC
PeptidePD-1 MHC
PD-1
Anti-PD-1
ligand
Killing
tumor
Tumor
Tumor
of
cell
cell
cell
Anti-PD-1
ligand
B
T umor
tissue
Fig.
5.23
surface
ceptors,
signals
AH,
Activation
m olecule
leading
to
transmitte d
Pillai
S:
of
with
Cellular
T
hos t
by
a n titum or
inh ibito ry
c ell
im m uni t y
a nt i bod y
ac tiv a tio n.
PD- 1,
and
are
sence
mmune
anbodes
cell
peptide-MHC
TCR
node
ces
ces
ces
CD28
Lymph
PD-1
T
responses
Dendritic
cell
A
or,
compo-
presenaon
acvaon
expressed
“jacked”
engaged
he
T-ce
and
evoved
are
n
CTLA-4
acvaon
ceckpons
PD-1
receptors.
“ceckpons”
PD-1
se-angens
T
a
o
ces.
mpose
hese
expresson
Dendritic
T
and
oten
express e gands or ese recepors (PDL-1 and PDL-2) or nduce
umor ces by CD8+ cyooxc T ympocyes (CTLs) specc or umor
T umor
to
for
5.23):
angen-processng
angens
recepors
Many
vaue
expresson
maure ces, and derepressed n cancer ces (e.g., e so-caed cancer–
angens).
immune
hijacking
immunity.
more
o
n
the
by
mecansms
erapeuc
ose
e
meanomas),
deveopmen,
or
Antgen oss varants. As umor subcones evove, ey end o eer
MHC-as-
ces
n
ey
evade
cells
Severa
and
ces.
norma
normay
elicit
that
processed
genes
n
genes
are
CD8+
muaed
an
e
are
that
sequences.
angens
angens
eves
tumors
mutated
oregn
pepdes
producs
of
mutated
ese
ese
socaed
Tumor
a g ain
mole c u la r
(B)
all o w s
Bl oc k ad e
le a di ng
to
by
c hec k poi n t
cy t ol y t i c
of
P D -1
a ct i v a t i on
im mu no log y ,
ed
C D8 +
7,
of
T
inh i bi t or s .
c el l s
rec e pt or
CT Ls .
or
(A )
( CTL s )
P D -1
( Re pr i nt e d
Philadelphia ,
2 0 1 2,
Bl o ck a de
to
en ga ge
l i g an d
f r om
of
B7
t he
a br og at e s
A bba s
Sa un ders .)
CTL A- 4
f a mi l y
AK,
c o- r e -
i nh i bi t or y
Li c ht m a n
cells
n-
eads
o
CHAPTER
e
regresson
ce
ung
hs
approac,
componen
normay
oten
as
•
o
cancer,
o
o
caed
preven
deveop
Hodgkn
Because
auommuny,
e
mecansms
by
o
mmunosuppressve
wc
organs,
umors
reguaor y
cyoknes
T
as
now
gven
an
ese
ncudng
ear,
and
non–sma
and
and
dsease. he rae o somac muaon n sun-exposed skn s greay acce-
eraed, resung n an exraordnary g ncdence o skn cancers suc
evoved
as
basa
cos,
as
we
Defects
in
Instability
magnancy,
a
a
wc
genes.
cancers
o
gged
repar
secon
o
norma
mporance
DNA
mutations
cancer
muagens,
because
s
of
precedng
nvovng
an
responses
producon
o
TGF-
Enabler
DNA repair pathways
accumulation
he
as
DNA
by
dened
o
Aoug
Diseases
are
abe
repar
o
n
tumor growth
he
umans
rare
sense
w
(msmac
by
are
allowing
o
repar
e
nered
n
negry
deecs
aeraons
encouners
damage.
o
n
o
envronmen-
ese
DNA
nuceode
eaures
genec
awas
oucomes
and
repar,
denng
by
genes
e
ypes
repar,
nered
repar
syndromes,
genes,
as
we.
sporadc
dscusson
cancers
Presumaby,
as
n
oten
beow
ncur
ndvduas
ocuses
w
o
and
a
n
o
o
a
Boom
ereby
e
deveopmen
o
he
roe
o
Nonpolyposis
DNA
msmac
Colon
repar
Cancer
genes
n
Evdence
muaons
usraed
by
e
eredtary
nonpoyposs
coon
cancer
wo
and
subsanay
DNA
ger
o
srand
ac
as
w
o
DNA
“spe
T ,
correc
raer
e
s
beng
ceckers. ”
an
deec.
repared,
For
e
e
exampe,
norma
Wou
A
ese
proens
ere
w
T ,
s
encoded
an
e
msmac
“prooreaders, ”
by
erroneous
errors
n
paens
repar
gene
s
w
HNPCC.
nered,
and
a
One
deecve
second
“”
n
copy
e
o
ese
genes
parng
repar
addon
o
G
oer
DNA
aee
a
an
msmac
o
e
same
gene occurs n coonc epea ces. In s respec, ey resembe umor
suppressor genes. DNA repar genes afec ce grow ndrecy by aow-
ng
A
muaons
n
caracersc
deecs
repeas
e
s
o
eng
w
oer
genes
ndng
n
mcrosaee
one
o
o
sx
ese
HNPCC,
durng
e
genome
nsaby
nuceodes
saees
process
o
norma
w
ce
consan.
unsabe
and
e
dvson.
msmac
Mcrosaees
rougou
remans
are
o
paens
(MSI).
ound
mcrosaees
ese
e
are
genome.
However,
ncrease
or
of
n
repar
andem
Usuay,
paens
decrease
n
eng. HNPCC syndrome accouns or ony 2% o 4% o a coonc can-
cers, bu MSI can be deeced n abou 15% o sporadc cancers. MSI-asso-
presumaby
because
e
deec
n
msmac
repar
eads
o
a
g burden o muaons producng umor neoangens. In ac, s ype
o
mmunoerapy
mac
repar
s
deecs
now
approved
regardess
o
or
e
a
umor
recurren
umors
ype—e
rs
w
me
as
or
o
or
o
DNA
are
cancer,
or
E ac
by
s
neura
s
o
and
syn-
agens
suc
repar
by
deecs
recomb-
a
damaged
cross-nked.
ncude,
sympoms
(n
o
Boom
caused
covaeny
and
(n
omoogous
used
compex
anema),
ataxa-teang-
ypersensvy
cross-nkng
repar
DNA
by
radaon
anema).
broken
dseases
sy ndrome,
onzng
DNA
srand
been
Boom
n
he
addon
aaxa-eangec-
deveopmena
deecs
(n
oncogenc
roe
o
deecve
omoogous
recomb-
rsk
rsk
o
breas
ger
o
rsk
aso
are
o
copes
o
n
women
ovaran
n
and
uncon
ound
cancer ;
cancer
meanoma,
bo
a
cancer,
prosae
breas
genes,
o
o
genes
BRCA2,
o
BRCA2
recombna-
breas
cancers.
muaons
men
women,
Smar
and
and
muaons
and
ympomas.
ama
BRCA1
carcnoma
men
BRCA1
omoogous
o
w
germne
bo
n
50%
n
as
as
a
sgy
ncrease
oer
umor
be
ave
a
BRCA2
we
oer
mus
ave
car-
suppres-
nacvaed
or
deveop.
a
Inflammation
as
an
Enabler
Inammatory cells can facilitate tumor cell growth and survival by
producing
ms-
rea-
soluble
Inrang
paens
w
exensve
(e
as
may
sroma
a
cancer
pasc
n
ces,
umors,
cer
(Fg.
o
s
more
As
o
and
enzymes
new
our
a
conceps
undersandng
ope
efecve
a
e
nex
argeed
oca
anumor
erapeuc
ave
o
on
a
umor
and
umor
and
resden
endoe-
may
ac
efecs
ces
oer
mmune
mcro-
hese
promoe
on
sur vva
e
neo-
paways
nvason
and
responses.
In
genes.
provded
agens
ew
anema
ces
ce
so
Anma
e
ces
In
be
as
brobass
acvang
suppressor
suc
can
nlammaor y
acors
enance
cancer.
cacexa.
cancer.
sroma
grow
efecve
umor
o
nlammaor y
resden
and
mody
beween
angogeness,
paopysoogc
5.24).
o
aso
amarks
of
reacon.
reacon
sympoms,
ague,
ces
e
producng
resembe
o
and
cancer-assocaed
ces
suppressng
ey
reason
many
by
promong
deveopmen
ere
efecs
parcuary
and
o
hallmarks
nlammaor y
nlammaor y
sgns
neracons
ndrec
producng
respec,
hese
e
many
drec
deveopmen
s
nlammaor y
enabe
the
cronc
nlammaon),
Inlammaor y
measass,
s
or
ces,
ces.
a
o
rom
ces,
sysemc
inuence
a
cancers,
cronc
sugges
sem
umor
cause
that
provoke
advanced
o
envronmen
factors
cancers
o
anema
modes
caed umors end o be more responsve o mmune ceckpon nbor
erapes,
Homologous
Malignancy
proens
accumuae
a
paens.
syn-
ncreased rae. Muaons n a eas our msmac repar genes ave been
ound
ese
cancer
(HNPCC)
drome, a dsorder caracerzed by ama carcnoma o e coon. Wen
a
by
caracerzed
Fancon
Fancon
e
n
cancer
predsposon
(n
BRCA1
DNA
cancer.
as
ese
o
n
Syndrome
e
o
(n
Tumor-Promoting s
n
naon aso comes rom e sudy o eredar y breas cancer. Germne
sor
Hereditary
carcnoma
syndrome).
cnomas,
and
are
suc
“good”
a
anema
muaons
genes
ce
Repair
dsorders
requred
a
predsposon
asa),
e
cancer
are
DNA
repar deecs, ese somac muaons speed e accumuaon o drver
n
agens,
wc
ese
nered
DNA
anema
musard
on
muaons
in
recessve
Fancon
penoypes
genome
ree
excson
he
pece
In
e
squamous
aaxa-eangecasa)
n
or
Aoug
and
nrogen
on,
cancer.
and
as
recombnaon repar), a o wc are assocaed w an ncreased rsk
deveopng
and
Defects
auosoma
ectasa,
naon,
eg
mananng
born
Malignancy
produced
with
DNA-damagng
genes.
e
be
reavey
persons
sysems
enable
cancer
appear
are
ces
in
of
carcnoma
Recombination
ssues.
drome
Genomic
ce
reamens
oer
oca
nuceode excson repar sysem, wc s deecve n paens w s
mporan
mmune
e
83
oers.
ceckpons
nb
ces
suc
s
e
paens
nlammaon,
endocrne
meanoma,
ympoma,
bockade,
erapy.
auommune
nducon
ncudng
cancer,
ceckpon
o
ncude
umors,
ancancer
nlammaon
Oter
many
badder
Neoplasia
5
or
cancer
years
e
a
road
paogeness
w
map
reamen
see
e
o
or
can-
expands,
deveopmen
erapes.
men as been approved based ony on a muaona sgnaure.
CLINICAL Xeroderma
Umaey, Paens
w
e
auosoma
recessve
dsorder
xeroderma
a
ncreased
rsk
or
cancers
arsng
n
sun-exposed
skn.
rays
n
sung
cause
cross-nkng
o
pyrmdne
norma
DNA
repcaon.
Suc
DNA
damage
s
e
mporance
dscusson
resdues,
and
pre-
neopasms. venng
NEOPLASIA
o
consders
cancer
e
s
s
efecs
mpac
o
on
umors
paens.
on
er
he
o-
oss,
e
Uravoe
gradng (UV)
OF
pgmentosum
owng are
ASPECTS
Pigmentosum
repared
by
e
cnca
sagng
o
cancer,
and
e
aboraor y
dagnoss
o
84
CHAPTER
Neoplasia
5
Checkpoint
Anti-CTLA-4,
inhibitors
Avoiding
anti-PD-1/PD-L1
immune
Evading
destruction
Reactivation
growth
MDM2
suppressors
Sustaining
Enabling
proliferative
replicative
signaling
immortality
of
p53
inhibitors
EGFR
inhibitors
Deregulating
Tumor-
cellular
promoting
energetics
inflammation
Activating Resisting BCL2
inhibitors
invasion cell
and
death metastasis
Inhibitors
Genome
Inducing
of
PARP VEGF
instability
angiogenesis
signaling
inhibitors
and
mutation
Fig.
5.24
trials
are
Therapeutic
listed.
targeting
(From
Hanahan
of
D,
hallmarks
Weiberg
of
cancer.
RA:
The
Therapies
hallmarks
of
approved
cancer:
for
the
use
next
or
in
advanced
generation.
Cell
clinical
144:646,
2011.)
Clinical
Benign
lems
Effects
and
through
efecs
puar y
gand,
bones
by
L o ca y
or
nan
e
produce
paoogc
and
duc
oca
o
e
a
may
due
cancers
or
may
e ad
o
ca as ropc
s e condar y
o
nor ma
a
sympoms
and
varey
magnan
n
e
o
cancer
prog ressve
crc u a ng
ac ors
me ab osm
exp endure
p ar y
a r bue d
(TNF),
o o d
o
ems eves,
w c
p oproen
10%
o
or
15%
o
severa
cancer
paens,
reasons:
hey may be severe and, n some nsances, may even be ea
hey
aa
“space--
sma
bar y
ncude
cord
o
a
sur ace,
w
concurreny :
o
or
rod
ormone,
boacve
or unaey
rare
pasc
me cansms
wounds
by
measac
syndromes
Broncogenc
ca
ves-
non e a ng
mmc
dsease,
ereby
conoundng
rea-
are
dverse
and
are
assocaed
w
many
dferen umors (Tabe 5.7). One umor may nduce severa syndromes
maj or
no
may
pannng
Paraneopasc
rac
spna
compromse
a
men
carc-
•
avng
e
carcnomas
efecs
seroonn,
subsances.
o
ACTH,
uman
he
may
coronc
oowng
eaborae
andurec
are
e
producs
ormone,
gonadoropn,
and
mos
common
oten
caused
den-
paray-
oer
paraneo-
syndromes:
Hypercacema
ess
ma g-
o
e
endocrne
ses
o
adrena
adoserone,
rom
b o dy
and
and
a
o
a
n
cancer
parayrod
may
eadng
o
o
e
e
as
e
hes e
ac ons
o
e
ac vae d
e
pre ven ng
Tumor
umor
and
b as a
cacexa,
skee a
app e e
a
sodum
by
and
me ab oc
c yokne
app e e
o
rae
s
caus e d
ncre as e
n
canges
n
s
C a or e
ncre as e d,
abnor ma es
or
ne cross
by
umor
n bs
re e
ay
s
accomp a-
mus ce.
umor
and
ree as e
an
caus e
skee a
me ab oc
w c
mus ce
cacexa
bu
macropages
e
paens
s
mos
ormone–reaed
proen
by
(PTHrP)
e
by
syn-
umor
syndrome,
•
ce
e
are
ac-
ce s
ac on
acds
rom
carcnoma
Hypercoaguabty,
ra
romboc
e
Suspeced
reaed
o
reeased
Grading
is
rom
reaed
cancer
e
o
venous
s
coaguaon
ncude
ces
mos
o
ACTH
commony
(suc
romboss
prmary
efecs
as
reaed
acors
canges
pronlammaor y
umor
producon
s
seen
or
w
ung.
endocards,
o
o
ces,
(raer
n
o
mucns)
and
o
nonbace-
canges
an
endoea
cancer,
a
and
drecy
a
paees).
uncon
subsances
acvae
e
cascade.
and
and
used
o
conrbuors
Staging
staging
aggressiveness
that
by
eadng
acvy
e
coaguaon
Grading
usuay
ormones
of
a
when
of
are
given
Cancer
used
to
estimate
neoplasm
comparing
the
and
the
to
outcomes
probable
provide
of
a
different
clinical
standard
treatment
protocols.
he sage o e cancer (ow exensve s n e paen) s assessed
many
by
cnca
and
radoogc
sudes,
wereas
gradng
s
done
by
paoogc examnaon usng eaures a are descrbed beow. In gen-
Paraneopastc
w
sma
can
eabo-
Cusng
ACTH-ke
gands.
Langerans
corex
•
enance
tumor
and
anorexa
suc
suppress es
p as e,
o
n
common
ypokaema).
n a ke.
by
arsng
are
p oproens.
paens
n
mporan
•
producon
pancreac
(e.g.,
suppress
e
pro duce d
e
umors
demands
g
ormone
sufer
oss
ssues,
remans
re duce d
and
a
o
o
ormones
we a kness
nu r ona
o
neopasms
and
p a ens
proound
e
despe
ces
yperenson,
ne d
by
β
serod
by
by
reaed
ypernsunsm,
Many
s
norma
be e dng,
rep ar
appear
surroundng
Eroson
o
hey
recognon
hey may be e eares manesaon o an occu neopasm
roug
ne c on
umor
•
A
comparaby
ne c on
e
cnca
•
oca,
srucura
u cerae
s e condar y
o
er
(1-cm)
nduce
o
orgn
sma
e
compcaons
racures
o
and
effects.
umors.
desroy
prob-
umors.
can
marke d
o
and
be
ner erence
arsng
reenon,
or
magnan
systemic
ces.
and
bengn
Tumors
e
indirect
and
ce s.
w
no
and
local
deermnan
and
compress
common y,
o
cruca
mporan
be e dng
e ar
a
cause
ypopuarsm,
nvasve
due
Sgns
rae
and
s
may
direct
common
Oer
More
be
o
e
of
bengn
can
magnan
cons e quen
e ven.
bo
rse
wn
compresson
may
ocaon
o e umor or by e eaboraon o ormones ndgenous o e ssue
tumors
variety
adenoma
obsrucon.
s es
a
o
gvng
noma
Tumors
malignant
Anaomc
ng”
of
syndromes
cancer
a
are
canno
sympom
be
compexes
expaned
by
oca
or
a
occur
dsan
n
spread
era,
aoug
vaue
an
e
bo
are
umor
useu,
grade.
e
umor
sage
s
o
greaer
prognosc
CHAPTER
Table
5.7
Clinical
Paraneoplastic
Neoplasia
5
85
Syndromes
Syndrome
Associated
Neoplasms
Causal
Mechanism(s)/Agent(s)
Endocrinopathies
Cushing
syndrome
Small
cell
lung
Pancreatic
Neural
Syndrome
mone
of
inappropriate
secretion
antidiuretic
hor-
Small
(SIADH)
Breast
Hypoglycemia
cell
ACTH-like
Antidiuretic
substance
lung
carcinoma
Parathyroid
TNF ,
or
atrial
natriuretic
hormone–related
protein,
TGF- α,
IL-1
leukemia/lymphoma
Insulin
mesenchymal
Ovarian
hormone
hormones
Fibrosarcoma
Muscle
or
carcinoma
T-cell
Other
and
carcinoma
neoplasms
carcinoma
cell
Adult
Nerve
lung
Squamous
Renal
ACTH
tumors
cell
Intracranial
Hypercalcemia
carcinoma
carcinoma
or
insulin-like
substances
sarcomas
carcinoma
Syndromes
Myasthenia
Lung
carcinoma
Immunologic
Thymoma
Disorders
vous
of
the
central
and
peripheral
ner-
Breast
systems
Dermatologic
Acanthosis
carcinoma
Disorders
nigricans
Gastric
Lung
carcinoma
Lung
Articular,
of
the
Soft
Tissue
and
and
Hematologic
thrombosis
Lung
(Trousseau
Pancreatic
aplasia
carcinoma
products
syndrome
Gradng.
umor
Gradng
ces
presence
eac
grade
o
essence,
and,
s
n
o
g
umors
o
hormone;
based
some
ceran
ype
and
specc
IL-1,
on
e
arcecura
grade)
are
interleukin-1;
cancers,
magnancy
judge
norma
Erythropoietin
o
descrbed
e
o
range
n
aer
aggressveness
o
wo
e
or
o
e
e
counerpars.
Aoug
soogc
gradng
as
TNF ,
vaue,
boogc
e
beavor
correaon
s
ar
rom
beween
soogc
mar y
eson,
e
presence
sagng
sysem
Cancer
TNM
or
exen
n
cc
orms
eson
used
T
spread
bood-borne
or
hs
use
s
sysem
prmar y
o
e
n
based
clotting
secretion
by
tumor
cells
ymp
a
N
nodes,
Jon
he
regona
and
major
caed
ymp
and
M
cancer,
or
measases.
bu
ere
caracerzed
wereas
and
wereas
M1
number
o
an
n
N1
o
range
o
or
as
T1
su
are
o
T4
eson.
N3
somemes
M0
M2
based
N0
denoes
nodes.
TNM
genera
sagng
on
no
nvovemen
sgnes
e
he
ncreasng
ndcaes
relecs
vares
prncpes.
no
sze;
noda
o
an
dsan
presence
or
spe-
prmar y
T0
s
nvove-
ncreasng
measases,
and
esmaed
measases.
Diagnosis
and
C ommee
casscaon
or
o
complexes
factor.
prog-
appearance
measases.
Amercan
uses
umor,
regona
necrosis
ndcae
number
No
s
s
o
men,
o
perec.
o
curren
Sagng.
sysem:
o
absence
tumor
nvovemen,
(ow
aemp,
oten
factor- α;
dfer
gradng
a
ces,
growth
and
scemes
bu
umor
Immune
caegores
Crera
capers,
o
moses
Gradng
rom
caegores.
cancers
transforming
dferenaon
number
eaures.
and
our
degree
e
TGF- α,
Stagng. he sagng o sod cancers s based on e sze o e pr-
on
tumor
activate
carcinoma
Cancer nosc
e
secreted
that
hemangioma
on e exen o wc e umor ces resembe (or a o resembe)
•
to
Immunologic
carcinoma
Various
Adrenocorticotropic
er
due
mucins)
factors
Thymoma
Renal
(e.g.,
Dysfunction
Nephrotic
or
Hypercoagulability
cancers
Hepatocellular
•
Unknown
carcinoma
Cerebellar
ACTH,
Immunologic
carcinoma
Changes
phenomenon)
Polycythemia
Renal
growth
carcinoma
carcinoma
Other
cell
epidermal
Changes
clubbing
Lung
Red
of
fingers
Vascular
Venous
and
osteoarthropathy
secretion
factor
carcinoma
Breast
Hypertrophic
Immunologic;
carcinoma
Uterine
Dermatomyositis
Osseous,
Immunologic
Teratoma
e
node
matter
diagnosis
of
cancer
Ever y
becomes
Eac
o
strongly
cancer
sampling
of
is
suspected
tissues
and
on
clinical
histologic
grounds,
identication
cells.
year
more
e
avodng
how
requires
e
approac
compex,
oowng
deas
o
o
more
secons
e
aboraor y
sopscaed,
aemps
ecnooges.
o
dagnoss
and
presen
more
e
o
cancer
specazed.
sae
o
e
ar,
86
CHAPTER
Morphologic
In
mos
n
many
e
O pen
sue
no
w
or
d c u
ma g nan
e quvo c a
are
o
ce s
e
o
ar r ve
ana ys s
a
c an
c anc er
b as e d
m cros c op e.
mor po og c
ess en a
mor poog c
d ag nos e
under
canges ,
e
be
on
cn c a
d ag nos s.
ac e ve d
e
Howe ver,
and
S ampng
roug
e
pro ce dures :
(surgca)
or
bopsy.
sampng
examned
on.
s
e
e aures
umor
o ow ng
•
o
c as es
radoog c
o
Methods
ns ances,
app e arance
Neoplasia
5
In
by
e
some
secton.
hs
saned,
on
roune
cases,
e
meod,
and
evauaon
hs
based
gross
s
wc
sen
a
under
severa
e
opporuny
appearance.
he
emaoxyn-and-eosn
bopsy
n
examned
wn
afords
s
or
sampe
e
mnues.
rapd
s
e
seec
sans
evauaon
vas
by
be
xa-
frozen
seconed,
perms
majory
s-
can
ater
quck-rozen,
mcroscope,
In
o
bopsy
soogc
o
cases,
ro-
A
zen-secon
dagnoss
ngusng
some
•
Fne-neede
evauang
spread
can
aso
se.
ands
a
used
s
ess
e
Cytoogc
luds
cancer.
cer vx
o
a
rapd,
(Fg.
s
bu
and
s
n
ds-
denyng
used
I
bopsy,
specc
meod
or
aspraon
s
used
mos
mage
n
means
re-
gudance
vruay
and
are
any
body
experenced
o
deny
(or
esons.
rom
ssue
meod
deny
ecnque
useu
and
by
w
nvovng
surgca
preparatons
o
wdey
examned.
morpoogc
deveoped
be
umors
wdrawn
masses
cancerous
anoer
5.25),
and
sensve,
o
(Papancoaou)
Inay
anoer
esons,
an
can
necon).
Ces
saned,
examne
presence
provde
s
papabe
and
magnan
(e.g.,
(FNA)
nvasve
accuracy
and
masses.
sde,
evauae
provdes
excude)
or
on
be
FNA
bengn
aspraton
o
g
processes
suspcous
ou
queny
•
beween
nonneopasc
as
or
scrapes,
e
precancerous
now
used
o
FNAs,
deecon
esons
evauae
o
o
e
suspeced
B magnancy
na,
n
peura,
many
oer
percarda,
ses;
and
o
deny
umor
cerebrospna
ces
luds;
n
and,
abdom-
ess
com-
Fig.
5.25
smears,
mony,
or
evauaon
o
oer
orms
o
smear
nuclei.
Protein
few
o
proens
or
oer
moecues
expressed
by
umor
broad
roe
n
esabsng
e
dagnoss
o
specc
cancer
•
Severa
compemenar y
Immunostocemstry
Tssue
secons
are
s
meods
a
saned
are
poweru
ce
o
among
pe,
e
cancers
dagnoss
Fow
usng
bodes
In
o
aed
w
a
meod
s
n
used
ce
e
o
a
roune
empoys
n
o
e
can
•
containing
Nuclear
eary
dsease
Markers
be
o
drugs
and
magnan
and
o
oer
ess
or
umor
uterine
are
cervix.
(A)
typical.
In
(B)
normal
Abnormal
sheet
of
malignant
is
cells
evident,
with
and
large
one
cell
hyperchromatic
a
recurrence
are
n
n
paens
curren
use
are
Cytogenetic
much
smaller
in
size
is
and
in
mitosis.
with
A
compact,
are
seen.
(Courtesy
University
of
of
Dr.
Richard
M.
DeMay,
Department
Chicago.)
o
For
demonsrae
and
en
and
ym-
luorescen
an-
anayzed
angens
or
a
sed
nances
umor
•
or
markers
cancers;
are
used
owever,
known
n
Tabe
cancer
dagnoss
o
emaopoec
cancers
suc
as
eu-
and
o
parain-embedded
acd
probes
ecnque
o
deny
bnd
can
be
secons
w
used
parcuar
n
specc
o
wc
arge
subype
luoresceny
regons
emaoogc
cromosoma
aberraons
o
e
mag-
n
any
ype
genome
n
anayss.
w
hs
Hybrdzaton
e
umor-assoc-
or
nucec
genome.
san-
e
ympomas.
sampes
abeed
canges
assays
ceran
suppor
and
Fuorescence n stu ybrdzaton (FISH) s a meod perormed on
res
e
ces.
umor
w
•
anbodes.
eukemas
o
exam-
o
bran
of
tumor
perms
copy
hs
DNA
e
number
meod
s
to
arrays
dencaon
a
used
are
o
of
o
beow
DNA
sma
e
dagnose
probes
deeons
resouon
and
subype
o
a
and
span
oer
kar yoypc
ceran
knds
umors.
ey
dagnoss.
5.9
Nucleic
A
Acid
number
response
o
o
Markers
ecnques
erapy
sequences
or
used
nvove
o
e
ragmens.
dagnose
umors
dencaon
Cncay
o
and
oow
specc
reevan
DNA
exampes
o
er
and
suc
Markers markers
subypes
o
cancer
aberraons;
a
ew
are
gy
saen
assocaed
exampes
o
w
suc
parcuar
assocaons
cromo-
are
gven
n T abe 5.8, aong w nucec acd markers dscussed aer. Cyogenec
meods
neutrophils,
Conventona karyotypng o meapase cromosomes s requeny
kemas
esabses
dferenaon
are
Bocemca
screenng
used
combnaons
wc
nuclei,
Pathology,
RNA
soma
a
pleomorphism
interspersed
used
dsngusng
are mos useu n assessng e response o erapy and n deecng
Many
the
nuclei
soog y.
anbodes
appearances.
casscaon
moecues
markers.
and
dferenaed
erapeuc
suspenson,
ormones,
as
aso
varous
surace
n
cancers
morpoogc
poory
I
penoype
tumor
success
a
arges
meod,
ces
enzymes,
var yng
smar
carcnoma.
s
oban
dferenaed
o
proen
o
Crcuatng
poory
keran
agans
bound
ng
•
o
o
o
cytometry
pomas.
are
orgn
deecon
presence
•
from
small
used:
adjunc
specc or proens o neres. hs meod s useu n deermnng
e
with
subof
ypes.
smears
cells
ces lobate
a
flat
Markers
Idencaon
as
Papanicolaou
large,
neopasa.
commony
used
o
deny
cromosoma
aberraons
ncude:
wc
•
are
sed
esng
Cmerc
oten
hese
s
n
done
nucec
creae
Tabe
mos
acd
uson
sequences
5.8
e
are
sequences.
genes
are
Among
requeny
encodng
ypes
e
o
abnormaes
Cromosoma
cmerc
umor-specc
and
or
oowng:
rearrangemens
mRNAs
can
be
and
proens.
deeced
even
CHAPTER
Table
5.8
Affected
Examples
of
Cytogenetic/Molecular
Markers
of
Importance
in
Specific
Neoplasia
5
87
Cancers
Gene/
Chromosomal
Region
Chromosomal
Event
Detection
Translocations/Fusion
ABL
Fusion
with
through
BCR
9;22
Clinical
Importance
Genes
gene
Karyotype,
FISH,
RT-PCR
Diagnosis
translocation
of
of
chronic
therapy;
tic
myeloid
marker
response
and
used
leukemia;
to
diagnose
follow
target
therapeu-
minimal
residual
disease
Gene
Amplification
NMYC
Gene
amplification
FISH
HER2
Gene
amplification
FISH,
Marker
IHC
Target
of
of
poor
prognosis
therapy
in
in
neuroblastoma
“HER2-positive”
breast
cancer
Chromosomal
Deletion(s)
1p
Segmental
deletion
FISH,
DNA
array
Diagnosis
good
Point
of
oligodendroglioma;
marker
of
prognosis
Substitution
JAK2
Valine
for
phenylalanine
substitution
Table
5.9
Circulating
Tumor
in
codon
DNA
sequencing
Diagnosis
617
blood
Tumor
antigen
polycythemia
vera
(a
type
of
Markers
Marker
Prostate-specific
of
cancer)
(PSA)
Use
Prostatic
carcinoma
Screening
test
(controversial);
following
response
to
therapy
Human
chorionic
gonadotropin
(HCG)
Choriocarcinoma
Some
Alphafetoprotein
(AFP)
Germ
mixed
cell
germ
antigen
(CEA)
Colonic
CA-125
presen
n
ver y
ow
abundance
usng
carcinoma
sensve
poymerase
can
reacon (PCR) meods. Many emaopoec neopasms, as we as
a
ew
sod
genes.
o
In
drugs
erapy.
can
be
er wse
•
umors,
oer
and
so
are
Fnay,
used
o
are
dened
nsances,
by
deec
o
presence
o
deec
PCR-based
sma
asympomac
e
producs
mporan
sensve
Snge-nuceotde
e
numbers
or
ess
o
o
uson
parcuar
genes
purposes
or
cancer
uson
are
o
cmerc
resdua
arges
seecng
sequences
ces
n
o-
paens.
varants
and
“ndes. ”
As
w
cmerc
gene
producs, snge-nuceode varans (pon subsuons) and ndes
(sma
and
nserons
ereore
oncoproens
deec
•
or
based
a
ve)
are
purposes
unque
deecon
dsncon
deeons)
dagnoscay
Antgen-receptor
exbs
and
o
gene
drug
arges
proeraons
o
recepor
monocona
o
and
and
rearrangements.
T-ce
beween
specc
or
n
some
oer
ereore
cancer
cases
are
ypes
generae
mporan
o
erapy.
rearrangemens
o
are
mporan,
gudng
•
s
or
T
angen-recepor
mmunogobun
(neopasc)
ympocyes.
eac
and
therapy
Following
response
to
therapy
and
B
genes,
genes
poycona
ce
PCR-
aows
(reac-
Following
response
to
therapy
Following
response
to
therapy
prong
deveoped
o
assess
of
anayze
epgenec
cancers.
a
snge
Dverse
gene,
modcaons
ecnooges
sequence
an
genome-wde,
ave
enre
quany
been
genome,
a
o
e
RNAs expressed n a ce popuaon, measure many proens smu-
aneousy,
advances
and
ave
aeraons
cay
cos.
nex
For
owever,
suppressor
perormed
accurae
uar
be
genes.
on
mos
ceners
esons
a
on
ecnques.
a
o
new
e
he
mey
ceners
e
o
o
o
and
mpac
now
a
n
usuay
oreseeabe
prognoss
perorm
w
and
normaon
uure,
e
cancer
and
gene
umor
bomarker
n
morpoogc
o
n
reasonabe
rouney
su
been
erapeu-
a
compemen
and
as
deny
ason
hese
caaogng
proooncogenes
ecnques
assessmen
meaboes.
specmens,
soog y
combnaon
man
seekng
a
umor
For
ce’s
sequencng
muaed
secons.
and
by
are
n
academc
convenona
ssue
a
cancers.
commony
hese
o
sysemac
uman
many
dagnoss
arrved
e
sequencng
cover
rom
snapso
genec
exampe,
a
a
varous
generaon
panes
w
n
ake
enabed
“aconabe”
obaned
Because
to
Moecuar
researc;
sma
response
carcinoma
carcinoma
Ovarian
Following
tumors
tumors
Hepatocellular
Carcinoembryonic
cell
ess
mos
paens
new
moec-
6
Genetic
Diseases
O U T L I N E
Mendelian Disorders: Diseases Caused
by
Single-Gene Defects,
Transmission
Diseases
Proteins,
Diseases
of
Single-Gene
Disorders,
88
by
Mutations
in
Genes
Encoding
Structural
by
Mutations
in
Genes
Encoding
Receptor
or
Channels,
by
97
Disorders
Involving
Autosomes,
Cytogenetic
Disorders
Involving
Sex
Trinucleotide
Caused
Proteins,
Abnormalities,
Cytogenetic
Single-Gene Disorders
90
Caused
Proteins
Diseases
Patterns
Caused
Structural
88
with Atypical
Repeat
Mutation
Diseases
Caused
by
Mutations
Diseases
Caused
by
Alterations
Patterns
Diseases,
in
98
Chromosomes,
100
of Inheritance, 101
101
Mitochondrial
Genes,
102
90
Mutations
in
Genes
Encoding
Enzyme
Prader-Willi
and
Angelman
of
Imprinted
Syndromes,
Regions:
102
93 Diagnosis of Genetic Disorders, 102
Complex
Multigenic
Disorders,
96 Genetic
Cytogenetic
Disorders,
Test
Indications
Numerical
Genec
Abnormalities,
abnormaes
Modalities
and
Applications,
102
97
a
for
Genetic
Analysis,
104
97
cause
ceuar
dysuncon
are
one
o
e
produced
prnc-
or
pa causes o dsease. Some genec dseases are nered (ama) due o e
by
sgnang
muaons
n
genes
beongng
o
e
same
meaboc
paways.
presence o germne muaons, wereas oers sem rom acqured somac
Transmission
Patterns
of
Single-Gene
Disorders
muaons (e.g., cancer) and are no ransmed rom one generaon o e
nex. I s mporan o dsngus beween congena and genec dsorders.
Congena
means
“born
w ”;
some
genec
dseases
are
congena
(e.g.,
penykeonura), wereas oers are manes aer n e (e.g., Hunngon
dsease).
Conversey ,
congena
or
syps).
paogencay
no
In
a
s
congena
caper,
neresng
we
genec
dseases
dscuss
dseases.
are
genec
some
W e
o
e
n
orgn
more
concude
e
(e.g.,
common
caper
Autosomal
Dominant
Disorders
Autosomal
dominant
disorders
fested
mal
the
by
revewng curren ecnooges a are used o dagnose genec dsease.
DISORDERS:
DISEASES
allele
Wen
c d
•
CAUSED
the
heterozygous
(out
as
one
a
SINGLE-GENE
e aures
Reduced
three
caused
patterns
autosomal
by
of
single-gene
Mendelian
recessive,
Aoug
rare
or
defects
(mutations)
inheritance:
follow
autosomal
one
of
•
dominant,
6%
o
dseases
ype
8%
o
oow
ndvduay
a
assocaons
are
6.1),
aken
ogeer
mendean
kep
•
n
mnd
ospa
paerns
o
somemes
wen
admssons.
nerance,
compex,
bu
Mos
snge-gene
consderng
reecng
mendean
dsease-assocaed
e
dverse
unc-
o
some
correae
cases,
w
may
dsorders:
genoype
are
penoypcay
Mutatons
types.
88
n
hs
genes)
is
of
are
one
sufcient
mani-
abnor-
to
cause
o
and
av ng
o
and
o er
e
s
ds e as e.
auos oma
varable
ner
e
e
on
o ow ng
dom nan
expressvty
deecve
no,
Te
gene
are
aver age
e ac
add -
ds e as es :
common.
deveop
e
No
a
dsease,
genoypes
be
n
expaned
dferent
genes
penomenon,
knd
o
dsease,
even
wn
one
or
amy.
and
symptoms. Because a 50% oss o enzyme acvy usuay
suc
by
cases
s
no
conerance
we
o
undersood.
varans
n
may
cause
ermed
smlar
genetc
or
dentcal
eterogenety,
dsorders
encode
compexes,
componen”
proens
oer
an
enzymes,
suc
as
or
a
wc
may
nereres
mumerc
be
w
dsruped
e
assembes.
by
ormaon
A
proen
e
o
a
presence
e
o
a
uncona
“posons”
e
•
In many autosomal domnant condtons, te age at onset s delayed,
•
Not all afected patents ave afected parents. Assumng e absence
wt
symptoms
and
o
nonpaerny,
o
new
were
n
muaons
derved.
sgns
suc
rst
paens
nvovng
her
appearng
sbngs
e
are
e
egg
n
adultood.
dsorder
or
e
unafeced
s
usuay
sperm
and
rom
no
a
arbuabe
wc
ey
rsk.
In
oer
Disorders
Autosomal
peno-
s
usuay
acvy o s norma counerpar s caed a domnant negatve.
norma;
genes a mpac e penoype; ese are caed moder genes.
•
a e c e d
p er a n
wo
muproen
n s suaon, e ra s sad o ave low penetrance. Wy penoypes
a
sgns
“bad
uas, a penomenon caed varable expressvty. In oer nsances, some
a
a s o
ger-order
genoype–peno-
duce many penoypc efecs (pleotropy) a may dfer among ndvd-
w
and
srucura proens, ranspor proens, or proens a uncon wn
Penotypc efects o specc sngle-gene mutatons vary wdely. Some pro-
persons
s
cance
penetrance
same
nan
ons o varous afeced gene producs (Tabe 6.2). Severa caveas mus
be
autosomal
sexes
inheritance
can be compensaed or, e genes a are afeced n auosoma dom-
(Tabe
pedarc
smpe
for
both
the
A 50% reducton n te normal gene product s suicent to produce cln-
cal
X-linked.
dsorders accoun or approxmaey 1% o a adu ospa admssons
and
two
so
DEFECTS e
Diseases
the
p aren
50%
ndvduas
BY
of
affect
state,
disease.
ona
MENDELIAN
in
oten
lian
a
of
Autosomal
recessive
disorders,
gene.
are
Recessive
diseases,
caused
by
which
genetic
Inheritance
are
the
defects
largest
that
group
alter
of
both
mende-
alleles
of
CHAPTER
As
by
•
e
he
a
•
a
genera
rue,
auosoma
recessve
dsorders
are
caracerzed
•
Reduced
oowng:
ra
25%
does
cance
n
no
o
usuay
beng
afect
te
parents,
wereas
eac
sblng
as
afected.
te
eous
afected
patent
(te
proband)
s
te
product
o
a
rers
consangun-
of
S e l e c te d
Disorder
Me ndelian
Estimated
o
te
Dseases
Dominant
kidney
disease
1
in
500
1
in
1000
resultng
because
spherocytosis
1
syndrome
in
5000
(Northern
disease
Recessive
1
in
5000
1
in
10,000
1
rers
in
400
(U.S.
be
afected.
Aoug
new
rom
enzyme
are
decences
normay
are
usually
presen
n
arge
deecs
n
bo
autosomal
excess
resulng
rom
and
alleles,
produce
are
penoypes.
fibrosis
to
cance
1
in
3200
(U.S.
Caucasians)
1
in
3500
(U.S.
Ashkenazi
Jewish;
1
Mucopolysaccharidoses—all
types
1
in
in
1
in
are
X-linked
frequently
recessive
are
than
and
therefore
caracerzed
by
females.
e
oowng:
o
ofsprng,
as
wo
emzygosty).
ave
ony
Sons
o
one
X
cromosome
eerozygous
women
(a
sae
ave
French
n
wo
o
recevng
e
muan
one
gene.
An afected male does not transmt te dsorder to sons, but all daug-
•
Because males ave only one “dose” o most X-lnked genes, deects n
•
Heterozygous
o
afected
males
are
carrers.
Canadians)
genes
are
lkely
to
produce
dsease
n
males.
10,000
emales
rarely
ave
te
ull-blown
dsease
because
tey
25,000
ave
diseases—all
dsorders
male
X-lnked Phenylketonuria
more
•
ters disease
disorders
much
African-Amer-
icans)
storage
o
males
reerred
Glycogen
may
he dsease s transmtted by asymptomatc eterozygous emale car-
Inheritance
anemia
Tay-Sachs
one
Disorders
X-nked
Cystic
least
Europe)
•
cell
at
enzymes
decences,
X-linked
affect
Sickle
or
Prevalence
Most
Autosomal
gene,
Inheritance
hypercholesterolemia
Huntington
mutant
severe
X-Linked
Marfan
tan
Dis o rd e rs
suicen
Hereditary
common
muaons or recessve dsorders do occur, ey rarey produce peno-
ony
Polycystic
less
Most autosomal recessve dseases are nerted rom parents wo are car-
recessve
Familial
are
ypes because o e keood a e oer aee w be norma.
Prevalence
Autosomal
expressvty
dsorders.
Onset s requently early n le.
•
6.1
varable
89
•
marrage.
Table
and
domnant
Diseases
•
I te mutant gene s rare n te populaton, tere s a strong lkelood
tat
penetrance
autosomal
Genetic
6
a
normal
allele.
However,
genoype–penoype
assocaons
50,000
n
emaes
are
compcaed
by
e
penomenon
o
X-nactvaton
types
(lyonz aton),
X-Linked
Duchenne
Inheritance
muscular
wo
dystrophy
1
in
3500
males
(U.S.)
1
in
5000
males
(U.S.)
X
cromos omes
cromos ome
average, Hemophilia
roug
express
a
e
a
o
s
are
mo s
s ence d
nac vae d
ce s
nor ma
w c
express
a ee.
s
e
In
o
e
e ary
n
“cos en”
mu ae d
mos
genes
on
one
de veopmen .
a
r andom ;
a ee
ns anc es ,
and
s
s
o
e
T e
enc e,
a
o
X
on
c e s
su c en
o
a
G6PD
deficiency
1
in
10
males
(U.S.
African-
bun
or
compeey
suppress
e
d s e as e
peno yp e,
bu
on
o c c a-
Americans)
son
ere
s
pronounce d
ske w ng
oward
s enc ng
o
e
nor-
a
Glucose-6-phosphate
dehydrogenase.
ma
Table
6.2
Biochemical
Basis
and
Disease
Marfan
Pattern
Abnormal
Autosomal
Familial
Inheritance
Dominant
of
Selected
a ee
(unavorabe
Mendelian
Protein
yon za on ).
Und er
suc
Disorders
Protein
Function
Inheritance
hypercholesterolemia
Low-density
syndrome
lipoprotein
receptor
Cholesterol
transport
Fibrillin
Extracellular
matrix
protein
Collagen
Extracellular
matrix
protein
a
Ehlers-Danlos
Hereditary
syndrome
spherocytosis
Neurofibromatosis,
Adult
polycystic
Autosomal
Cystic
type
kidney
1
ankyrin,
Neurofibromin-1
disease
Recessive
fibrosis
Spectrin,
Polycystin-1
CF
Hexosaminidase
disease
β-Thalassemias
cell
X-linked
anemia
Recessive
Hemophilia
Duchenne
Fragile
X
dystrophy
syndrome
a
Some
forms
are
autosomal
Cell
membrane
Regulator
Cell:cell,
of
stabilizer
RAS
signaling
cell:matrix
interactions
regulator
hydroxylase
Ion
channel
Enzyme
Enzyme
Hemoglobin
Oxygen
transport
Hemoglobin
Oxygen
transport
Factor
Coagulation
Inheritance
A
muscular
(NF-1)
transmembrane
Tay-Sachs
Sickle
4.1
Inheritance
(CF)
Phenylalanine
and
protein
(PKD-1)
Phenylketonuria
α-
or
recessive
disorders.
VIII
Dystrophin
Cell
FMRP
RNA
factor
membrane
translation
stabilizer
regulator
crc ums anc es ,
90
CHAPTER
ema es
ess er
may
exb
deg re e
Diseases
an
Caused
Genetic
6
e aures
a e c e d
by
o
e
Diseases
ds e as e,
oug
usu a y
o
a
Ehlers-Danlos
Mutations
in
Genes
Ehlers-Danlos
syndromes
orders
by
caused
are
a
collagen
heterogeneous
genes
or
genes
group
that
of
dis-
regulate
assembly.
are
sngle-gene
dsorders
a
may
ave
auosomal
Syndrome
domnan Marfan
syndrome,
a
connective
tissue
disorder
of
autosomal
inheritance,
is
caused
by
mutations
affecting
e
Fbrn-1
s
encoded
by
e
FBN1
recessve
modes
o
nerance.
A
leas
sx
varans
are
clncal
varans
are
and
recognzed.
brillin-1.
• Pathogeness.
or
domgenec
inant
in
Proteins
Pathogeness. EDSs
Marfan
(EDS)
defects
Encoding collagen
Structural
Syndromes
ma es.
gene,
wc
maps
molecular
Deicency
of
bases
e
o
e
enzyme
more
ysy
common
ydroxyase.
In
s
as
ollows:
varan
called
e
o kyposcoloss ype, decreased ydroxylaon o lysne resdues n ypes
cromosome
15q21.
I
s
a
gycoproen
secreed
by
broblass
a
s I
e
major
componen
o
mcrobrls
ound
n
e
exracellular
and
III
collagen
molecules. o
many
ssues.
Mcrobrls
provde
a
scafold
a
enables
nereres
w
e
covalen
cross-lnkng
o
collagen
marx
e
As
w
oer
enzyme
decences,
s
dsease
s
nered
e
vascular
proper as an auosomal recessve dsorder.
assembly
o
elasc
bers
and
are
parcularly
abundan
n
e
aora,
•
D eicen
syness
of
ype
III
coagen.
s
varan,
e lgamens, and e clar y zonules o e ocular lens, predcably e ype, ssues
a
are
mos
promnenly
afeced
n
Maran
s
nered
abnormales
n
Maran
syndrome
are
arbuable
o
by
alure
o
connecve
ssues.
However,
oers,
suc
as
weakness
bowel
appear
o
be
relaed
o
excessve
domnan
dsorder
and
s
ransormng
o
ssues
rc
n
ype
III
collagen
carac-
(e.g.,
wall),
predsposng
em
o
rupure.
e
blood
causave
bone muaons
overgrow,
auosomal
a vessels,
srucural
an
syndrome. erzed
Many
as
grow
oten
lead
o
e
expresson
o
a
deecve
collagen
III
acmonomer a nereres w assembly o normal collagen, a classc
or-β
(TGF-β)
acvy.
Normal
mcrobrls
sequeser
TGF-β,
and
loss example
o
mcrobrls
ereore
ncreases
e
boavalably
o
s
• Excessve
TGF-β
sgnalng
as
deleerous
efecs
on
o
a
“domnan
negave”
muan.
cyokne.
vascular
D eicen
syness
of
ype
V
coagen.
s
varan
s
also
nered
smoo as an auosomal domnan dsorder and resuls n classc EDS. More
muscle
developmen
and
e
negry
o
e
exracellular
marx.
O an
noe,
angoensn
recepor
blockers,
wc
lower
blood
pressure
90%
encode nb
mouse
e
acvy
models
o
o
TGF-β,
Maran
mprove
aorc
and
cardac
uncon
e
eye,
•
and
Skeea
Abnormales
e
mally
suc
Paens
long
arced
cardovascular
abnormaes
syndrome.
legs,
palae;
as
Baera
e
Clncal
ocular
mos
promnen
sysem,
e
a
as
mos
and
may
excavaum
skeleon,
eaure
o
Maran
abus;
(aracnodacyy);
jons.
presen.
(a
e
deeply
Spnal
e
ces
depressed
abnor-
a
g-
deormes
s
deormed,
sernum)
s
abnormal
or
a
and
(subuxaon)
lgamens
s
of
(ecopa
e
ens
ens)
abnormaly
suggesve
C ardovascuar
sysem
Fragmenaon
because
o
n
8).
o
o
a
s
dagnoss
abnormaes
o
e
elasc
aneurysmal
ese
yperenson
o
and
o
ssue
jons
n
collagen,
mos
lack
rauma
are
suc
varans
adequae
n
njures
as
o
ensle
ypermoble
Mnor
ssues
also
ncludng
cornea
and
s
so
due
e
o
weakness
mos
e
genes
a
skn,
EDS.
sreng,
e
skn
produce
lgamens,
Because
e
also
gapng
e
skn
s
s
ragle
deecs,
and
may
ack
lead
rupure
renal
o
norma
o
oer
e
deacmen;
ense
colon
and
sreng.
serous
and
njures
large
e
n
areres;
dapragmac
deec
e
n
absence
rupure
o
erna.
specc
a
s
Diseases
Caused
Receptor
Proteins
o
Maran
consue
a
bers
dlaon
n
e
and
canges,
and
w
called
cysc
agng.
Loss
meda
medal
e
aorc
valve
rng,
gvng
rse
rea
o
e
also
suppor
o
in
Genes
Encoding
Channels
pres-
Hypercholesterolemia
hypercholesterolemia
aorc
is
caused
most
commonly
by
muta-
o in
the
gene
that
encodes
the
receptor
for
low-density
lipopro-
aora
dssecon
medonecross,
o
Mutations
or
syndrome.
serous
aorc
by
o
caracer-
(LDL)
and
is
characterized
by
high
serum
cholesterol
levels
(see early-onset
atherosclerosis.
occur
causes Pathogeness.
dlaon
rc
n
bers
connecve
rauma,
e
and Caper
Tssues
nvolved
collagen
connecve
tein predsposes
are
vulnerable
tions fe.
muaons
surgcal repar or ner venon s accomplsed only w grea dicuy
Familial
•
carr y
deormy.
cange.
gly
paens
collagen.
Features.
jons,
Familial
ence
afeced
V
yperexensble
elongaed
ngers
be
n
ollows:
obvous
slender,
yperexensble
dsocaon
suspensor y
sc
arms,
and
pecus
pgeon-breas
•
are
ave
kyposcooss
exbng
are
ype
n
syndrome.
and
Morphology.
o
and
Famlal
ypercoleserolema
s
an
auosomal
domnan
ncomdsorder w a requency o 1 n 500 n e general populaon, makng one
peence.
e
cardac
valves,
especally
e
mral
valve,
may
be o e mos common mendelan dsorders. Undersandng s paogeness
excessvely
dsensble
and
regurgan
(loppy
vave
syndrome), requres a workng knowledge o normal coleserol meabolsm.
gvng
rse
o
mral
valve
prolapse
and
congesve
cardac
alure Coleserol may be derved rom e de or rom endogenous syne-
(see
Caper
8).
Dea
rom
aorc
rupure
may
occur
a
any
age ss. Deary coleserol s ncorporaed n e nesnal mucosa no cy-
and
s
e
mos
common
cause
o
dea.
Less
commonly,
cardac lomcrons,
alure
s
e
ermnal
Some
s
Clncal Features. e prevalence o Maran syndrome s esmaed o
be
1
res
n
5000.
are
cells
o
more
mos
sporadc,
an
600
paens
exbs
par,
Approxmaely
parens.
wde
rom
arsng
dsnc
70%
rom
Molecular
are
de
causave
penoypc
efecs
o
85%
novo
dagnoss
dagnosed
dferng
wc
are
delvered
o
e
lver
and
aken
up
by
epaocyes.
even.
cases
FBN1
no
on
a
specc
n
e
n
large
o
e
a
e
germ
ere
FBN1
sem,
muaons.
and
e
because
eaures.
beleved
FBN1
amlal
muaons
clncal
s
are
roune,
muaons
based
varaon
o
s
o
are
gene;
dsease
leas
n
o
s
excreed
erol
also
coleserol
no
s
e
eners
blary
syneszed
by
e
rac
as
meabolc
ree
epaocyes
pool
coleserol
and
(see
or
released
laer),
ble
no
and
acds.
e
some
Coles-
crculaon
(Fg. 6.1). e rs sep n s process s e secreon o rglycerde-rc
very-low-densy
lpoproen
(VLDL)
no
e
blood.
Wle
n
e
crcu-
laon, e VLDL parcle loses rglycerdes roug e acon o lpases
expressed
by
lpoproen
endoelal
(IDL)
and
cells
and
low-densy
s
convered
lpoproen
o
nermedae-densy
(LDL).
e LDL recepor paway akes up wo rds o crculang LDL par-
cles, as well as IDL parcles, wereas e res o e LDL parcles are aken
CHAPTER
Genetic
6
Diseases
91
wc s e rae-lmng enzyme n e synec paway; (2) smulaes e
ormaon o coleserol esers, a sorage orm o coleserol; and (3) nbs
e
syness
and
down-regulaes
e
number
o
LDL
recepors
on
e
cell
surace, proecng cells rom e excessve accumulaon o coleserol.
In
most
mutations
lism,
instances,
in
the
resulting
Overall,
familial
LDL
in
hypercholesterolemia
receptor
accumulation
LDL receptor
protein
that
of
cholesterol
mutations
LDL
account
impair
for
90%
is
caused
LDL
in
of
by
metabo-
the
plasma.
cases.
e paucy o LDL recepors on lver cells also mpars e ranspor o
IDL no e lver, so a greaer proporon o plasma IDL s convered no
LDL.
Paens
levels
o
bosyness.
upake
w
amlal
coleserol
no
as
a
ypercoleserolema
resul
o
bo
Hypercoleserolema
macropages
and
reduced
leads
vascular
o
walls
us
ave
caabolsm
an
ncrease
medaed
g
and
n
by
serum
excessve
coleserol
e
LDL
scav-
enger recepor, resulng n premaure aeroscleross and coleserol-rc
deposs
n
sot
ssues
called
xantomas.
Mos
o
e
remanng
cases
o
amlal ypercoleserolema are caused by muaons n e gene encod-
ng
Apo
wc
ese
B-100
proen
conrols
(6%–10%
degradaon
muaons
are
o
clncally
o
LDL
cases)
or
recepor
muaons
(2%
ndsngusable
o
n
cases).
rom
PCSK9
gene,
Paens
ose
w
w
amlal
ypercoleserolema caused by LDL recepor muaons.
Clncal
caused
Features.
by
plasma
LDL
Heerozygoes
recepor
coleserol
w
muaons
levels,
wereas
ave
amlal
a
wo-
o
omozygoes
ypercoleserolema
ree-old
may
ave
elevaon
n
excess
o
o
a
ve-old elevaon. Aloug er coleserol levels are elevaed rom br,
eerozygoes
coleserol
reman
deposs
aeroscleross
more
severely
asympomac
(xanomas)
resulng
afeced,
n
unl
along
coronary
developng
adul
endon
arery
le,
wen
seas
dsease.
cuaneous
ey
and
develop
premaure
Homozygoes
xanomas
n
are
cldood
and oten dyng o myocardal narcon beore e age o 20 years.
Recognon o e crcal role o LDL recepors n coleserol omeo-
sass led o e desgn o e san amly o drugs a s now wdely used
o lower plasma coleserol. ey nb e acvy o HMG-CoA reduc-
ase,
ncreasng
Smlarly,
PCSK9
e
level
recognon
uncon
led
o
a
o
LDL
recepors
paogenc
e
on
epaocyes
PCSK9
developmen
o
muaons
PCSK9
(see
cause
nbors,
Fg.
6.1).
ncreased
wc
also
are now approved or reamen o ypercoleserolema.
Fig.
6.1
normal
with
of
Low-density
individuals
normal
levels
low-density
(IDL)
bearing
uptake
Apo
B-100
(LDL)
(left),
and
delivers
cholesterol
metabolism
In
intermediate-density
the
cholesterol
bearing
to
is
packaged
Apo
B-100
step
for
and
clearance
lipoproteins
hepatocytes,
rate-limiting
in
in
Cystic
Fibrosis
Cystic
brosis
individuals
receptor-mediated
cholesterol
reductase,
(VLDL)
and
hypercholesterolemia.
receptors
hepatocyte
lipoproteins
(LDL)
familial
LDL
HMG-CoA
Some
low-density
of
in
lipoproteins
inhibits
synthesis.
lipoprotein
and
where
its
cholesterol
export
into
Apo
proteins.
E
transport
exocrine
and
that
of
VLDL
by
lipoprotein
lipase
in
capillaries
releases
glands
are
then
stored
in
fat
cells
and
used
as
a
source
of
and
autosomal
to
recessive
secretion
the
linings
of
of
disorder
abnormally
the
of
epithelial
viscid
respiratory,
mucus
ion
from
gastrointestinal,
tracts.
very
Cysc
bross
(CF)
s
e
mos
common
le-sorenng
triglycerides,
genec which
an
reproductive
Pathogeness. Lipolysis
is
leads
energy
in
dsease
n
Caucasan
populaons,
w
an
ncdence
o
skel-
approxmaely 1 n 2500 brs. I s caused by muaons n an epelal on etal
muscle.
Lipolysis
converts
VLDL
into
IDL
and
some
LDL,
completing
cannel the
cycle.
In
individuals
with
familial
hypercholesterolemia,
a
deficiency
proen
(CFTR) dysfunction
and
els
of
increased
of
blood
B-100
tional
LDL
receptors
cholesterol
LDL
prevent
(the
LDL
deficiency
of
“bad”
and
LDL
leads
to
synthesis,
IDL
form
of
binding
receptors,
decreased
which
cholesterol).
to
the
LDL
thereby
LDL
together
and
IDL
produce
Mutations
receptors,
causing
encoded
by
e CF
transmembrane
conductance
reguator
or
gene
locaed
a
cromosome
7q31.2.
Penoypes
vary
wdely
clearance
elevated
affecting
creating
a
lev-
Apo
func-
hypercholesterolemia.
dependng
on
e
underlyng
causave
muaons.
e
mos
common
CFTR muaon s a deleon o ree nucleodes codng or penylalanne
a
amno
leadng
acd
o
s
poson
508
degradaon
(ΔF508)
and
loss
o
a
causes
uncon.
msoldng
e
small
o
CFTR,
amoun
o
e
muaed ΔF508 proen a reaces e cell surace also s dysunconal. up
by
a
scavenger
recepor
or
oxdzed
LDL.
Aoug
LDL
recepors
are Muaons
wdey
dsrbued,
approxmaey
75%
are
ocaed
on
epaocyes,
so
meable ver
as
a
cenra
roe
n
LDL
meabosm.
e
paway
nvolves
LDL
o
e
LDL
recepor,
endocyoss,
and
enzymac
degradaon
LDL
parcle
wn
lysosomes,
releasng
e
coleserol
load.
e
no
only
s
used
or
membrane
syness,
bu
also
conrols
omeosass
roug
a
sopscaed
eedback
conrol
o
sysem
suppresses
coleserol
syness
by
nbng
e
acvy
o
e
epelal
6.2);
membranes
owever,
e
relavely
consequences
mper-
are
ssue-specc.
In
swea
ducs,
e
major
uncon
o
o
s
CFTR
reabsorb
lumnal
ereore,
loss
o
clorde
CFTR
ons
and
uncon
augmen
leads
o
sodum
decreased
reabsorp-
reabsorpon
sodum
clorde
and
producon
o
yperonc
(“saly”)
swea
(see
a Fg.
(1)
(Fg.
coo
leserol
render
ons
ree on.
coleserol
CFTR
clorde
o s
e
o
bndng deec
o
n
e
6.2,
top).
In
conras
o
swea
glands,
n
respraory
and
nesnal
enzyme epelum,
CFTR
s
mporan
or
lumnal
secreon
o
clorde,
and
3-ydroxy-3-meylgluaryl–coenzyme A reducase (HMG-CoA reductase), as
a
resul
o
CFTR
muaons
reduce
clorde
secreon
no
e
lumen
92
CHAPTER
Genetic
6
Diseases
NORMAL
LUMEN
OF
CYSTIC
SWEA T
DUCT
LUMEN
FIBROSIS
OF
SWEA T
DUCT
+
Cl
Na +
Cl
CFTR
Na
ENaC
NORMAL
CYSTIC
FIBROSIS
AIRWA Y
AIRWA Y
Nor mal
Dehydrated
mucus
mucus
+
Cl
Fig.
6.2
and
sodium
epithelial
6.2,
bottom).
s
In
Cl
O
2
cystic
sodium
cells,
and
defective
regulator;
causes
in
water
(CF),
H
a
channel
Bottom,
reabsorption
mucociliary
in
airways,
and
sodium
sodum
defect
Patients
the
action,
epithelial
lumnal
Cl
O
2
chloride
sweat.
ENaC,
ncreased
+
Na
fibrosis
concentration
conductance
Fg.
H
Top,
increased
(see
+
Na
with
the
CF
leading
mucous
channel
in
sweat
have
to
plugging.
CFTR,
for
epelal
clorde
drves
sodum
waer
cannels.
Increased
reabsorpon
rom
e
nracellular
lumen,
sodum
o
mucus
coang
e
underlyng
epelal
cells.
deydrang
In
leads
o
deecve
mucoclary
acon
and
e
of
the
Cystic
increased
chloride
Na
H
O
2
chloride
secretion
mucous
fibrosis
intracellular
e
lungs,
bronc s
layer
and
coating
transmembrane
sodium
and
abs cess es
s
conduction.
bronce c ass.
D e vel opmen
o
lung
common .
Pancreatc
abnormates
e are
presen
n
85%
o
90%
o
paens.
In
s severe
deydraon
causes
Cl
O
2
and
• layer
H
absorpon cronc
roug
duct
decreased
dehydration
responsible
+
Na
cases,
e
pancreac
ducs
are
obsruced
by
mucous
plugs,
accumulaon causng aropy o e exocrne glands and progressve bross (Fg.
o
vscd
secreons
a
obsruc
ar
passages
and
predspose
o
recur6.4).
ren
pulmonary
necons.
Vscd
secreons
also
may
obsruc
e
on, ac
ducs
and
e
vas
deerens,
leadng
o
pancreac
loss
o
pancreac
exocrne
secreon
mpars
a
absorp-
pancre-
nsuicency
leadng
o
vamn
A
decency,
wc
may
conrbue
o
and squamous meaplasa o e pancreac duc epelum.
mae nery, respecvey. In addon, CFTR reguaes e ranspor o
• bcarbonae
ons
n
e
epea
ces
o
e
exocrne
pancreas,
and
Meconum
small dysuncon
causes
e
acdcaon
o
pancreac
secreons.
s
precpaon
o
mucn
and
mpars
e
acvy
o
dgesve
as
rypsn
a
uncon
bes
under
alkalne
a
o
ype
o
nans
bowel
obsrucon,
because
o
e
may
presence
occur
o
n
ck
e
plugs
mucus.
enzymes
• suc
nesne
resuls o
n
eus,
s
condons,
bo
Lver nvovement may lead o mucus pluggng o ble canalcul,
o accompaned by ducular proleraon and pora nammaon.
wc
exacerbae
pancreac
nsuicency. Hepac
seaoss
resung
n
nvovemen Morphology.
Lesons
var y
n
dsrbuon
and
severy
s
epac
encounered
Over
me,
crross
noduary.
n
ewer
Suc
an
10%
may
deveop,
severe
o
epac
paens.
Azoosperma
and
nfertty
are
ound
n
95%
o
e
afeced
genoype. maes
•
common.
dependng
• on
s
dfuse
P umonar y
d s eas e
semmng
rom
ob s r uc on
and
e
ar
p ass ages
broncoles
w
o en
marke d
cre ng
cel ls.
s
are
e
mos
s er ous
d send e d
yp er pl as a
and
Sup e r mp os e d
w
e aure
ck
yp er ropy
ne c ons
(Fg .
muc us
o
g ve
e
r s e
sur vve
o
aduood;
baera
absence
of
e
vas
def-
ne c on erens
o
wo
6.3).
s
a
requen
indng.
Te
ass o c ae d
muc us -s e-
o
s e vere
Clncal
and
Features.
sympoms
e
vary
clncal
rom
mld
manesaons
o
severe,
may
o
CF
are
presen
a
proean.
br
or
Sgns
years
CHAPTER
Fig.
are
6.4
Pathologic
dilated
glands
and
are
Enzyme
changes
plugged
atrophic
Diseases
Genetic
6
and
Caused
of
with
cystic
fibrosis
eosinophilic
replaced
by
Diseases
by
fibrous
Mutations
in
the
mucin,
in
93
pancreas.
and
the
The
ducts
parenchymal
tissue.
Genes
Encoding
Proteins
Phenylketonuria
Fig.
6.3
Lungs
of
a
patient
who
died
of
cystic
fibrosis.
Extensive
Phenylketonuria mucous
plugging
and
dilation
of
the
tracheobronchial
tree
are
phenylalanine The
pulmonary
secretions
parenchyma
and
pneumonia;
is
consolidated
the
greenish
by
a
combination
discoloration
is
of
the
Pseudomonas
of
infection.
Pittsburgh,
(Courtesy
of
Dr.
Eduardo
Yunis,
by
mutations
that
disable
the
enzyme
both
Penylkeonura
(PKU)
s
an
nborn
error
o
meabolsm
Children’s
a Hospital
caused
hydroxylase.
product
Pathogeness. of
is
apparent.
afecs
1
n
10,000
lve-born
Caucasan
nans.
e
mos
common
PA.)
(classc)
orm
s
relavely
common
n
persons
o
Scandnavan
descen
and uncommon n Jews populaons and n persons o Arcan descen. aer,
and
may
be
reaed
o
e
nvovemen
o
one
o
aenon
organ
or
many. s
Approxmaey
5%
o
10%
o
e
cases
come
a
br
o soon
ater
because
o
meconum
leus
Exocrne
pancreac
auosomal
penyaanne
n
a
majory
(85%
o
90%)
o
paens
w
CF
dsorder
ydroxyase
s
(PAH),
caused
wc
by
a
blocks
severe
e
decency
converson
o
nsuicency penylalanne
occurs
recessve
or
and
s
o
yrosne
and
leads
o
yperpenylalannema.
Afeced
assocaed nans are normal a br bu wn a ew weeks exb a rsng plasma
w
nerance
o
wo
“severe”
CFTR
muaons
(e.g.,
ΔF508/ΔF508), penylalanne level, wc mpars bran developmen. As penylalanne
wereas paens carryng a eas one “md” CFTR muaon oten rean levels pancreac
exocrne
uncon.
Pancreac
nsuicency
s
assocaed
rse,
yeldng maabsorpon
o
proen
and
a.
e
auly
a
absorpon
may
normally
mnor
meabolc
paways
become
more
acve,
w nermedaes
a
are
excreed
n
large
amouns
n
e
urne
nduce and
n
e
swea,
mparng
a
srong
musy
or
“mousy”
odor
o
afeced
decency saes o e a-soluble vamns A, D, and K. Hypoproenema nans. may
be
severe
enoug
o
cause
generalzed
edema.
Perssen
o resuls
n
e
oer
recal
prolapse
gasronesna
demonsrae
exceen
Cardorespraor y
ons,
obsrucve
common
Saes).
w
n
as
pancreas-suicen
cause
By
18
o
suc
Sgncan
sadowed
sur vval,
by
grow
as
and,
dsease,
s
paens
dsease
and
now
n
suc
and
s
w
no
ese
w
paens
perssen
o
severe
aaes
CF
oten
aerugnosa
lae
pancreac
rd
n
e
and
ung
are
n
mos
Uned
colonzed
Burkodera
and
w
common
nec-
e
e
are
course
nvolvemen;
mos
Clncal
menal
o
pumonae,
yrosne,
paens
w
CF
(ater
cardopulmonar y
and
s
ore-
mproved
cause
o
Features.
I
unreaed,
dsably
ese
swea
elecrolye
s
usually
suspeced
concenraons,
based
caracersc
on
or
neurologc
eczema
never
also
seen.
nake
mmedaely
adulood;
walk
abnormales,
are
penylalanne
PKU
(nellgence
cldren
s
melann
due
o
e
deecve
syness
syness.
owever,
and
6
mons
wo
decreased
ese
early
ater
by
quoen
rds
n
le;
le
an
PKU
60).
canno
can
ereore,
Deary
o
o
pgmenaon
complcaons
br.
women
less
age
rd
Sezures,
oer
ar
s
severe
one
and
avoded
nans
reamen
cldbearng
alk.
o
be
produces
Abou
are
skn,
by
screened
dsconnued
wo
ave
and
lmng
PKU
or
ater
mus
go
on a low penylalanne de pror o concepon because o e eraogenc
efecs o penylalanne and s meaboles on e eus.
Storage
Diseases
ransplan-relaed
Lysosomal
dagnoss
coloraon
requred
dea
complcaons).
e
pale
s
Lysosomal n
nans’
wc
CF .
assocaed
genera,
as
cor
80%
w
occurs
e
cldren
deveopmen.
Pseudomonas
lver
dsease
and
o
usuay
(approxmaey
age,
pulmonar y
lver
10%
compcaons,
dea
o
as
compcaons
pumonar y
years
paogens
cepaca.
many
penoype
Afeced
darrea
perssenly
clncal
elevaed
ndngs
(pulmo-
ciencies
olites
of
and
storage
enzymes
certain
diseases
stem
required
from
for the
mutations
degradation
that
of
lead
various
to
de
metab-
organelles.
nary dsease and gasronesnal manesaons), and amly sory, and
s
esablsed
pancreac
by
sequencng
enzyme
e
replacemen
CFTR
gene.
erapy,
as
e
well
use
as
o
anbocs
blaeral
lung
and
rans-
Pathogeness.
number
o
planaon, as mproved oucomes n paens w severe CF . New drug
complex
erapes
derved
rom
may
aken
also
expresson,
ave
and
exended
dsease
o
are
now
avalable
uncon
e
o
medan
cldood
no
a
a
muaed
le
mprove
CFTR
expecancy
cronc
dsease
e
oldng,
molecules.
o
o
40
years,
aduls.
membrane
ese
advances
cangng
a
leal
be
Lysosomes,
ydrolyc
subsraes
no
soluble
nracellular
up
no
e
enzymes
e
dgesve
a
end
are
producs.
organelles
cell
by
sysem
nvolved
a
are
o
n
cells,
e
ese
subsraes
undergong
pagocyoss.
I
an
conan
breakdown
may
auopag y
enzyme
a
o
be
or
requred
or e caabolsm o a subsrae s mssng, parally degraded nsoluble
meaboles
accumulae
wn
e
lysosomes
(Fg.
6.5).
In
addon,
94
CHAPTER
Genetic
6
Complex
Diseases
T ay-Sachs
substrate
ndase
Dsease
Tay-Sachs
by Normal
lysosomal
Lysosomal
(G
Ganglosdoss:
M2
Deicency
n
Hexosam
A)
loss
of
disease,
the
function
most
common
mutations
gangliosidosis,
affecting
expression
of
is
caused
the
enzyme
enzyme
hexosaminidase A. degradation
deficiency
Pathogeness.
A
In
Tay-Sacs
dsease,
glycolpds
called
gangosdes
A
accumulae
and
glal
njur y
and
n
many
cells
s
no
s
ssues,
rougou
e
undersood.
may
nduce
e
bu
In
damage
CNS.
many
s
e
conned
molecular
cases
unolded
mosly
e
proen
bass
muan
o
neurons
or
neuronal
proen
msolds,
response
(see
Caper
1),
Small B
B
wc
can
lead
o
apopoc
cell
dea.
diffusible
end
products
Morphology.
Elecron
Afeced
mcroscopy
cells
appear
reveals
swollen
worled,
and
onon
somemes
skn–lke
oamy.
layers
o
C
membranes
rougou
swollen
ganglon
nonmetabolized
STORAGE
nans
red”
rena
spo
o
wn of
autophagosome
with
2
or
degradation
and
unafeced
bu
pallor
resuls
cenral
varan
moor
canges
are
auonomc
e
rena
common
br,
ese
were
perperal
mos
a
nerves,
nvolved,
relavely
e
of
intracellular
by
severe
years.
neurologc
neurologc
Tay-Sacs
Askenaz
carrers
o
n
ound
nervous
produced
a
by
conrasng
macula.
Tay-Sacs
weakness
begns
dsease,
a
mparmen,
3
o
blndness,
6
dysuncons.
dsease,
lke
oer
Dea
lpdoses,
and
occurs
s
s
Jews,
esmaed
among
o
be
1
wom
n
e
mos
requency
o
30.
organelles
Niemann-Pick
tion
Accumulation of
e
ollowed
among
Type A and
Disease
type
mutations
B
Types
A
and
Niemann-Pick
that
affect
the
B
disease
enzyme
is
acid
caused
by
loss
of
func-
sphingomyelinase.
SECONDARY of
toxic
In
more
3
eerozygous
Accumulation
n
s
6.6).
lysosome
common
Defective
perperal
e
normal
age,
progressvely
fusion
n
(Fg.
products
mons
Defective
lysosomes
usually
cells
Features.
appear
e
CNS,
e
Clncal
Stored
e
sysem.
“cerry
PRIMARY
wn
proteins
aberrant
STORAGE mitochondria
Pathogeness.
myenase,
breakdown
Induction
of
Generation CELL
cell
e
more
o
damage
free
Pathogenesis
of
s
ype
spngomyeln
caused
A
no
an
by
n
a
decency
ype
ceramde
B,
and
resulng
o
spngo-
n
mpared
posporylcolne.
of
radicals
pagocyes 6.5
n
DEATH
Morphology.
Fig.
dsease
severe
lysosomal
storage
diseases.
In
this
In
and
ype
A,
neurons.
excess
e
spngomyeln
macropages
accumulaes
become
sufed
n
w
example,
droples or parcles o e complex lpd, mparng a ne vacuolaon a
complex
enzymes
or
substrate
(A,
B,
malfunction
and
insoluble
this
primary
from
as
of
dysuncon
naure
o
Ceran
the
o
e
of
nereres
wc
are
and
common
in
B),
the
and
cearance
leads
o
o
a
deficiency
of
based
mos
dseases
Hepatospenomegay,
In
addition
accumulaon
o
on
e
eFg.
6.1).
Wen
to
result
n
s
(Table
group:
parally
dgesed
pagocyes
dysfuncton,
maeral
bu
caused
also
by
a
no
only
cascade
o
by
accumulaon
secondar y
evens
o
und-
rggered, Fig.
by
macropage
acvaon
and
release
o
6.6
lysosome
sorage
dsorders
are
ver y
rare;
only
a
ew
o
the
are
consdered
cells
electron
in
Tay-Sachs
microscope
disease.
shows
A
portion
prominent
of
a
neuron
lysosomes
with
e whorled
condons
Ganglion
cyoknes under
common
(Supplemenal
bocem-
meaboles
Ceuar
more
cyoplasm
radcas.
Frequent CNS nvovement w assocaed neuronal damage
Mos
e
organees
ree
•
example,
o
dysfunctional
•
or
oamness
dea.
accumulaed
Onset of dsease n nfancy or eary cdood
gesed
or
incomplete,
deecve
cell
•
o
lysosomal
effects
desrucve
Autosoma recessve transmsson
due
is
toxic
accumulation
•
n
is
lysosomes.
•
meaboles
there
of
catabolism
subdvded
o
If
series
wastes.
generae
e
a
storage
the
w
may
dsorders
are
to
toxic
ulmaely
subsraes
eaures
(e.g.,
secondary
leading
by
products.
accumulate
deecs
sorage
end
enzymes
defect,
mocondra,
degraded
soluble
accumulation
combnaon
6.3).
into
autophagy,
and
Lysosomal
cal
one
normally
intermediates
defective
suc
s
of
C)
storage
mitochondria
ysosome
and
is
configurations.
Part
of
the
nucleus
is
shown
above.
(Courtesy
ere. Dr.
Joe
Rutledge,
Children’s
Regional
Medical
Center,
Seattle.)
CHAPTER
Table
6.3
Selected
Lysosomal
Disease
Storage
Deficient
Tay-Sachs
Gaucher
disease
disease
Enzyme
Genetic
6
Diseases
95
Disorders
or
Protein
Accumulating
Metabolite(s)
Hexosaminidase
GM2
Glucocerebrosidase
Glucocerebroside
Clinical
ganglioside
Features
CNS
disease
Mild
forms:
organomegaly,
bone
marrow
failure
Severe
Niemann-Pick
types
A
disease,
and
Sphingomyelinase
Sphingomyelin
Type
B
forms:
A:
B:
CNS
type
MPS
disease,
NPC1
C
or
lipid
Type
I
(Hurler
NPC2;
part
transport
of
a
Cholesterol,
gangliosides
Type
II
α-L-Iduronidase
Heparin
and
dermatan
sulfate
L-iduronate
sulfatase
Heparin
and
dermatan
sulfate
by
e
2,
a
Lysosomal
mcroscopy,
oten
o
enlargemen
glucosidase
bone
may
e
marrow,
be
vacuoes
myeln
mos
lymp
srkng.
are
membranous
lamellaed
pagocyes,
lver,
e
conan
concenrc
conen
spleen,
variable
including
ataxia,
organomegaly
cardiovascular
disease,
disease
Similar
to
Hurler
syndrome,
but
milder
(acid
Glycogen
Cardiac
failure
maltase)
eecron
resemblng
g
type
disease
ysosomes
late-onset
phenotype
Glycogenosis
vewed
organomegaly,
symptoms,
Organomegaly,
CNS
(Hunter
early-onset
dementia;
syndrome)
Pompe
disease,
disease
Neurologic
complex
syndrome)
MPS
disease
CNS
organomegaly
Type
Niemann-Pick
CNS
early-onset
engorged
gures.
severely
nodes,
Neurons
secondary
cyoplasmc
Because
afeced
and
lungs.
rougou
bodes
o
er
organs
e
e
are
splenc
CNS
Morphology.
so-called
Pagocyes
Gaucer
sufed
ces—become
w
markedly
glucocerebrosde—
enlarged
and
acqure
a
paognomonc cyoplasmc appearance caracerzed as “wrnkled
ssue
paper”
marrow
may
(Fg.
be
6.7).
largely
Splenomegaly
replaced
by
may
sees
o
be
massve,
Gaucer
and
e
cells.
also
accumulae spngomyeln, wc resuls n neuronal enlargemen and
vacuolzaon.
Type
B
s
assocaed
w
less
severe
spngomyelnase Clncal Features. One varan, ype 1, accouns or 99% o cases o Gaucer
decency and e manesaons are mlder. dsease.
I
absence
Clncal
Features.
organomegaly
occurs
ype
B
wn
and
e
varan
Type
rs
ave
A
severe
3
presens
neurologc
years
o
le.
organomegaly
In
bu
n
nancy
w
deeroraon
comparson,
no
neurologc
massve
Dea
paens
usually
w
e
Jews
and
s
Type
port,
C
Disease
Niemann-Pick
leading
to
lipid
Nemann-Pck
genes,
NPC1
and
Type
NPC2,
ype
is
wc
C
bone
compable
w
lesons,
Type
long
1
le.
s
epaosplenomegaly,
mos
Types
2
common
and
3
are
n
and
e
Askenaz
caracerzed
by
or laer n le (ype 3). Aloug e lver and spleen also are nvolved, e
convulsons
and
progressve
menal
deeroraon.
O
neres,
eerozygous carrers o Gaucer dsease are a ncreased rsk o Parknson
caused
accumulation
dsease
w
nvolvemen.
clncal eaures n ypes 2 and 3 are domnaed by neurologc dsurbances,
manesaons.
C
disease
assocaed
CNS
neurologc sgns and sympoms, wc may appear durng nancy (ype 2)
ncludng
Niemann-Pick
s
o
in
resuls
encode
by
defects
in
lipid
trans-
dsease, or reasons a are unceran.
relaed
sdes
Curren
cells.
rom
muaons
proens
a
orm
n
a
wo
complex
a
a
by
erapy
nuson
nb
s
o
amed
a
reducng
recombnan
glucocerebrosde
e
burden
o
glucocerebrosdase
glucocerebro-
and
w
drugs
synase.
s nvolved n nracellular raickng o coesero and oer pds. Deec-
ve
pd
ranspor
and
gangosdes
resus
suc
as
n
e
GM1
nraceuar
and
GM2.
accumuaon
Afeced
cldren
o
coesero
exb
aaxa,
Mucopolysaccharidoses
Mucopolysaccharidoses
tion
vsual dsurbances, dysona, dysarra, and psycomoor regresson.
and
ious
Gaucher
rebrosidase
phagocytes
that
and
is
caused
result
more
in
by
the
loss
of
function
accumulation
variable
mutations
of
in
glucoce-
glucocerebrosides
accumulations
in
in
Gaucer
varable
dsease
expressvy
Gucocerebrosdase
ssue
s
due
normally
an
o
cleaves
auosomal
muaons
a
glucose
o
recessve
dsorder
dferng
severy.
resdue
rom
enzymac
deecve,
degrada-
in
var-
coronar y
normally
e
removed
s
rom
macropages
glucocerebrosde
derved
and
e
are
rom
senescen
crculaon
acvaed
release
a
by
cells,
macropages
wle
number
red
o
aempng
cyoknes.
wc
n
o
ese
dges
ese
are
common
causes
cloudng
lesons,
w
and
varable
degrees
occasonally
o
oseopena,
oseonecross.
oseopoross,
and
o
e
wn
Morpholog c
are
syneszed
exracellular
lysosomes.
manly
I
any
eparan
o
o
all
excreon
o
o
and
lesons
e
by
marx.
o
ese
sulae
connecve
T urnover
enzymes
and
or
are
dermaan
Mos
n
Hepaosplenomegaly,
deposs
ear
valves
(parcularly
and
mucopolysaccardoses
oten
and
cases
cornea,
areral
lesons
e
narcon
dea
o
Features.
subendoelal
areres),
myocardal
o
dsease
par
degradaon
subendoelal
suspeced o alerng bone meabolsm and may explan e assocaon
Gaucer
are
sulae, accumulae wn e lysosomes o pagocyes and oer cells.
o
oseolyc
defective
ceramde.
deormes,
glucocerebrosde
and
mucopolysaccardes,
Clncal
e
by
mucopolysaccharides
remodelng o mucopolysaccarde s medaed by upake no pagocyes
neurons.
parcularly n e spleen, lver, and bone marrow. s s because muc
ssues.
of
Mucopolysaccardes
broblass
Is dec leads o an accumulaon o glucocerebrosde n macropages,
are
characterized
tissues.
Pathogeness.
and
Pathogeness.
e
are
accumulation
Disease
Gaucher disease
w
excessive
lead
cardac
are
jon
o
myocardal
assocaed
and
oten
s
w
coarse
menal
e
(MPSs).
decompensaon
sfness,
mucopolysaccardes
n
n
bran
scema,
are
e
are
Coronar y
and
mporan
acal
dsably
ncreased.
skeleal
eaures,
Urnar y
CHAPTER
Supplemental
cytes
from
Basic
Dr.
and
eFig.
Kupffer
deposition
Pathology,
Arthur
6.1
cells
of
lipids.
10th
ed.,
Weinberg,
Southwestern
Medical
Niemann-Pick
have
a
foamy,
(From
St.
Kumar
Louis,
Department
Center,
disease
vacuolated
V,
Abbas
Elsevier,
of
Dallas.)
in
A,
2018,
Pathology,
liver.
The
appearance
Aster
Fig.
J:
7.10;
University
hepato-
resulting
Robbins
Courtesy
of
Texas
6
Genetic
Diseases
95.e1
96
CHAPTER
Genetic
6
Diseases
A
B
Fig.
6.7
Gaucher
cytoplasm.
thew
Severa
cency
mer
•
o
cnca
a
bre
o
exs,
Only
wo
involving
micrograph
Department
MPS
enzyme.
disease
Electron
of
the
of
Pathology,
eac
resung
bone
marrow.
Gaucher
cells
University
rom
well-caracerzed
e
of
(A)
with
Gaucher
elongated
Texas
Southwestern
de-
o
mus cle
sve
o
due
n
o
ave
a
cardac
o
e
swol len
o
rons
accouns
MPS
engorge d,
type
s
cloudng.
Unlke
nae
e
II,
mode
I
or
or
o
also
lae
because
requres
e
Hunter
oten
as
(a
o
e
s
n
acc umu lae
smo o
afe c e d
rom
oten
e
cel ls
are
n
rom
and
e
rom
an
mlder
a
•
a
Pompe
neu-
cogen
o
α-L-durondase).
sulae
subsraes
and
course.
The
various
ciencies
in
Storage
of
glycogen
enzymes
excessive
glycogen
Diseases
in
storage
accumulation
of
n
blo o d
d s eas e
mus cle
mus cl e
l ac ae
( yp e
c ramps
and
le vels
V
we a k ness
or ms
o
a er
a lure
exerc s e,
o
b e c aus e
s
e
exerc s e
o
g lycogenos s ) ,
pospor y l as e,
due
g lyc ogen
a
bl o ck
resu l ng
proo yp e
o
(ype
II
e
s
glycogenoss)
(acd
rougou
mos
afeced
promnen,
owng
enzyme
o
can
s
malase),
e
cell
and
caused
wc
body
ype
mos
s
cardac
paens
cardac
a
decenc y
o
requred
(Supplemenal
e
cardorespraor y
reverse
by
s
de
muscle
gly-
eFg.
6.2).
myoc ye.
Car-
wn
alure.
or
2
years
erapy
damage
w
and
o
e
ncrease
dermaan
sulae
COMPLEX
MULTIGENIC
DISORDERS
enzymes.
diseases
in
are
caused
glycogen
glycogen
multiple
or
by
inherited
metabolism
some
and
abnormal
de
result
form
of
multigenic
gene
Genec
allele
sorage
dseases,
e
specc
enzyme
disorders
variants
varans
requency
n
are
e
and
are
caused
by
environmental
reerred
o
populaon
o
as
a
interactions
polymorpsms
leas
between
factors.
1%.
ey
Accordng
o
ave
e
an
com-
mon dsease–common varan ypoess, complex mulgenc dsorders
occur
glycogen
by
and
Myop a c
myog lob nur a,
mus cle
glucosdase
onse
wen
penerance,
In
mus cles
Despe
tissues.
Pathogeness.
n
accumu-
(Glycogenoses)
involved
o
Mat-
Dallas.)
longevy.
Complex
Glycogen
o
granular
Dr.
g lycogenos es .
breakdown
mssng
(Courtesy
marke d
McArde
dsease
dsease
L-duro-
are
le adng
de cenc y
domegaly
corneal
lipid-laden
pro duc on .
ele va on
g lycolyss.
lysosomal
syndrome
o
clncal
decency
dencal
eparan
Hurler
absence
an
myop a c
acc umu la-
g lycogen
ds e as es
nduce
rom
mus cle
o
Center,
energ y
njur y
However,
prolonged,
enzyme
o
de a
Acc umu la on
dfers
resuls
bo
and
cel ls.
lys os omes.
decency,
breakdown
uncon
and
Afe c e d
ds ab ly.
more
ye ars,
resu l ng
(X-lnked)
a
dferen
enzyme
10
o er
syndrome,
syndrome,
dferen
and
men a l
o
α-L-durondas e.
endo elum
vac uolae d
e
6
c yoplasm,
nerance
Hurler
sulaase
wa l l,
cle ar
o
o
Mucop olys accar des
broblass,
ave
on
decenc y
exp e c anc y
vas c u lar
and
a
complca ons.
macropages,
cel ls
n
le
by
abundant
lysosomes.
Medical
mp are d
sorage
caus e d
with
acc umu l a on
syndromes
dscusson.
ds order
cells
distended
M PS ty pe I, a ls o k nown as Hurer sy ndrome, s an auos oma l re ces-
c ldren
•
Fries,
varans
dferen
(B)
n
s
several
are
group,
polymorpsms,
conered.
ncludng
eac
auommune
and
allergc
e
cyoplasm
glycogenoses
and
are
somemes
nered
Approxmaely
a
as
dozen
Glycogen
wn
e
auosomal
may
nucle
o
recessve
glycogenoses
ave
accumulae
afeced
wn
cells.
Mos
been
mulgenc
•
dseases.
descrbed.
On
e
dsorders,
Aloug
o
several
complex
several
oer
dsorders
polymorpsms,
dseases,
ceran
oten
sould
rom
e
be
no
low
o
all
dabees,
kep
collecve
polymorpsms
n
mnd:
nerance
may
enzymes
lver
nvolved
o
resulng
(Fg.
rom
epac
Myopatc
ae d
n
type.
a
glycogen
6.8).
o
o
and
lack
orm
mus cle.
enzy mes
a
syneszes
o
caused
meabolsm
accumulaon
ypoglycema
Von
Gerke
and
by
ave
o
due
dsease
also
deecs
wo
a
or
alure
(ype
s
I
breaks
n
epac
major
normal
o
glucose-6-pospaase,
efecs:
abnormal
o
mos
Glycogen
s
an
re qu re d
or
50%
ave
ds e as es
g lycogen
energ y
c aus e d
s ource
by
•
mpor-
bre a kdow n
n
e
same
Many
l e ad
o
n
e
ype
genec
uaor y
s r -
d ee c s
o
e
20
o
a
30
rsk.
(e.g.,
auommune
dsorders),
wereas
oers
are
dsease-specic.
cange
•
varans
regons
quanave
mp or an
sorage
an
n
S ome poymorpsms are assocaed w mupe dseases, usuay
o
glucose
glycogenoss),
e
more
•
glycogenoss.
Glyco gen
are
glycogen
Glycogenoses
due
glycogen,
producon
•
lver
glucose.
enlargemen
orms
an
e
ree
varans
o
genes are mpcaed n ype 1 dabees, a ew HLA aees conrbue
type.
aoug
possble
•
no
exampe,
s
and
domnan
down
For
prncples
resul
efec
oug
bass o paopysologc ndngs, ey all no ree groups (T able 6.4):
Hepatc
nuence.
bu
are
pnpon a specc causave polymorpsm. Wen consderng complex
dsrbuon.
dsease,
modes
yperenson,
ssue
ear
a
dseases
locaon,
s
scemc
w
common
decency dcaes e ype o glycogen a accumulaes, s nracellular
and
and
Many
n
e
e
nked
n
encoded
acors
mugenc
o
genome
varaon
Envronmena
compex
o
dsease
and
gene
us
a
are
expresson,
n
e
key
raer
noncodng
assocaed
an
a
reg-
w
a
srucura
proen.
pay
a
sgnican
dsorders.
Type
2
roe
n
dabees
e
s
an
expresson
exampe
o
o
a
CHAPTER
Table
6.4
Subgroups
Clinicopathologic
of
Genetic
6
Diseases
97
Glycogenoses
Category
Specific
Hepatic
von
Type
Gierke
Myopathic
McArdle
Miscellaneous
Pompe
Enzyme
Deficiency
Organs
disease
(type
I)
Glucose-6-phosphatase
syndrome
(type
V)
Muscle
disease
(type
II)
Liver,
phosphorylase
Lysosomal
Skeletal
glucosidase
numb er
a
Affected
kidney
s
(acid
no
maltase)
an
exac
Cardiac
mu l ple
muscle
and
o
n
skeletal
s
muscle,
c a l le d
liver
aneupod.
Te
omologous
p ar
NORMAL Liver
ce
o
c aus e
o
aneuplody
cromos omes
croma ds
o
a
e
s ep arae
s
nondsjunc on
rs
meo c
dur ng
e
o
dv son
s e cond
a
or
a
meo c
a lure
o
dv son.
sser
Te
l a-
Glycogen
er
Various
Glucose
a ls o
may
pro duc on
tissues
o cc ur
o
wo
cromos omes
dur ng
moss
aneuplod
ol lowe d
by
cel ls.
n
s oma c
Fa lure
random
o
cel ls,
le adng
p ar ng
ass or men
o
o
e
omologous
(anapas e
l ag)
a ls o
Blood
c an
le ad
o
aneuplody.
Wen
nondsjunc on
o cc urs
a
e
me
o
glucose
meoss,
1)
or
e
one
gamees
less
or me d
cromos ome
ave
(n
−
e er
1).
an
ex ra
Fer lza on
cromos ome
o
suc
(n
gamees
+
by
Glycolysis
Glucose
nor ma l
gamees
may
resu l
n
wo
yp es
o
zygoes,
r s omc,
w
Muscle Energy
an
ex ra
cromos ome
(2n
+
1),
or
monos omc
(2n
−
1).
Monos omy
Glycogen
nvolv ng
an
r s omes
o
auos ome
cer an
cromos omes
GLYCOGEN
STORAGE
DISEASE—HEPATIC
o
TYPE
des cr b e
d eren
yp e
o
are
e
s
comp a ble
pres ence
complemens
mos acsm
embr yogeness,
a a l
s
dur ng
auos omes
o
o
and
w
wo
e a l
a
le.
or
c aus e d
resu l ng
by
n
mo c
e
Mos ac sm
more
cromos omes
de velopmen,
monos omy
s
a
p opu l a ons
n
e
s ame
o
er m
o
cel ls
w
dur ng
r s omc
and
s ex
us e d
ndv du a l.
nondsjunc on
pro duc on
w ere as
nvolv ng
One
e arly
mono -
Glycogen
s omc
d aug er
Mos acsm
cel ls,
a e c ng
w os e
s ex
des cend ans
cromos omes
s
en
pro duce
common,
a
mos ac.
w ere as
auos o-
Glucose
ma l Low
blood
mos acsm
Structural
Srucural
somal GLYCOGEN
STORAGE
s
no.
glucose
DISEASE—MYOPATHIC
Abnormalities
canges
breakage
n
e
cromosomes
ollowed
by
loss
or
ypcally
resul
rearrangemen
o
rom
cromo-
maeral.
Suc
TYPE
canges
p
usually
denoes
e
are
desgnaed
sor
arm
o
a
usng
a
cyogenec
cromosome
and
q
sorand
e
long
n
wc
arm.
Eac
arm s en dvded no numbered regons (1, 2, 3, and so on) rom e
Glycolysis Glucose
cenromere ouward, and wn eac regon e bands are numercally Low
ordered.
energy Glycogen
e
output
are
•
Fig.
the
6.8
liver
ciency
The
Top,
and
of
A
simplified
skeletal
hepatic
scheme
muscles.
enzymes
consequences
of
a
of
normal
Middle,
involved
genetic
in
The
glycogen
effects
glycogen
deficiency
in
the
of
metabolism
an
inherited
metabolism.
enzymes
in
man
e
ypes
Transocaton
anoer
glycogen
in
skeletal
mples
mens
are
and,
ranslocaons
that
excanged
dsease
a
as
mporan
neracons
rsk
because
dsease
or
afeced
only
dabees
e
persons
oten
exb
clncal
long
arm
ater
weg
gan.
In
s
s
“unmasked”
by
caused
by
that
50%
of
rst-trimester
spontaneous
has
chromosome
a
o
Cyogenec
abnormalities
chromosome
dsorders
are
are
and
that
1
in
every
o
cromosome
recprocal
cromosomes).
by
order,
o
ndcaes
a
In
ollowed
or
(.e.,
genec
by
e
example,
recprocal
cromosome
5,
regon
excanged,
armul
cromosomes
durng
ormed,
fuson
occur
o
rag-
sor-
nvolved
46,X X,(2;5)
2
a
ranslocaon
regon
3,
band
1,
nvolv-
and
1,
band
4.
Wen
e
e
broken
o
e
e
resulng
carrer,
baanced
wo
as
recproca
e
and
e
ull
gameogeness,
complemen
abnormal
o
normal
genec
mae-
(unbalanced)
o
are
resulng
nvolvng
n
abnormal
wo
zygoes.
acrocenrc
A
specal
gam-
cromosomes
paern
type,
or
robertsonan,
transocaton.
e
s
called
breaks
close
o
e
cenromere,
afecng
e
sor
arms
o
yp-
bo
aberration.
dened
auosomes
or
by
e
sex
presence
o
numercal
Transer
o
e
segmens
leads
o
one
ver y
large
or and
one
exremely
small
one.
e
sor
ragmens
are
cromosomes. and
e
arms
afeced
o
all
ndvdual
acrocenrc
as
45
cromosomes.
cromosomes
carr y
Because
gly
e
redundan
Abnormalities
genes e
nor ma l
cromos ome
coun
s
46
(.e.,
2n
=
46).
(e.g.,
mu l ple
o
e
aplod
numb er
(n)
s
c a l le d
eupod.
rbosomal
RNA
genes),
suc
loss
s
compable
w
Any sur vval.
exac
one
200
sor
umans,
(q)
no
ranslocaon
los,
In
wo
ndcaed
numercal
evenly
s
cromosome aleraons
Numerical
are
cromosome
cromosomes.
srucural
o
usually
abortions
cally newborns
beween
noaon
arm
However,
centrc are
par
s
DISORDERS
o estimated
a
e
ees
is
o
process
obesy.
ral.
It
e
man-
nsance,
number
CYTOGENETIC
ranser
w
transocaton genec
n
s
ragmens o
6.9)
metabo-
sor acors,
(Fg.
muscles.
mugenc
esaons
abnormales
defi-
ng
oer
cromosomal
Bottom,
(q31;p14).
compex
srucural
cromosome.
cromosomes lize
o
ollowng:
Any
However,
dicues
agan
arse
durng
gameogeness,
CHAPTER
A
6
Genetic
Diseases
B
Supplemental
abundant
dial
fibers
logic
of
eFig.
6.2
eosinophilic
full
Basis
of
Pathology,
of
glycogen
Disease,
Pompe
cytoplasm.
seen
9th
University
of
ed.,
as
disease
(B)
(glycogen
Patient
clear
spaces.)
Philadelphia,
Texas
with
(From
Elsevier,
Southwestern
storage
Pompe
Kumar
2015,
Medical
disease
disease
V,
Fig.
Abbas
5.16;
Center,
type
(same
A,
II).
Aster
Courtesy
Dallas.)
(A)
Normal
magnification
J:
Dr.
myocardium
showing
Robbins
Trace
and
the
Cotran
Worrell,
with
myocar-
Patho-
Department
97.e1
98
CHAPTER
Genetic
6
Diseases
Trisomy resung
n
abnorma
•
e
unbaanced
gamees
a
may
ead
Down
ay
older
raer
a
s
an
en
os,
cromosome
mos
long
common
arm
o
erlzaon
mosome,
genes
on
D eeton
break
an
e
One
e
X
o
wo
resul
s
a
wo
arm
sor
and
gamee
monosomy
or
n
s
a
arms
s
arms
presen
cromosome
by
e
remanng
ony
socromosome
e
cromo-
dupcaed,
resung
or
o
wo
lve
ong
brs
desgnaed
conans
genes
on
a
arms.
(Xq).
normal
Xp
e
nvolves
and
e
Wen
X
e
nernal
s
are
loss
a
o
poron
ermnal
proxmal
segmen.
almos
a
segmen.
and
e
never
o
dsal
a
cromosome.
Two
nersal
segmens,
removed
reaned,
resuls
ragmen,
and
e
•
e
s
w
lacks
a
cen-
by
•
w en
and
e
ere
are
nvolve d
wo
ners a l
s eg men
reun es
bre a ks
a er
n
rom
About
eac
end
o
e
cromosome,
e
arms
une
o
orm
a
•
4%
ree
syndromes
5p,
and
and
Disorders
auosomal
(cr
22q11
ave
deleon
of
rsomes
du
cat
deeton
18,
sy ndrome,
sy ndrome)
caracersc
syndrome
Involving
(13,
clncal
occur
and
Autosomes
21; Fg.
caused
are
Only
suicen
disorder
in
o
requenc y
wo
wo
22
major
causes,
age:
20
e
wt
bu
provdes
s
s
e
and
ova
rsomy
Down
e
of
21
and
1
n
n
1550
25
lve
lve
exra
ncreased
o
e
exra
1
21;
er
syndrome
s
brs
brs
n
cromosome
suscepbly
o
undersood.
arm
14.
s
trsomy
Down
e
syndrome
penoypcally
avng
o
o
cases,
no
long
cromosome
rses
o
or
Down
e
ave
orm
ncdence
95%
reason
nvolves
21
Is
years
In
syndrome
s
nondsjuncon
or
or
Down
years.
persons
a
rsk
cases
an
resul
early
n
21
o
Aloug
deleon
cromosome
common
rsomy
lve
and
brs
22q11
mer
bre
been
known
elusve.
rom
sage
e
or
o
carry
a
robertsonan
cromosome
ranslocaed
cromosomal
normal.
Oer
21
and
segmen
maeral.
sblngs
o
e
are
a
syndrome.
moc
nondsjuncon
embryogeness.
Mouse
cromosomal
many
models
mosome
21
RNAs
responsble
s
producs
consderaon.
Clncal
o
cromosome
manesaons
bearng
gve
rse
years,
sugges
loc
o
or
e
abnormaly
e
a
encodng
e
gan
o
a
mulple
obser ved
clncal
n
paogeness
Down
o
e
parcular
proens
penoype,
eaures
reman
o
regon
and
bu
be
syndrome
dsease
21
are
ow
Balanced
Centric
fusion
Robertsonian Lost
ISOCHROMOSOMES
DELETIONS
Fragments
INVERSIONS
RING
CHROMOSOMES
Paracentric
Fragments Pericentric
6.9
Types
of
chromosomal
rearrangements.
on
cro-
mcro-
ese
gene
deermned.
reciprocal
as
remans
several
TRANSLOCATIONS
Fig.
the
varable and mlder, dependng on e proporon o abnormal cells.
and
deleon
relavely
eaures.
w
by
6.10)
o
carrer
ese
durng
Cytogenetic
chromosome
nondisjunction
Rarey, persons wt a Down syndrome penotype are mosac for trsomy
21.
rng.
as
kar yoype.
an
45
orgn.
ovum
ncreased
A rng cromosome s a varan o a deleon. Ater loss o segmens
meiotic
wt
maernal
an
maernal
agng
o
younger
older
parenal
lpp ng
common
by
syndrome
norma
lnked
cromosome
a
most
patents
a
transocaton
around.
•
of
cromosome
o cc ur
cromos ome
o
Down
ave
women
e
s
the
caused
ransocaon.
95%
women
los.
Inversons
About
srongly
or
removal
encoded
frequently
parens
sngle
breaks,
n
wc
genes
A
Syndrome)
is
mothers.
n
delee
o
most
robersonan
cro-
rsomy
(Down
syndrome
Pathogeness.
Xq.
nvolves
romere,
regon
and
w
occurs
e
may
reunon
o
vercay.
21
o
is
n
•
o
Isocromosomes are ormed wen e cenromere dvdes orzon-
some
•
ormaon
zygoes.
CHAPTER
Intellectual
Genetic
6
Diseases
Epicanthic
disability
folds
and
facial
flat
profile
Abundant
neck
TRISOMY
21:
Incidence:
1
DOWN
SYNDROME
skin
Single
in
palmar
Karyotypes:
crease
Trisomy
700
21
type:
Translocation
Mosaic
births
47,XX,
type:
type:
+21
46,XX,der(14;21)(q10;q10),+21
46,XX/47,XX,
+21
Congenital
heart
defects
Umbilical
Intestinal
hernia
stenosis
Predisposition
to
leukemia
Prominent
occiput
Intellectual
disability
Hypotonia
Micrognathia
Gap
between
first
and
second
toe
Low
set
Short
ears
neck
Overlapping
fingers
Congenital TRISOMY
18:
EDWARDS
SYNDROME heart
Incidence:
1
in
8000
defects
births
Karyotypes: Renal Trisomy
Mosaic
18
type:
type:
47,XX,
malformations
+18
46,XX/47,XX,
+18
Limited
Microphthalmia
Microcephaly
intellectual
hip
abduction
and
disability
Polydactyly
Cleft
lip
and
palate
Rocker-bottom
feet
Cardiac
defects
Umbilical
Renal
hernia
defects
TRISOMY
13:
Incidence:
1
in
PATAU
15,000
SYNDROME
births
Karyotypes:
Trisomy
13
type:
Translocation
Mosaic
Rocker-bottom
Fig.
6.10
Clinical
syndrome;
features
trisomy
18,
and
karyotypes
Edwards
of
syndrome;
the
and
three
47,XX,
+13
46,XX,+13,der(13;14)(q10;q10)
46,XX/47,XX,
+13
feet
most
trisomy
type:
type:
13,
common
Patau
autosomal
syndrome.
trisomies:
trisomy
21,
Down
99
100
CHAPTER
Clncal
Features.
obque
e
papebra
Genetic
6
acal
appearance
issures,
and
o
Diseases
e
epcanc
nan—a
ods
(see
aca
Fg.
proie,
emaes.
X
6.11)—s
cepon.
Durng
nacvaon
occurs
process,
ea
abou
o
carres
•
50.
ave
a
Mosacs
norma
g
rsk
Congenta
w
or
o
Down
oer
eart
syndrome
near-norma
deveopmena
dsease
ave
a
negence.
occurs
n
and
ave
an
mder
penoype
Down
syndrome
acqured
approxmaey
aso
dsorders:
40%
o
a
o
paens,
mos commony ara sepa deecs, arovenrcuar vave maorma-
X
•
s
o
nacvaed.
e
Penoypc
occurs
ood.
cromosome
Aresas
Cdood
o
e
acute
ger
esopagus
eukema
an
Neuropatoogc
ose
(see
n
canges
neurodegenerave
dsease
age
Abnorma
uary
bass
o
or
naa
21,
mmune
e
and
medca
dagnoss
screenng
maerna
o
ess
care
(see
rey
o
occurs
o
common.
a
raes
10-
o
17),
occur
as
n
dsease,
vruay
ncreased
on
e
a
e
and
and
s
a
s
oer
o
span
parc-
common.
persons
50
rsomes
he
w
years.
s
ea
drecy)
he
resus
n
22q11
deeon
possbe
DNA
usng
ound
karyoypng
o
n
ces
Syndrome
syndrome
he
are
in
Mos
a
he
exra
rom
X
assocaed
range
a
specrum
o
penoypes
a
•
penoypes
ncude:
ncrease
durng
•
Parayrod ypopasa resung n ypocacema
•
S czoprena and bpoar dsorder
and
poson
penoypes.
domnae,
Paens
paogeness
because
e
suspeced
deeon
aso
and
are
a
sczoprena,
22q11
deeed
on
by
o
e
Wen
paens
are
pronounced
g
rsk
wc
deeons
T-ce
sad
o
s
oug
n
su
or
psycoses
n
syndrome
encodes
grounds
uorescence
o
be
Numerical
ranging
and
many
s
up
DGeorge
s
uy
he
by
(FISH)
and
as
25%
no
genes.
ybrdzaon
suc
o
esabsed
other
in
45,X
to
patien ts
syn-
wh o
Sex
i nv o lv ing
4 9 ,XXXXY,
somes
ave
been
cromosomes
o ften
ones
a
abnormaes
maes
denied.
produce
are
nvovng
In
aypca
md
dose”
because
o
o
oss
a
and
o
are
rom
an
X
severa
cromosome,
regons
one
acve
gans
Turner
X
e
as
X
cromosome
on
or
on
bo
osses
syndrome,
X
o
cro-
X
cro-
respecvey.
the
most
from
the
common
presence
cause
of
at
of
hypogonad-
least
one
extra
X
may
e
he
be
cnca
sex
o
paens
presence
mder
syndrome
o
eer
are
o
a
ave
a
47,X XY
cromosomes
maerna
mosacs,
46,XY
or
suc
ne
n
kar yoype
durng
meoss.
paerna
as
orgn.
46,XY/47,X XY ,
mosacs
usuay
s
condon.
manesaons
s
wde,
and
ey
oten
ncude
e
bpoar
o
he
undersood,
dagnoss
may
deecon
(descrbed
o
be
e
aer).
are
w
wo
conras,
the
se x
c h ro m os o m e s ,
with
i nf e r t il it y
compared
auosoma
w
and
even
numerca
penoypes
n
ose
wc
promnen,
o
oss
evauaon
o
and
Hsoogc
may
ack
as
a
resu
o
ubues.
nfery.
Sery
examnaon
spermaogona
o
yperpasa
he
s
reveas
enrey.
or
dagnoss
due
s
an
o
yan-
Ley-
apparen
oten
made
nery.
appearance
ar
and
md,
n
some
esoserone
eves
persons
be
may
Kneeer
norma
body
s
deic
e
w
ower
a
arge
w
cancer
upus
deecabe.
germ
(20
o
exra
an
Paens
assocaed
exragonada
s
number
are
eevaed.
breas
sysemc
no
w
eves
are
syndrome
as
cases,
mosacs
ncudng
maes),
suc
eongaed
correaes
gonadoropn
dsorders,
an
g ynecomasa
and
Serum
o
are
he
a
norma,
rarey
ger
and
ere,
o
and
n
urnar y
and
46,XY
requency
more
umors,
reducon
cromosomes.
proporon
mes
ce
X
o
common
suc
ces.
severa
an
auommune
n
ds-
er yemaosus.
Chromosomes
c o m pa t i bl e
exh ibi t
aropy,
Mena mparmen. he degree o neecua mparmen ypcay
ds-
cases.
escuar
•
l ife
a nd
a nd
c e r t ai n
Turner
bo
ree
In
and
w
arge
syndrome,
females,
of
results
the
X
characterized
from
partial
or
by
primary
complete
hypogonadism
monosomy
of
the
in
short
chromosome.
cromo-
abnormaes
maes
observed
cromosomes.
Y
Syndrome
Turner
arm
norma
“ exra
Eunucod body abus, marked by reduced aca, body, and pubc
cardac
abnormaltie s .
Penoypcay
abe
Involving
abnor ma l i ti es
from
observed
Disorders
an
a
•
eases
Cytogenetic
ave
Noe
Increase n eng beween e soes and e pubc bone, wc creaes
mmunodeicency
ave
dysmorpoog y
deveops
deeon
regon
cnca
o
reaed
e
negence
and
is
Kneeer
ubues,
are
s
order
no
•
e
o
ces
md
deecs.
a
o
drome, wereas ose w e so-caed veocardofaca syndrome ave
mmunodeicency
hus,
genes
spermaogeness.
o
hymc ypopasa and mpared T-ce mmuny
dferng
w
Hypogonadsm,
Abnormates of te paate, faca dysmor psm, deveopmenta deay
or
oss
because
resung
nondsjuncon
15%
w
•
ypocacema
w
syndrome
results
47,X XY/48,X X XY .
•
and
do
cromosome.
appear
ose
cromosome
Approxmaey
dg
responsbe
and
paens
sems
zaon
sze
o
Kneeer
males
Congenta eart dsease afecng e ouow racs
e
assocaed
dsorders
syndrome
ism
•
n
wo
Syndrome
some
Varaon
emaes
X
oowng:
encompasses
hese
e
nacvaon.
Klinefelter
mpared
(de22q11).
escape
monosomy
resu rom nersa deeons o band 11 on e ong arm o cromo-
22
resu,
syndrome,
Klinefelter
he
Deletion
canges
Turner
mosomes
r-
pre-
obaned rom e concepus by amnoceness or coronc vus sampng.
22q11
a
on
chromosome.
o
around
ce-ree
(mos
s
As
ound
a
uncear.
e
dea
anayss
sudes,
necons,
auommuny,
dsurbance
age
o
n
mosomes.
Azemer
predsposes
yrod
syndrome
magng
are
cdren.
Caper
a
medan
Down
a
bood,
and
curren
9)
aso
40.
mmunoogc
e
bowe
Caper
unafeced
functon
ungs,
s
Improved
somy
an
sma
caracersc
paens
oder
and
genes
embryo
one w an acve maerna X and e oer w an acve paerna X.
are responsbe or a majory o e deas n nancy and eary cd-
20-od
•
one
deveopng
con-
cro-
yonzaon, norma emaes are mosacs composed o wo ce popuaons,
ons, and venrcuar sepa deecs (see Caper 8). Cardac probems
•
bu
mos
e
ater
Moreover, exra X cromosomes are presen (e.g., n 48,XXXX emaes),
25
may
alced
o
days
maerna
and
o
ose
ce
16
e
and remans genecay sen n e progeny o ese ces rougou e.
o
eac
or
mosome
80%
n
e,
paerna
IQ
approxmaey
nacvaed
n
e
dsaby
common;
randomy
eary
eer
caracersc and mmedaey suggess e dagnoss. Severe neecua
s
s
s
o
X
emaes,
numerca
par,
e
ack
Pathogeness. Norma oogeness occurs beore yonzaon and requres
bo
X
nay
cromosomes
deveop
o
be
normay
acve.
eary
n
In
T urner
syndrome,
embr yogeness,
bu
ea
e
ovares
absence
o
e second X cromosome eads o an acceeraed oss o oocyes, wc
o a penoype reaed o abnormaes o sex cromosomes reaes o wo
s
acors: (1) e sma amoun o genec normaon carred by e Y cro-
srands,
compee
by
age
mosome (ncudng e gene SRY a species mae sex) and (2) X nac-
syndrome aso causes nongonada abnormaes, genes requred or e
vaon (yonzaon), wc ends o baance gene expresson n maes and
grow
devod
and
o
2
years.
ova
he
and
deveopmen
o
ovares
oces
somac
are
reduced
(sreak
ssues
o
ovares).
aso
mus
aropc
ibrous
Because
T urner
resde
on
e
X
CHAPTER
cromosome.
s
s
one
Clncal
X
o
An
e
exampe
genes
Features.
cromosome
e
and
s
a
e
are
sor
acve
majory
a
45,X
o
saure
on
paens
kar yoype.
omeobox
bo
X
afeced
and
are
dagnosed
a
complee
paens
br
loss
are
o
e
one
mos
or
early
n
Short
posterior
eaures
6.11
and
assocaed
w
45,X
Turner
syndrome
stature
hairline
cldood.
Webbing
Typcal
Fg.
101
(SHOX).
Low
severely
Diseases
cromosomes.
ave
ese
gene
Genetic
6
are
sown
of
neck
n
nclude:
Coarctation
•
Growt
retardaton
and
sor
saure
(below
e
rd
of
percenle) aorta
•
Swellng o e nape o e neck due o dsended lympac cannels
(n
nancy)
a
s
seen
as
webbng
of
te
neck
n
older
Broad
and
cldren
spaced
•
Low posteror arne
•
Cubtus vagus (an ncrease n e carr yng angle o e arms)
•
Sed-ke cest w wdely spaced npples
•
Hg-arced paate
•
Lympedema
chest
widely
nipples
Cubitus
valgus
Streak
o
e
ands
and
ovaries,
ee infertility,
•
Maformatons
coarcaon
o
suc
e
Cardovascular
dea
cen
n
al
o
orsesoe
abnormales
cldood.
grls
as
kdney,
bcuspd
aorc
valve,
and
amenorrhea
aora
B ecause
develop
are
o
e
mos
ovaran
secondar y
sex
common
aropy,
cause
afeced
caracerscs:
e
o
adoles-
genala Pigmented
reman
nanle,
appears.
caused
In
Mos
by
a
developmen
paens
ave
auoanbodes
sgncan
mosacsm
46,XX
breas
(n
cells)
wc
or
by
e
prmar y
occurs
mnory
o
n
as
s
mnmal,
and
amenorrea.
many
paens,
ndvdual
srucural
s
as
T urner
made
abnormales
up
o
lle
o
paens.
syndrome
a
e
s
mxure
X
nevi
ar
Hypoyrodsm
50%
o
pubc
caused
o
45,X
cromosome.
by
and
e Peripheral
mos
common
s
deleon
o
e
sor
arm,
resulng
n
paral
monolymphedema
somy
are
o
e
X
repored
cromosome.
and
accoun
Combnaons
or
sgncan
o
deleons
varaons
n
and
e
mosacsm
at
TURNER
Some
mal
paens
w
appearance
mosacsm
and
may
or
paral
presen
only
deleons
w
ave
prmary
an
birth
penoype.
almos
SYNDROME
nor-
amenorrea.
Incidence:
In
1
in
3000
female
births
Karyotypes:
adul
paens,
a
combnaon
o
sor
saure
and
prmary
amenorrea Classic:
sould
promp
srong
suspcon
or
T urner
syndrome.
e
dagnoss
45,X
s Defective
usually
esablsed
by
karyoypng. second
X
chromosome:
46,X,i(Xq)
46,XXq–
SINGLE-GENE
DISORDERS
WITH
PATTERNS
INHERITANCE
ATYPICAL
46,XXp–
46,X,
OF
Mosaic
ree
groups
o
genec
dseases
resulng
rom
sngle-gene
no
ollow
mendelan
rules
o
r(X)
45,X/46,XX
muaons
Fig.
do
type:
6.11
Clinical
features
and
karyotypes
of
Turner
syndrome.
nerance:
•
Dseases caused by rnucleode repea muaons
•
Dseases caused by muaons n mocondral genes
A
unque
eaure
o
dseases
caused
by
rnucleode
repea
mua-
ons s a penomenon called antcpaton, n wc e dsease becomes
•
Dseases assocaed w aleraons o mprned regons o e genome more
severe
relaed
Trinucleotide
Repeat
Mutation
o
repeat
diseases
are
eac
successve
dynamc
naure
o
generaon.
s
rnucleode
unusual
repea
eaure
muaons.
s
An
Diseases example
Trinucleotide
w
e
caused
by
mutations
that
can
be
ound
n
Hunngon
dsease,
n
wc
expanson
o
amplify a
CAG
repea
sequence
wn
e
Hunngn
gene
(HTT)
gene
s
a DNA sequence consisting of three base pair (trinucleotide) repeats. responsble
ey Pathogeness.
Fragle
X
syndrome,
Hunngon
dsease,
and
are
all
assocaed
w
neurodegeneraon,
are
among
e
examples
o
genec
dseases
caused
by
rnucleode
a
e
expansons
may
nvolve
e
promoer,
o
(as
e
n
encoded
mRNA
Hunngon
(as
n
dsease,
ragle
X
descrbed
syndrome),
n
Caper
or
gene.
o
s
Wen
muaons
suppressed
and
ere
afec
s
noncodng
“loss
o
regons,
uncon. ”
By
nvolvng
codng
sequences
o
e
gene
encode
oten
gve
rse
ablty
racs,
wc
c yoplasm,
a
cause
proen
common
msoldng
eaure
o
dseases
and
encode
polygluamne
aggregaon
suc
as
number,
a
s
more
spermaogeness,
severe
and
occurs
an
earler
aler-
n
compared
o
e
dsease
n
e
paren.
Snce
le
CAG
polygluamne
are
oten
racs
called
n
e
afeced
ploygluamne
proens,
dseases.
For
CAG
unclear
oer
rnucleode
repea
repea
nsably
dseases,
s
more
suc
as
ragle
pronounced
n
X
ds-
develop-
and
wn
Hunngon
down
ence
ancpaon
roug
e
s
seen
wen
e
abnormal
alleles
moer.
o
by
a
dsease
muaon
oocyes,
passed
dsease.
repeas
ceran
RNA
Frag le
CAG
n
rple
and ave a oxc “gan-o-uncon” acvy. s propery s conerred
nvolvng
n
ofsprng
dseases
msolded proens a bo nerere w e uncon o e proen
muaons
a
conras, are
muaons
durng
reac
e
ng ranslaon
expansons
repeas
codng
16)
ease, afeced
ese
repea
reasons, regons
urer
Once
unranslaed repea
porons
resuls
afeced
repeas expansons.
o
dsease.
more n
promnen
prone
e
myoonc aon
dysropy,
or
e
dsease.
I
X
syndrome
It
s
(ater
resuls
wc
the
Down
rom
encodes
s
the
second
a
e
prototypc
most
trnucleotde
common
genetc
repeat
cause
o
mutaton
mental
ds-
syndrome).
rple
repea
amlal
muaon
menal
afecng
reardaon
e
proen
FMR1
gene,
(FMRP).
As
102
CHAPTER
w
a
males.
cles
30
X-nked
Afeced
are
presen
CGG
dseases,
males
n
repeas
n
rage
ave
90%
o
e
Genetic
6
a
long
cases.
FMR1
X
syndrome
ace
In
Diseases
and
unafeced
gene,
afecs
large
males,
wereas
predomnanly
mandble.
n
Large
ere
afeced
are
es-
and e paen develops Angelman syndrome. e precse way a e
afeced
genes
conrbue
males
200
ons
o
w
52
muaons
e
4000
o
by
200
marked
o
ese
repeas.
urer
ranslaon
causes
repeas.
“ull”
e
menal
arse
premuaons
amplcaon
synapc
muaons
durng
proens,
and
are
absence
FMRP
n
syndromes
s
no
undersood.
OF
GENETIC
DISORDERS
premua-
convered
oogeness.
s
rom
ese
ere
DIAGNOSIS are
o
around
o
ull
regulaes
afeced
males
dsably.
Once
der,
a
penoype
pedgree
s
recognzed
analyss
may
be
a
used
o
suggess
urer
a
parcular
evaluae
e
genec
dsor-
possbly
a
a
genec dsease s segregang wn a amly. e absence o oer afeced
amly
members,
owever,
does
no
exclude
a
genec
dsorder,
as
many
muaons arse de novo. An addonal conoundng acor s nonpaerny,
Diseases
Caused
by
Mutations
in
Mitochondrial
Genes
esmaed o nvolve 2% o 5% o brs. Conrmaon o a suspeced genec
dsorder
Mitochondria
in
the
fertilized
zygote
are
entirely
derived
from
reles
on
specc
ess,
wc
also
ave
mporan
roles
n
evalu-
the ang euses a are deemed o be a ncreased rsk or genec dsorders.
ovum;
thus,
only
mothers
transmit
mitochondrial
genes
and
their e
defects
to
their
erang
s
unusual
paern
o
ransmance
s
reerred
o
as
o
A
esng
Dseases
caused
by
muaons
n
bre
or
genec
revew
o
dsorders
curren
s
esng
evolvng
a
modales
a
rapdly
and
er
accel-
use
or
materna e
nertance.
eld
pace.
offspring.
mocondral
genes
dagnoss
o
genec
dsorders
s
ofered
below
and
s
summarzed
n
are T able 6.5.
rare.
One
class
dral
dsorders
on,
and
as
o
mocondral
encode
mg
be
genes
enzymes
a
nvolved
expeced,
e
s
n
ssues
muaed
n
oxdave
a
are
mocon-
pospor yla-
mos
afeced
Genetic
Test
Modalities
and
Applications
n Tess a are used o conrm e dagnoss o varous genec dsorders
ese
dsorders
are
ose
a
are
mos
dependen
on
oxdave
posare
por ylaon,
a
s,
skeleal
muscle,
e
ear,
and
e
desgned
o
deny
e
causave
genec
abnormaly
or,
n
some
bran. nsances, e efec o e abnormaly on proens encoded by muaed
genes.
Diseases
Caused
by
Alterations
of
Imprinted
1.
Prader-Willi
and
Angelman
ese
genes
through
and
are
normally
epigenetic
disturbances
abnormal
gene
this
process
expression
and
in
to
differential
male
(termed
and
“silencing”
female
imprinting)
developmental
gametes,
can
lead
were
blood
to
e
acves
on
o
omologous
e
male
and
maernal
emale
and
abnormalities.
alleles
paernal
o
some
dfer.
ese
mprnng
reers
o
ranscrponal
slencng
o
e
maernal
ovum
derved
Two
an
o
or
e
rom
syndrome
e
sor
(Fg.
gonadsm.
ound
•
n
ype
also
as
e
be
nal
all
are
Afeced
ga,
n
uncon
gene
Prader-Wll
some
15q12
uncon
deleed
o
all
by
occurs
n
somac
deecs
syndrome
e
e
and
dsnc
s
no
greaer
and
nvolvng
ton
Angelman
nellecual
n
o
all
cromosome
and
w
and
band
q12
e
dsably,
and
n
e
long
dsably,
syndrome.
Afeced
15q12,
cromosome
a
bu
15
e
scope.
s
o
as
(a
peno-
o
ese
s
o
paens
an
e
depends
on
s
A
e
(and
paernal
dferen
on
syndromes
compleely
e
depends
maernal
wo
mprnng.
on
allele,
gene
e
gene
allele.
and
a
s
se
ence
los
paernal
A
complex
o
genes
slenced),
I
e
e
also
maps
uncon
allele.
agan
s
suc
a
o
I
can
a
Tests
compleely
s
los
a
w
and
s
beng
several
caegores:
anayss,
n
w
ybrdzed
a
dye
a
bands
replaced
(CGH),
DNA
a
dark
labeled
sde
span
n
e
on
by
n
wc
wo
o
e
DNA
dferen
an
array
genome.
rao
produces
eac
mea-
o
o
a
a
unque
cromosome.
array-based
wc
correspondng
cange
o
a
and
tat
3.
can
are
s
rom
compar-
a
paen
uorescen
o
probes
Over-
or
dyes.
dspayed
underrep-
parcuar
uorescen
se
ag
genomc
1
o
(PCR),
s
a
genome,
uo-
rsomes
snge
can
and
or
n
beng
a
18,
used
requres
ave
bood
n
o
n
and
regons
sex
by
n
parc-
a
norma
many
by
(NGS),
a
poymerase
w
bu
cromo-
21.
genes,
ybrdzng
sequencng
wdey,
aso
maerna
sequence
specay
e
numbers
compared
and
on
mcro-
ransocaons
muaon
sequencng
DNA
nerpase
ess
ampied
o
afec-
denicaon
canges
DNA
sequences
s
be
easer
capurng
and
or
sequence
ncude
I
ybrdza-
uorescence
osses,
13,
genes.
generaton
and
compex
a
muc
dscree
conanng
spreads
ound
number
regon
nuceode
next
DNA
as
o
stu
woe-cromosome
becomng
by
n
Moecuar
appcaons
sequenced,
s
gans,
aso
abnormaes
probes
w
6.13).
ea
copy
n
and
number
compemenar y
assess
o
e
meapase
(Fg.
ncudng
mutatons
o
o
s
ree
o
by
Fuorescence
vsuazed
Curren
afordabe
resus
ce
nerpre,
cromosoma
cromosoma
deecon
caed
o
en
use
I
o
ony
array.
apped
bopsy)
sequence.
easy
Fuorescen
regons
suspeced,
enre
e
regons.
auosomes,
s
n
s
med
deny
deec
eus.
detect
s
ybrdzes
a
e
meod,
e
o
genomc
qud
ncreasngy
o
presen
wc
reacton
e
cuure,
wc
used
probe
known
hs
ce
neres
and
gene
even
e
gene
a
are
and
genomc
FISH
reerence
cromo-
s
s
o
he
sex
can
genes
a
are
deveoped
somes
2.
develops
suc
as
requre
deveopng
ea
maer-
paernal
paen
cromosome,
maernal
bu
on
on
resouon,
so-caed
uar
mprned
uncon
no
karyotype
saned
lg
paen
scored
parcuar
e
deleon
raer
mxed
o
cromosome,
been
lauger,
conrol
spos
specic
nuce.
ypo-
deleon
by
ybrdzaton
are
(FISH)
ng
15.
nellecual
cromosome
derved
ee,
cases
napproprae
Prader-Wll
conex
15q12
gene
DNAs
does
cells
cromosome.
bass
e
by
ands
deleons
assocaed
nvolvng
mprned
s
rom
s
rom
syndrome.
s
derved
maernally
derved
ave
small
(15q12),
sezures,
dsnc
molecular
deleed,
o
caused
caracerzed
obesy,
15
paernally
cromosome
gene
are
Prader-Wll
paens
syndrome
undersood
s
ypoona,
e
paernally
Imprnng
he
sequences
deleons
n
sperm.
ransmed
dsorders
regon,
syndrome
aaxc
ave
occurs
e
6.12).
e
que
n
sably
normal
probes
genec
cromosome
Angeman
well
allele
en
dvded
rescen ag 2. Array CGH as severa advanages over kar yoypng: I
zygoe.
saure,
o
s
genomc
Prader-W
arm
and
uncommon
mprned
•
paernal
sperm
a
regon
are
kar yoypng
genomc
resenaon
allele n e ovum, wereas paernal mprnng reers o ranscrponal
slencng
solely
alernang
and
as
dferences arse rom an epgenec process called genomc mprnng.
Maernal
o
Increasngly,
cromosomes,
genes
dened
lympocyes)
paern
Pathogeness. Aloug all umans ner wo copes o eac auosomal
carred
broadly
pase cromosomes prepared rom culured cells (usually perperal
atve
gene,
be
Syndromes
subject
modications
in
can
T ests tat detect structura abnormates of cromosomes. Hsorcally,
ese
Certain
ess
Regions:
a
s
o
ese.
becomng
nerpreaon
raned
ndvduas.
Tests tat detect bocemca abnormates assocated wt partcuar
genotypes.
In
many
nsances
nvovng
snge-gene
dsorders,
s
CHAPTER
Imprinted
MA TERNAL
P A TERNAL
(M)
(P)
Prader-Willi
Active
genes
Active
Angelman
Deletion
in
Deletion
mater nal
Prader-Willi
Imprinted
Angelman
Active
Testing
Modalities
for
Genetic
Genetics
of
Angelman
Prader-Willi
SYNDROME
syndromes.
Applications
and
Examples
Assays
assays
for
metabolites
or
electrolytes
Detection
of
detection
of
and
Disorders
Type
Assay
deletion
gene
PRADER-WILLI
6.12
of
Angelman
SYNDROME
Fig.
Quantitative
Prader-Willi
genes Site
ANGELMAN
Biochemical
(P)
deletion
gene
Test
pater nal
(M)
Imprinted
6.5
in
chromosome
genes
Table
Angelman
gene
(P)
Active
of
103
Prader-Willi
Imprinted
chromosome
Site
Diseases
genes
gene
(M)
Genetic
6
enzyme
activity
Detection
abnormal
of
high
metabolite
sodium
of
enzyme
of
abnormal
levels
deficiencies
levels
in
in
metabolic
sweat
(e.g.,
(cystic
acid
disorders
(e.g.,
phenylketonuria);
fibrosis)
maltose
in
Pompe
disease;
G6PD
defi-
Down
syn-
ciency)
Hemoglobin
electrophoresis
Cytogenetic
Detection
hemoglobins
(e.g.,
sickle
hemoglobin)
Assays
Karyotyping
Grossly
evident
structural
changes
in
chromosomes
(e.g.,
trisomy
21
in
drome)
Fluorescence
in
situ
hybridization
(FISH)
Subtle/submicroscopic
structural
changes
in
chromosomes
(e.g.,
del(5)
in
cri
du
chat
syndrome)
“Molecular”
Multiplex
Cytogenetic
ligation-dependent
Array-based
genomic
NextGeneration
Assays
probe
amplification
hybridization
sequencing
Small
deletions
changes
Copy
number
changes,
changes
(e.g.,
and
(e.g.,
partial
trisomy
21
in
deletion
Down
translocations
(mainly
translocations
in
used
cancer
of
BRCA1
in
familial
breast
cancer)
syndrome)
clinically
to
identify
somatic
copy
cells)
Assays
Allele-specific
PCR
and
related
techniques
Specific
CFTR
Sanger
insertions
number
number
Genetic
and
Copy
DNA
sequencing
base
pair
mutations
Mutations
in
changes
in
cystic
individual
(single,
e.g.,
sickle
hemoglobin
mutation,
or
multiple,
e.g.,
fibrosis)
genes
(e.g.,
glucose-6-phosphatase
mutations
in
von
Gierke
disease)
NextGeneration
sequencing
Mutations
in
mutations
unusual
many
in
genes
cancer
and/or
cells
phenotypes)
and
in
in
noncoding
research
to
regions
(used
discover
clinically
mutations
to
identify
responsible
somatic
for
104
CHAPTER
Genetic
6
Diseases
B
A
Fig.
6.13
trisomy
Fluorescence
18.
Three
centromere
specific
cent
to
for
probes
with
deletion
ceaper,
er
drecy.
ss;
or
uncons
Exampes
dencaon
aser
an
o
o
abound
o
g
onura;
dencaon
dsease;
and
o
of
o
es
o
red
probe
of
used,
one
22q11.2
for
or
ncude
indicating
(Courtesy
n
emoglobn
enzyme
DNA
n
n
levels
red
decences
n
a
Y
used:
copies).
chromosome
two
Nancy
R.
22q13
proens
bro-
sckle
(B)
this
22q13
One
region.
and
Jeff
or
precedng
e
meods,
esng
and
dsorder.
esng,
on
o
nclude
bes
genetc
e
can
se
anayss
ree
by
eal
or
be
o
ollowng:
e
wc
deecon
cell
varey
ecnques
persons
o
no
avalable
applcaon
e
o
ese
requre
genec
suspeced
genec
prenaal
and
posnaal
ndcaons.
be
ofered
abnormal
amnoceness,
DNA
o
judcous
dvded
sould
cyogenecally
obaned
cell
own
some
For
recognze
ecnque
esng
s
dseases.
o
and
two
and
the
suspected
chromosome
an
which
aqua
two
other
gives
Cytogenetics
probe
fluores-
hybridizing
chromosomes
abnormality
Doolittle,
X
does
rise
to
not
the
Laboratory,
greaer
rsk
o
rsomes
carrer
robersonan
saus
or
ranslocaon,
a
or
balanced
recprocal
ranslocaon,
nverson
•
A cromosoma abnormay afecng a prevous cld
•
D eermnaon
carrer
of
o
genec
fea
an
sex
wen
X-lnked
anayss
e
genec
usually
s
paen
or
parner
s
a
con-
dsorder
perormed
on
perperal
blood
Analysis
descrbed
genec
mporan
w
avng
or
o
Genec
eac
cells
ral,
s
e
Prenata
rsk
dscusson
dagnoss
in
with
Conirmed
lympocyes
e
This
the
copy),
spread
(green)
the
for
•
Posnaa
Genetic
(one
patient
Advanced materna age (beyond 34 years), wc s assocaed w
rmed
for
of
male
•
dsorders.
Indications
a
specific
metaphase
region
in
from
probe
centromere
A
signals.
Schneider
penylke-
n
green
Dallas.)
muaon
wde
nucleus
a
chromosome
microdeletion
cysc
n
cells
to
are
a
Interphase
been
(three
Center,
muaed
esng
penylalanne
Dr.
Medical
the
18
There
(A)
have
for
hybridizing
underyng
swea
specific
(red).
22q11.2,
aeraons
e
(FISH).
probes
chromosome
Southwestern
deny
sckle
hybridization
fluorescent
syndrome.
Texas
serum
dencaon
been
probe
and
a
region
22q11.2
University
or
copy),
have
the
situ
centromere
chromosome
stain
easer,
(one
the
in
different
obaned
on
o
all
progeny.
I
coronc
rom
paens
may
vllus
maernal
be
wo
a
perormed
bopsy
blood.
are
mae-
Indcaons
because
o
ease
o
samplng.
Indcaons
are
as
ollows:
•
Mupe congena anomaes
•
Unexpaned neecua dsaby and/or developmenal delay
•
Suspeced aneupody (e.g., eaures o Down syndrome)
•
Suspeced unbaanced auosome (e.g., Prader-Wll syndrome)
•
Suspeced sex cromosome abnormay (e.g., Turner syndrome)
•
Suspeced frage X syndrome
•
Infery (o rule ou a sex cromosome abnormaly)
•
Mupe sponaneous aborons (o rule ou a balanced ranslocaon
n
a
paren)
7
Diseases
of
Blood
Vessels
O U T L I N E
Mechanisms of Vascular Diseases, 105
Kawasaki
Congenital
Thromboangiitis
Vascular Anomalies,
Hypertension,
105
106
Atherosclerosis,
Small-Vessel
107
Infectious
Aneurysms and Dissections, 110
Disorders
of
Vasculitides,
Vasculitis,
Veins,
Aneurysms,
110
Varicose
Dissections,
111
Thrombophlebitis,
112
Cell
Takayasu
ease
(Temporal)
Arteritis,
arges
o
because
e
and
can
s
a
bran,
rom
as
dseases
un,
and
surgca
o
low
oer
va
aso
are
and
common
e
ear,
e
soud
be
e
o
as
organs.
oowng
o
n
reaed
e
and
ner venons,
moray
bood
and
Aoug
a
Saes.
aerosceross,
serous
In
vascuar
Uned
causes
dscusson
o
crcuaor y
cncay
sysem
a
ea
efecs
yperenson
separaes
recognzed
nersum
he
many
deeerous
addon,
ds-
and
dsurbances
low
se
sgn-
dseases
e
prmar y
o
(see
uncon
componen
neracons
n
Caper
w
be
oten
ave
o
e
o
sass
sage
gged
mporan
mpacs
rougou
e
on
anoer.
oowng
Caper
bood
or
or
o
VASCULAR
Common
vascuar
o
dsease
eer
progressvey
romboss
•
compete
or
(e.g.,
by
caper
and
Anaomc
Anaomcay,
arera
uson
o
venous
ck
and
gases
pressure
umna
wc
roug
of
vesse
aerosceross)
and
CO
n
reguaon,
voume
o
a
norma
2
)
reurn
rc
can
suppy
and
wo
umens,
or
bre
prncpa
o
wereas
vesses
s
manans
lud
e
capar y
appens;
ear.
musce
venous
owng
covered
crcumsances
baances
a
dsurbances
dsease.
ranson
can
aer
vascuar
Aso
rom
o
endo-
mporan
norma
endoea
are
amnar
uncon
and
dsease.
ANOMALIES
bood
and
vesses
are
common
ner venona
caenges.
Severa
may
bu
are
cardoogss,
cause
argey
or
dsease,
o
con-
wom
ey
owever,
and
menon:
Berry
aneurysms
(e.g.,
by
by
ces
a
nbs
and
er
ayer
pay
•
ave
e
no
or
o
d-
nner
endoea
and
vascuaure
vens
can
n
was
he
ces,
n-waed
arera
•
deecs
an
or
vens,
oupoucngs
n
cerebra
are
may
e
medum-
produces
and
arera
orm
cardac
o
e
s
a
senoss
o
o
a
nracerebra
vascus.
aure
by
can
arera
as
areres
be
deve-
aneur ysms
areres
vesses,
and
may
Arerovenous
sunng
rreguar
be
o
may
arge
vens,
occur
suas
voumes
o
crcuaon.
muscuar
or
beween
hey
perce
adjacen
venous
oca
bed.
rupure
njures
orms
arge-szed
umna
aa
connecons
capar y
ater
necross
dyspasa
and
abnorma
oowng
oer
causng
17).
ner venng
g-oupu
rom
Fbromuscuar
o
stuas
nlammaor y
cause
sponaneousy,
Caper
wou
necons
bood
rupure
(see
adjacen
rom
w
ave
roe
dsensby.
coaguaon
beween
g-pres-
were
key
may
Arterovenous
opmena
vesses
a
ey
emorrage
ow-pressure
Arera
and
vesses
o
no
beds,
are
vesses, mos commony ound a branc pons around e crce o
occurrng
acuey
subdvded
soues
bood
capacy,
be
bood;
smoo
o
surgeons
deser ve
and
vascuaure
wc
wc
surace
and
2
was
bood
under
maon
(O
vesses,
g
e
o
VASCULAR
varans
o
cnca
embosm)
vesses,
muscuar
bood
ony
presen
Weakenng o vesse was, causng daon and/or rupure
sure
low
ypes
dscuss,
DISEASES
deveop
obstructon
because
urbuen
severa
w
vascuar
hese
Ws;
or
low,
we
n
ear
mecansms:
Narrowng
As
W s as a bre prmer, we now urn o specc dseases o bood
•
orms
3).
common
vesses.
cern
OF
115
deecs
8
MECHANISMS
•
115
116
are
CONGENITAL one
114
115
Sarcoma,
Angiosarcomas,
compcaons
romboss
dsease.
114
114
Hemangiomas,
113
cause
compromses
venous
uncon
by
112
Kaposi
medca
eadng
aken
ear,
vesses
n
Arteritis,
113
Nodosa,
advances
remans
Disease),
Tumors of Blood Vessels and Lymphatics, 115
Polyarteritis
Despe
Veins,
(Buerger
114
114
Aortic
Giant
n
114
Obliterans
Aortic
Vasculitis,
on
Disease,
ckenng
areres.
assocaed
he
o
wa
w
e
was
ckenng
abnorma
ves-
nlam-
se spasm a reduces vascuar low. In e rena areres, can ead
and
o
e
renovascuar
ypertenson.
105
106
CHAPTER
Diseases
7
of
BLOOD
Blood
Vessels
HUMORAL
VOLUME
FACTORS
Sodium Constrictors
Dilators
Mineralocor ticoids Angiotensin
Atrial
natriuretic
II
Prostaglandins
peptide Catecholamines
Kinins
Thromboxane
NO
Leukotrienes
Endothelin
LOCAL
BLOOD
CARDIAC
PERIPHERAL
PRESSURE
OUTPUT
RESISTANCE
FACTORS
Autoregulation
pH,
Constrictors CARDIAC
Dilators
FACTORS
α-adrenergic Hear t
hypoxia
β-adrenergic
rate
Contractility NEURAL
Fig.
7.1
Blood
pressure
regulation.
ave
NO,
b een
FACTORS
nitric
oxide.
mpcaed
n
e
rsk
o
de veopng
yp er enson,
bu
n
HYPERTENSION 95%
Sustained
high
end-organ
damage
Bood
ensure
blood
pressure
dever y
o
peruson,
organ
Low
a
(hypertension)
major
be
and
2
wases.
is
mus
O
meaboc
pressure
and
risk
factor
mananed
nurens
pressure
dysuncon,
o
wn
ssues
and
severe
narrow
remova
resus
and
vessel
and
atherosclerosis.
a
and
(ypotenson)
causes
for
range
o
n
CO
o
and
2
nadequae
sysemc,
sock
and
somemes dea (see Caper 3). Muc more common s ypertenson,
an
nsdous
bu
mporan
cause
o
morbdy
and
ta
o
cas es
e
y per tenson).
s econdar y
(e.g.,
o
umors
R arey,
Resng
bood
pressure
s
a
ncreas e
kdne y,
s ecreng
ressance
empaszng
(Fg.
o
7.1).
low,
A
o
wc
ese
s
dcaed
acors
are
uncon
by
e
subjec
o
cardac
muscuar
o
by
ormones
produced
by
e
one
reguaon
o
and
as
we
as
by
neura
npus
rom
e
kdney
and
e
ear
adrena
o
es e
or
o
o cc ur
umors
epneprne).
ndvdua
reabs or pon
mp or ance
essen-
genes
s o dum
mecansms
by
o
a
e
bo o d
Hyp er enson
sympaec
ner vous
canges
n
acceeraes
e
wa s
o
a erogeness
arge-
and
and
c aus es
me d u m -s ze d
a
can
ead
o
(descrbed
aorc
aer
dssecon
and
n
and
Caper
cerebrovascuar
17).
Areroes
can
(Fg. be
afeced
by
ese
canges.
sysem,
Hyane
arteroosceross
s
marked
by
ckenng
o
e
arer-
oows: was
by
pnk,
amorpous,
yane
maera
and
narrowng
Renn s a ormone a s produced n e kdney by ces a sense o rena
peruson.
renn,
a
Decreased
peruson
smuaes
producon
vesse
umens
proease
a
ceaves
crcuang
angoensnogen
o
ensn
and
pds
7.3A).
a
he
eak
ckenng
across
njured
s
caused
by
endoea
pasma
ces
no
angovesse
was
and
by
ncreased
producon
o
exraceuar
marx
I. proens
he
(Fg.
o proens
•
or
n
caed
yp er enson
norepneprne,
muaons
s
are-
oar
•
by
pro ducon
e
o
ormone-s ecreng
adoserone,
caus ed
cas es
coun-
• as
remanng
or
(ence
oupu
aso 7.2),
unknown
conro.
emorrage erreguaon
e
s
moray.
ar er es roes
o
s
adoserone
pressure
caus e
ds eas e
yp er enson
degenera ve and
Mos
rena
Morphology. Pathogeness.
sp ecc
acve
orm
o
angotensn
s
a
ormone
w
wo
(1)
ncreases
vascuar
smoo
musce
by
smoo
musce
ces.
mporan
• acves:
one
and
Hyper pastc arteroosceross s more ypca o severe yperen-
ressson.
Vesses
exb
“onon
skn, ”
concenrc,
amnaed
ck-
ance o low and (2) smuaes e reease o adosterone rom e enng adrena
gand,
eadng
o
ncreased
reenon
o
sodum
by
e
and
ncreased
bood
voume,
wc
n
urn
enances
sroke
voume,
and
cardac
oupu.
Bo
o
ese
and
bood
pressure.
he
acve
orm
o
angoensn
s
deposon
umna
due
o
proeraon
o
smoo
musce
o
narrowng
basemen
(Fg.
membrane
7.3B).
In
ver y
maera,
severe
eadng
yperenson,
aeraons brnod
rase
was
cardac o
ng,
areroar
kdces
ney
o
creaed
necross
o
vesse
was
may
occur.
by
successve ceavages o angoensnogen by renn oowed by ango-
ensn-converng
rea
•
he
o
ear
ara
bood
rena
voume
sympatetc
cardac
ob esy,
mporan
arge
o
drugs
used
o
reeasng
on
bood
ese
nervous
a
o
respond
atra
sodum
o
ncreased
natruretc
and
waer
srec
ormone,
and
ereby
due
wc
owers
or
o
s
ormona
system,
dened,
130
greaer.
smokng,
Clncal
wc
reguaors
ac
o
are
ncrease
npus
vascuar
rom
one
e
and
mm
B o
Hg
s ome wa
or
greaer
genec
pysca
and
nacvy,
arbrary,
or
a
as
dasoc
envronmena
and
g
sa
a
resng
pressure
ac ors
sys-
o
80
(sress,
consumpon)
Features.
many
carda
ons
years
ncude
areroes.
(e.g.,
Uness
un
narcon,
enance
pressure.
oupu.
pressure
Hg
by
and
Hyp er enson
mm
ces
excreon
Supermposed
oc
an
or
conans
daon
ncreases
•
enzyme,
yperenson.
aorc
sowy
hese
rena
severe,
aneur ysm)
progressve
compcaons
sodum
or
aces
o
>
mm
200
prevenve
Hg)
and
aered
can
ead
dea
yperenson
o
and
s
ess
sensorum.
a
aure
be
or
o
hs
varan,
emergency
due
mos
s
a
sroke,
rena
and
screenng
mporan
(sysoc
w
magnant
a
producon
hereore,
efecve
requres
o
medcaons
angoensn
aure,
myo-
presena-
narrowng
by
assocaed
ermed
rena
asympomac
dramac
yperenson
and
be
(e.g.,
o
nbors).
e
Severe
Less
prevened
nb
commony
emorrages,
medca
deveop.
enzyme
one
medcne.
occurs
rena
s
may
compcaons
rena
can
excreon
angoensn-converng
paens
yperenson
cardovascuar
pressures
eadace
ypertenson,
cerebra
mmedae
edema,
and
reamen.
CHAPTER
Atrial
natriuretic
Diseases
7
of
Blood
Vessels
107
peptide
Cardiac
volume
sensors
+
Excretes
and
Vasodilation
Na
water
Blood
volume
BLOOD
Normotension
PRESSURE
BLOOD
PRESSURE
Blood
Vaso-
volume
(Low
volume
renal
or
low
ar ter y
constriction
resistance;
stenosis)
+
Resorbs
and
Na
water
Aldosterone Low
renal
pressure
Low
renal
sodium
Adrenal
Liver
Renin
Angiotensin
II
AngioAngiotensin
I
tensinogen Angiotensin-conver ting
enzyme Endothelium
Fig.
7.2
Interplay
of
renin,
angiotensin,
aldosterone,
in
and
many
atrial
tissues
natriuretic
o
es e
peptide
a re
in
blood
ox d z e d
pressure
ow - d e n s y
regulation.
p opro e n
( L DL )
and
co-
ATHEROSCLEROSIS e s e ro
Atherosclerosis
underlies
and
vascular
peripheral
mortality
in
the
Orgnay
ross
s
des
and
conned
ncreasngy
esyes
ateromatous
low.
e
More
aer
and
daon
o
many
and
o
provokes
on
n
e
vesse
aeromaous
o
causes
any
cnca
more
paques
vesse
counres
caed
and
can
rapd
re c o g n z e d
and
by
aerosce-
as
resrc
or
o
or
as
vesses
consequences.
chronc,
Atheroscleross
repettve
appears
endothelal
njury
to
the
leadng
to
consequence
inlammaion
o
and
vesse wa damage
he
over
ng
•
evens
decades
scenaro
a
(Fg.
s
•
an
hs
are
eves
or
resus
smoo
o
r g ge r ng
In
oer
rsk
pre s e n ,
“d a n g e r
an
e y
a re
s g n a s” )
n a m m a or y
o
o
Facors
T
ce
ces,
marx
conrbues
a
o
be
o
dyspdema
assocaed
are
reease
and
e
naon,
e
suc
pro-
esons.
(yperenson
major
naors
assocaed
aso
ncreased
o
w
g
assocaed
w
aerosceross.
w
nlam-
componens
acors
e
condons
sgncan
o
wc
proeraon
aerosceroc
beeved
genera,
cncay
accumuaon
and
emodynamc
are
orms
o
mupcave.
and
low)
e
musce
nlammaon
bood
n
exraceuar
compcaons
damage.
ncreased
cumnae
7.4)
and
are
n
ormaon
no
enrey
o
an
aeroma
undersood,
bu
pay
e
ou
oow-
•
Hy percoesteroema.
speccay
LDL,
ss
fama
seen
kocye
deecs
adeson,
wa
(so-caed
macropages
deposon
and
urbuen
s
ve ss e
n or m a y
Rsk
rsk
acors
ncude
e
oowng:
avored:
and
and
Ac c umu at on
and
nduce
Hypercoeseroema
and
Endotea njury eads o ncreased vascuar permeaby and eu-
nlammaon
n o
m a c rop a g e s ,
ncudng
a
coagen.
endoea
be
as
a re
sub s anc e s
nlammaton
ces,
gresson,
sec-
aneur ysma
wa
syness
LDL
Pathogeness.
es e
ore g n
suc
c yoknes
racure;
o
Vesse
maor y
bood
Inlammaon
eadng
•
Wesern
ateromas
beed
ce s
as
Snce
re s p on s e
occuson
ssues.
was,
morbidity
counres,
umens
causng
cerebral,
disorder.
nma
downsream
weaken
coronary,
other
ower-ncome
romboss,
can
of
ger-ncome
Lesons
narcon
sgncan
and
than
n
mpnge
mporany,
and
disease,
spread.
aeromas
pathogenesis
world
prevaen
paques
oten
scema
ondar y
western
the
cr ys a s.
of
aers
endoea
gene
expresson,
avorng
romboss.
p o prote n s
b e c au s e
o
esero
an d
e n d o e a
a s s o c ate d
d amage.
p d s
Te
o cc urs
mos
n
e
mp or a n
n
caracerzed
n
e
o
by
LDL
he
cenra
gged
roe
by
e
o
recepor.
LDL
ssues
poproen
coesero
serum
(HDL)
rom
LDL
(“bad”
ncudng
e
coesero,
acceeraed
y percoesteroema
eevaed
perpera
g-densy
mobzes
s
(see
Caper
eves
due
coesero)
e
coesero
perper y
vesse
o
6),
more
wc
nered
devers
wa,
(“good”
and
and
aeroscero-
co-
wereas
coesero)
ranspors
o
e
108
CHAPTER
Diseases
7
of
Blood
Vessels
Endothelium
Intima
Media
Adventitia
1.
Chronic
endothelial
“injur y”:
Hyperlipidemia
Hyper tension
Smoking
Homocysteine
Hemodynamic
T oxins
Viruses
Immune
factors
Response
to
injur y
reactions
A
2.
Endothelial
(e.g.,
dysfunction
increased
per meability , Platelet
leukocyte
adhesion), Monocyte
monocyte
and
3.
adhesion,
migration
Macrophage
activation,
B
Smooth smooth
muscle
recruitment,
muscle accumulation Fig.
7.3
Hypertensive
vascular
disease.
(A)
Hyaline
arteriolar
teinaceous
wall
(B)
Hyperplastic
nal
obliteration
MD,
Brigham
ver
is
material
or
thickened
with
(hyalinized),
arteriolosclerosis
(periodic
and
bar y
lumen
stain).
Hospital,
excreon.
deposition
the
is
(onion-skinning)
acid–Schiff
Women’s
the
and
(B,
w
a
reduced
of
amorphous
markedly
(arrow)
Courtesy
pro-
Fatty
narrowed.
causing
Helmut
Rennke,
S evera
oer
ger
acors
eves
o
HDL
assocaed
cor-
w
4.
Macrophages
rsk
smokng,
dabees)
o
aerosceross
ower
HDL
(de,
sedenar y
eves
or
esye,
eevae
LDL
and
muscle
cells
an engulf
ncreased
streak
lumi-
Boston.)
C onsequeny,
rsk.
cell
in
wall
smooth
reae
lipids
arteriolosclerosis. vessel
The
of
lipid
obesy,
eves.
Sa-
Lymphocyte
n
drugs,
eves,
wc
aso
ower
nb
e
coesero
rsk
o
syness
and
aerosceross-reaed
suppress
LDL
cardovascuar
Fibrofatty
atheroma
dsease.
•
Hemody namc
bu en
bo o d
branc
aor a.
p ons,
Te
s ceross
a
fac tors .
ow :
s
and
roe
o
A eromas
e
os a
a ong
o
e
due
o
o
n
e
o cc ur
vess es ,
p oser or
y p er enson
presumaby
end
ex ng
wa
a
a
o
ses
maj or
e
d e veopmen
emo dy nam c
e e c s
o
u r-
ar er a
ab dom na
o
on
a ero -
end o e-
unc on. 5.
•
Genetcs. Famy sor y s an mporan rsk acor or aeroscero-
ss.
Fama
ypercoeseroema,
an
auosoma
domnan
Smooth
muscle
proliferation,
and
dsease,
other
collagen
ECM Lipid
deposition,
and
mugenc
aso
are
dseases
suc
as
yperenson
and
ype
2
extracellular
dabees,
debris lipid
•
assocaed
w
ncreased
rsk.
Lymphocyte
Collagen
Age. Sympoms rom advanced esons appear n mdde age or aer. Fig.
he
40
ncdence
and
rse
60
w
o
years
eac
myocarda
o
age,
and
successve
narcon
dea
decade.
raes
ncreases
rom
ve-od
scemc
beween
ear
dsease
7.4
events
Summary
of
of
the
atherosclerosis.
morphologic
features
and
main
pathogenic
CHAPTER
A
Diseases
7
of
Blood
Vessels
109
B
Fig.
7.5
Atherosclerotic
denoted
arrow),
by
and
the
a
arrow.
lesion
lesions.
(B)
with
Aorta
(A)
with
overlying
Aorta
with
severe,
mild
diffuse
thrombus
atherosclerosis
complicated
(closed
composed
lesions,
including
of
an
fibrous
plaques,
ulcerated
plaque
one
(open
arrow).
FIBROUS
(smooth
foam
CAP
muscle
cells,
elastin,
cells,
collagen,
neovascularization)
CENTER
debris,
foam
macrophages,
proteoglycans,
NECROTIC
(cell
cells,
lymphocytes,
cholesterol
crystals,
calcium)
MEDIA
Fig.
•
G ender.
Premenopausa
women
are
7.6
reavey
The
structure
proeced
of
an
atheromatous
plaque.
agans e exraceuar marx (remodeng) and rombus organzaon, and
aerosceross
compared
w
age-maced
men,
possby
because oten undergo caccaon, wc can be seen radograpcay.
o
e
beneca
efecs
o
esrogen
and
progeserone
on
pd
proAcue
and
cronc
canges
n
aeromas
can
ave
serous
es. consequences:
•
Cona
ematopoess.
he
perpera
bood
ces
o
over
10%
o
•
Rupture
or
uceraton
exposes
rombogenc
subsances,
nduc-
adus over e age o 70 years w norma bood couns ave cona ng
muaons n genes a are assocaed w varous ypes o myeod
neopasms,
suc
as
acue
myeod
eukema
(see
Caper
9).
•
rombus
Hemorrage,
dyng
w
rom
cona
emaopoess
cardovascuar
ave
dsease,
a
wo-od
possby
eevaed
because
rsk
ese
o
wn
eads
In
descendng
abdomna
order,
aora,
aerosceross
e
coronary
mos
oten
areres,
e
e
nerna
Lesons
a
carod
varous
or
capares
paque
n
e
a-
rupure.
cause
scema
n
formaton
downsream
s
caused
by
organs.
oss
areres,
sages
o
and
e
severy
vesses
oten
o
e
coexs
srucures
Features.
rom
Myocardia
e
o
meda
easc
ayer
infarcion
o
bers
e
and
(ear
vesse
oer
aack),
wa.
cerebra
nvoves
(sroke),
aoric
aneur ysm,
and
peripera
vascuar
dis-
popea
crce
(Fg.
(gangrene
of
exremiies)
are
e
major
cinica
consequences
o
of Ws.
rage
aeromas.
ease areres,
o
expanson
Aneurysm
infarcion nrarena
damage
paque
•
Clncal
e
rapd
Embosm o sma ragmens o aeroma durng paque rupure
supporng
Morphology.
o
•
may
nlammaon
by
7.7).
mua-
ons dysreguae e uncon o macropages and ereby enance
oca
caused
(Fg.
Inderoma,
vduas
ormaon
aeroscerosis.
7.5).
hese compcaons may sem rom sow progresson o aerosceAeromaous paques are we o yeow rased esons w sot pd
roc cores
covered
by
brous
caps
conanng
smoo
musce
ces
• coagen,
assocaed
w
macropage
and
T-ympocye
esons
or
rom
dramac
acue
evens,
as
oows:
and
Ateroscerotc stenoss. Sowy advancng senoss may presen w
nraes
sympoms o scema n ssues supped by e afeced vesses. he and
varabe
degrees
o
neoangogeness
(Fg.
7.6
and
Suppemena
occuson s descrbed as a crtca
stenoss wen bocks 70% o e
umen,
beyond,
eFg. 7.1). Macropages sufed w pd, so-caed oam ces, may be
promnen.
Exraceuar
coesero
s
oten
presen,
requeny
n
because
o
crysane
aggregaes
(coesero
cets).
he
meda
s
pon
and
e
ssue
demand
oten
e
oupaces orm
a
e
bood
suppy.
Presenaons
ncude
angna
pectors,
benea
wc
ypcay
appears
w
exeron
and
rems
w
res;
cronc
e paque may be aenuaed and broc, w smoo musce aropy.
scemc Paques
progressvey
enarge
roug
syness
and
degradaon
eart
dsease,
w
sympoms
reaed
o
ear
aure;
o
ntermttent
caudcaton,
due
o
eg
scema
w
exeron.
and
CHAPTER
Diseases
7
of
Blood
Vessels
109.e1
L
F
C
Supplemental
a
is
central
plaque
ated
and
fibrous
eFig.
necrotic
free
photograph
of
the
cap
C
B
A
7.1
core
(arrow);
a
and
of
core,
of
the
features
containing
the
section
media
Histologic
(C)
lesion
the
therefore
plaque
artery
showing
is
is
of
atheromatous
cholesterol
shown
thinned
scattered
and
other
“eccentric.”
in
(A)
under
In
stained
the
most
inflammatory
plaque
lipids.
this
for
The
the
coronary
lumen
section,
elastin
advanced
cells,
in
(L)
collagen
(black),
plaque
calcification
has
artery.
been
has
(A)
been
demonstrating
(arrow).
(C)
(arrowhead),
Overall
moderately
stained
that
architecture
blue
the
(Masson
internal
and
Higher-magnification
and
demonstrating
compromised.
neovascularization
Note
that
trichrome
external
a
stain).
elastic
photomicrograph
(small
fibrous
segment
arrows).
(B)
the
of
(F)
the
and
wall
Higher-power
laminae
at
cap
are
attenu-
junction
of
the
110
CHAPTER
Diseases
7
of
Blood
Vessels
B
A
Fig.
7.7
died
tion
Atherosclerotic
suddenly.
of
the
plaque
fibrous
rupture.
Correlations
•
Acute
paque
(B)
cange.
Acute
cap,
(B,
and
Acue
plaque
rupture.
coronary
triggering
Reproduced
Basic
paque
Plaque
thrombosis
fatal
from
Principles,
(A)
FJ:
Philadelphia,
canges,
suc
as
without
superimposed
myocardial
Schoen
rupture
infarction.
on
In
both
Interventional
Saunders,
rupure,
superimposed
an
and
1989,
p.
(A)
and
Surgical
an
arrow
in
a
points
Cardiovascular
patient
with
focal
to
the
Pathology:
who
disrup-
site
of
Clinical
61.)
Pathogeness.
he
ces,
oten
ave
serous
consequences.
Supermposed romboss and rapd, compee occuson may ead o
son,
myocarda
here
s
bu
may
narcon
rapdy
and
and
sroke,
reaed
medca
w
emergences
ancoaguans
a
mus
(parcuary
be
an-
wc
a
paee drugs) and romboyc agens or endovascuar sens. Oer
sceross,
mes,
paque
daons
ear,
wou
rupures
ead
narcon,
angna,
wc
o
a
ncreased
cange
may
scema,
marked
srke
even
by
wen
parcuary
ncreasngy
e
paen
s
n
e
severe
a
res.
be
Aneurysms
and
AND
in
the
of
are
blood
caused
vessels
or
by
the
durng
sysoe
are
congenital
or
produces
(nma,
oupoucngs
meda,
a
nvove
a
ree
ayers
o
and
advena)
or
e
aenuaed
wa
o
rena
and
or
may
sem
ransmura
rom
nered
myocarda
arera
surace
and
dssecons
cause
ure—oten
he
ons
w
bood
mos
nvove
puses
sass
deecs,
yperenson,
narcons.
gans
apar
and
enr y
common
aora
and
and
e
Dssecons
o
e
arera
underyng
romboss
caasropc
e
Aortic
and
ayers.
wa
roug
ave
a
Aneur ysms
catastrophic
Aneur ysms
ors:
horacc
ass o cae d
aor c
w
E ers-D an os
syp s
(AAAs)
over
are
e
mporan
are
vascuar
descrbed
enson
are
o
e ac
and
ye ar.
more
60
a
he
are
propensy
aneur ysms
o
wa
and
and
aready
aone
or
exraceuar
seng
e
sage
or
prove
and
dssec-
aorc
e
aneur ysms
aorc
ypcay
burcaon;
ey
occur
can
be
beween
n
sape
and
up
o
15
cm
n
dameer
and
saccuar
25
(Fg.
7.8).
In
mos
cases,
exensve
aerosceross
s
cm
n
presen,
nnng
sac
and
oca
usuay
desrucon
conans
o
band,
e
underyng
amnaed,
meda.
poory
he
organzed
rombus,
wc
can
muc
o
e
daed
segmen.
Clncal Features. Mos AAAs are asympomac un an acue comp-
and
and
n
cond ons.
1%
o ows
o
s
ma es
I
s
and
on
n
and
yp er-
w
AAAs.
are
examnaon
dagnosed
urasound.
and
Acue
may
szed
revea
by
a
pusang
magng
compcaons
o
abdom-
sudes,
AAAs
mos
ncude
e
of
a
brancng
areres)
due
romboss,
spna
cord,
or
vesse
o
(e.g.,
e
expanson,
resung
n
dsa
gasronesna
rena,
ac,
exenson,
and
scema
o
verebra,
oten
e
or
super-
kdneys,
rac
Embosm rom a rupured aeroma or a mura rombus
•
Impngement on adjacent structures (e.g., compresson o a ureer or
•
Rupture no e peronea cavy or reroperonea ssues, eadng
eroson
o
o
verebrae
massve,
oten
by
aa
e
expandng
aneur ysm)
emorrage
Women are ess key o ave AAAs, bu ose a occur n women
an
r upure
Pysca
•
a
ave
Obstructon
egs,
adu s
es mae d
S aes
esons
o c us e d
aneur ysms
abdomna
mposed
n
cardovas c u-
hey
mesenerc
are
as
deveops.
mass.
oowng:
ac-
and
ma r x,
aor c
Une d
es e
r sk
uncommon
ex race u ar
e
prone
•
A eros ceross
n
are
dferen
ab domna
smoke.
and
fatal.
ave
p ar c u ary
ndvdua s
a
abdomen
syndrome,
w ere as
w o
the
e
Mar an
6),
0.5%
ds c usson
and
rup-
caon
rea vey
n
pre dsp osng
1,000,000
b ewe en
vesse
musce
as
acors,
a
nex.
ab domen
dee c s
common,
ye ars
mp or an
approxmaey
AAA
C aper
in
often
and
aneur ysms
syndrome,
muc
occur
which
orax
n er e d
(s e e
age
e
smoo
wc,
hese
aero-
resus.
often
ruptures,
n
scarrng.
and
Aneur ysma
and
oten
most
smoke.
orm.
wen
Aneurysms
aneurysms
e
yperenson
obacco
ey
undersood,
aerosce-
occur
na
Aortic
weakenng
o
once
we
e
mura deec
oss
no
aerosceross,
meda
o
Abdomna
areres
aneur ysm g-pressure
ead
o
o
s
mos
daon.
usorm
w ross,
areas
o
n
AAAs
e
an
eng ear,
w
rsk
oxns
o
a
aora,
acquired
or arer y
may
smokng
eevaed
o
nrarena
expanson
w
efecs
e
heart. e
Aneur ysms
an
o
n
DISSECTIONS
dissections
walls
rae
conrbue
Morphology. defects
o
e
componens,
aneur ysma
ANEURYSMS
as
combnaon,
marx
e
concde
can
urbuence
assocaon
reaed
we
oten
dscussed,
n
enances
srong
as
and
produced
common se o AAAs. hese wa sresses are exacerbaed by yperen-
nlammaory
sress
wave
reeased
rom
wa
pressure
maxma
“unsabe”
ar
(B),
plaque
nrapaque emorrage, or weakenng o e brous cap by proeases
dagnosed
to
thrombus,
atherosclerotic
are
more
key
Aneur ysms
5
o
cm
rupure.
n
he
dameer
rsk
or
or
arger
rupure
are
s
deermned
consdered
g
by
rsk
sze:
and
CHAPTER
requre
surger y.
eecve
gency
Tmey
procedures
surger y
ater
s
ner venon
s
approxmaey
rupure
s
crca:
5%,
rougy
e
wereas
moray
e
rae
rae
or
or
Pathogeness.
emer-
men
50%.
40
cases)
Aortic
and
the
Dissections
dissection
splays
aortic
when
media
arterial
to
form
blood
a
penetrates
blood-lled
intima
yperropy
within
vesse
roug
e
may
produce
advena
and
aa
escapes
emorrage
no
adjacen
e
bood
rup-
wa);
smoo
marx.
ssues.
gans
pa
e
o
eas
ces
e
ear
(see
or
In
aora
canne
cystc
7.8
Abdominal
aortic
ruptured
at
site
is
(A)
External
indicated
by
view
the
of
a
arrow.
large
(B)
with
the
location
of
the
rupture
tract
indicated
by
a
of
layered
the
aneurysm
is
attenuated,
and
the
lumen
is
probe.
filled
by
canges
s
n
ssue
mos
Pa ens
o
aor c
or
Aortic
occurred
arrows)
the
in
lies
a
region
at
dissection.
elastic
dissection.
(identified
layers
the
(B)
are
by
(A)
the
largely
edge
of
a
and
opened
probe)
free
Histologic
black,
An
of
a
large
blood
aorta
with
of
is
red
are
e
narc on
by
emor rage
re ae d
ne ck
w c
proximal
an
or
may
o
o
no
bood
and
e
oss
bood
aong
e
ypc a y
s abbng
md d e
may
pres en
o
e
d s r up
e
be
e
o
e
musce
abnorma
(Suppemena
e
sud den
n
e
sp ac e.
dss e c -
u nc on ,
ar er es,
O er
ons e
aner or
R e rog rade
va ve
c oronar y
p er c ard a
o
dened.
w
b ack.
o
vascuar
Hsoogcay,
b eg nn ng
aor c
or
sac.
umen
a
smoo
seen
s
e
areres
percarda
aorta).
oss
deec
p a n ,
compressng
no
may
specc
oward
creang
n
he
emorrage,
reeners
by
ound
7.9A).
emora
e
ear,
s
(Fg.
accumuaon
marx,
no
and
massve
(doube-barreed
exenson
e
rena ,
b e come
plaque.
this
the
dissection
intramural
The
atherosclerosis
showing
in
a
with
atherosclerotic
area
once
meda
rerograde
o
e
dss e c on
mes ener c ,
ac,
o
or
e
c aus e
or
e ad
comp c a-
g re a
spna
obs r uc e d.
R apd
d ag nos s ,
large,
associated
preparation
o
exraceuar
bu
usuay
vave
ac
nma
caracerzed
e
ro o
e
occurs
ragmenaon,
e ar ng
exend
as
dssecng
meda
orgn
aorc
causes
dsa
e
B
tear
suppy
ar er es
ar er es,
any
The
A
7.9
(see
meda
eadng
e
e
*
intimal
sow
a
unknown,
thrombus.
Fig.
syndrome
meda,
o
connecve
aortic
o wall
e
rad a ng
e
massve
vesses
e
(1)
(>90%
Opened
o view,
In
myo c ard a
aneurysm.
the
a
degeneraton,
Features.
and
ons that
e
excr uc a ng
no
o
sengs:
o
paens
roug
e
can
ar
rupure
amponade
second
wn
as
nsances,
o
aneurysm
Exerna
o
meda
exraceuar
on
Fig.
e
cm
eFg.
ces
B
unnes
proeogycan-rc
o
dseases
sma
earng
markng
10
nsances,
easc
Clncal
A
ear
roug
7.2).
(e
peruson
occasonay
cardac
meda
ces,
wa
wo
Eers-Danos
degenerave
wn
wn
7.9B).
some
e
pane
n
genec
and
n
yperenson
yperensve
nma
nma
aora
dsay,
Fg.
resus
occurs
111
ressance.
ascendng
dssecon
w
agng
and
e
Vessels
aneceden
vasorum
vesse
Morphology. he
e
o
dmns
naes
many
w
syndrome
vasa
may
musce
access
o
o
Blood
paens
aoras
s
Wa
age
Maran
he
of
dssecon
o
younger
as
6).
the
o
dssecon
years
(2)
channel
wall.
Aorc
ures
the
Aorc
60
suc
Caper
occurs
apart
o
and
ssue,
Aortic
Diseases
7
distal
(white
dissection
section,
stained
edge
arrow),
and
with
originating
hematoma.
of
the
which
intramural
Movat
Note
from
that
intramural
arrested
small,
the
oblique
intimal
hematoma
the
hematoma
stain.
a
tear
(black
propagation
(asterisk).
of
Aortic
an yp er ens ve
CHAPTER
7
Diseases
of
Blood
Vessels
A
B
Supplemental
eFig.
Marfan
syndrome,
but
actually
are
layered
pattern
filled
of
7.2
Cystic
showing
with
elastic
medial
elastin
degeneration.
fragmentation
proteoglycans
tissue.
In
both
and
(asterisks).
A
and
B,
(A)
Cross
areas
(B)
elastin
Normal
is
section
devoid
of
media
stained
of
aortic
elastin
for
black.
media
that
from
resemble
comparison,
a
patient
cystic
showing
the
with
spaces
regular
111.e1
112
CHAPTER
erapy,
o
85%
s e c ons
c a y
ave
and
o
or
surg c a
e
a
rep ar
p a ens
do
no
manage d
s ome w a
Diseases
7
w
o
e
nvove
e
Blood
n ma
nvov ng
aor c
c ons er va vey
b eer
aor c
d ss e c on
of
w
arc
e ar
e
c an
Vessels
c an
aor c
be
s ave
65%
Pathogeness.
arc.
Ds -
caon
rep a re d
an yp er ens ve
surg -
dr ugs
and
oucomes.
peuc
w
he
response
arers
key
response,
caracersc
ceran
o
HLA
cass
serods
occurs
as
presumaby
a
o
a
granuomaous
II
apoypes,
suppor
resu
o
angens
a
an
e
mmune
cronc
presen
nlammaon,
and
h1
n
e
an
exceen
eoogy.
Gan
ce–medaed
vesse
wa.
asso-
era-
ce
mmune
he
deny
o ese angens and e bass or e predecon or vesses o e ead
are
unknown.
VASCULITIS
Vasculitis
encompasses
a
group
of
disorders
with
highly
varied Morphology.
pathophysiology
and
clinical
features
that
are
dened
by
the
ds r bu on ence
of
vessel
wall
a ong
e
eng
nl amma on
o
afe c e d
o cc urs
vess es.
a
p acy
Invove d
n
ar er a
inammation. s eg mens
Cnca
Granu omaous
pres
manesaons
depend
on
e
specc
vascuar
bed
exb
no du ar
n ma
ckenng
(and
o cc asona
a romb os es) a mpnge on e umen and c aus e ds a s cem a.
s
afeced
and
somemes
ncude
sgns
and
sympoms
o
sysemc Fu y
nlammaon.
Many
orms
o
vascus
are
recognzed,
some
w overappng
eaures.
Eoog y
s
dverse
and
ncudes
de veop e d
mu nuce ae d
nlammaon,
necons,
drugs
and
cemcas,
and
rauma.
I
s
crca
o
dsngus
necous
njur y
approprae
w
mon
y
or
resrc
or
o
afec
e
our
aer
because
bu
dscusson
greaes
arge
orms
coud
o
paogenc
mmunosuppressve
exacerbae
orms
o
neres,
necous
vascus
sarng
a
w
erapy
Giant
that
Cell
vascus.
are
ose
mos
cell
a
prmar-
principally
he
be
affects
empora,
nvoved.
permanen
Arteritis
arteritis
a
chronic
large-sized
verebra,
Opamc
bndness;
is
and
arteries
opamc
arer y
ereore,
granulomatous
in
nvovemen
promp
the
can
dagnoss
disorder
head.
ar eres
and
e
cause
and
w c
s
oten
s
ass o c ae d
cus
sudden
can
and
reamen
e
are
essena.
among
years
me d a,
o
oder
age.
(ever,
rag mene d
w
and
Sgns
mos
papaon.
Ocuar
range
bopsy,
s
rom
ypcay
pacy,
a
coserod
n ma
adven a
arers
n
and
e
(Fg .
7.10).
dpopa
e
oss)
aong
sympoms
o
o
e
bopsy
or
e
mos
may
ake
7.10
tion.
cells
(B)
Giant
near
Elastic
associated
cell
the
arteritis.
tissue
medial
(A)
fragmented
staining
attenuation
Hematoxylin-and-eosin
internal
elastic
demonstrating
and
scarring.
nnng
does
necross
n
no
acor
oss.
(H&E)–stained
membrane
focal
(arrow),
destruction
of
section
along
the
with
of
a
medial
internal
temporal
and
elastic
artery
adventitial
membrane
showing
and
rare
o
and
wc
s
50%
vas-
beore
pan
panu
o
Dagnoss
e
o
nlamma-
aca
e
are
or
o
paens
requres
arers
dagnoss.
erapes
inflamma-
(arrow)
orm
s
because
excude
(TNF)
o
abou
owever,
I
sysemc
orm
arer y,
vson
arer y ;
resu
relec
abrupy
compee
common
counres.
e
empora
appear
empora
an–umor
s
B
A
giant
e as c
He a ng
bross.
reamens.
Fig.
g ranu omas
ner na
ckenng ,
ger-ncome
sympoms
weg
nense
negave
or
ce
adus
maase,
eadace,
and
aora
o
Clncal Features. Gan
50
(temporal)
on
We
com-
vesses.
(Temporal)
nonne cro zng
s
on
Giant
o
cenere d
rom s c ar r ng
mmune-medaed
ce s
radaon e
exposure,
conss
g an
mmune-memembrane,
daed
esons
w
Cor-
efecve
CHAPTER
Takayasu
Takayasu
Arteritis
arteritis
bu
is
a
arteries
characterized
pulses
the
in
Takayasu
ng
o
e
upper
granulomatous
by
ocular
vasculitis
disturbances
of
large-sized
and
maness
aora—parcuary
Polyarteritis
w
e
ransmura
aorc
arc
scarrng
and
grea
and
cken-
vesses—and
umna narrowng o e major branc vesses. Is eaures overap w
ose
made
years
ce
o
gan
argey
o
age
on
arers
e
beng
arers,
uomaous
ce
bass
e
o
a
Takayasu
dsncon
paen’s
desgnaed
as
arers
T-ce–medaed
age,
avng
appears
mmune
beween
w
ose
Takayasu
o
be
wo
o
enes
younger
arers
caused
response
e
by
an
a
an
Lke
cronc
unknown
Polyarteritis
cular
he
and
usually
50
gan
aora,
akeofs
7.11),
o
e
eadng
rena,
e
grea
o
Inlammaor y
and
aorc
arc,
vesses
upper
o
T
may
exremy
nraes
accumuaons
coronar y
and
s
n
ces
areres,
brances,
be
narrowed
weakness
vesse
and
may
was
and
or
be
gran-
vesse
as
we
range
macropages
afeced.
oberaed
an
carod
rom
o
1
o
vsua
2
or
years
and
are
neuroogc
113
compabe
w
decs.
that
is
a
systemic
commonly
the
vasculitis
involves
of
medium-sized
renal
and
visceral
mus-
vessels
lung.
e
dsease
ore
s
ave
he
cause
responds
beeved
cronc
o
ave
epas
compexes
composed
depos
vesse
n
o
poyarers
o
an
B
was
compexes
o
we
mmunoogc
necon
vra
and
and
angens
provoke
ocaze
nodosa
mmunosuppressve
n
bass.
may
and
an
s
One
ave
unknown,
agens
rd
o
crcuang
specc
areres
paens
mmune
wc
response.
and
bu
ere-
anbodes,
nlammaor y
medum-szed
and
no
n
Wy
oer
as s
unknown.
he
(Fg.
puses.
nonspecc
granuomaous
nlammaon, bo o wc may be assocaed w wa ckenng
and
ater
w
Vessels
Nodosa
spares
Pathogeness.
vesses pumonar y,
abe
nodosa
arteries
mmune
e
quescen
Blood
s
angen.
Morphology.
become
sur vva,
of
weakened
extremities.
arers
oers
ong-erm
Diseases
7
Morphology.
vesses
Fuy
deveoped
necrozng
areres,
bross.
Vesses
rac
are
o
e
esons
w
n
are
nlammaon
oten
kdney,
afeced
o
ear,
ver,
descendng
composed
o
gasronesna
o
requency.
segmena
medum-szed
supermposed
and
order
or,
romboss.
ransmura
occasonay,
Acue
sma
esons
ave
brnod necross o e vesse wa and nrang neurops (Fg.
7.12),
Clncal
Features.
Invovemen
o
e
aorc
arc
and
major
wereas
oder
nlammaon.
produces
reduced
upper-exremy
bood
pressure
and
puse
decs,
vsua
ed
deecs,
and
bndness.
o
nvovemen
o
e
dsa
aora
(eg
are
and
broc
cronc
and
assocaed
esons
w
coexs,
cronc
suggesng
recurren
nlammaor y
damage.
he
vascuar
njur y
may
Sympoms mpar
reaed
Acue
sreng, ongong
neuroogc
esons
brances
caudcaon),
e
e
peruson
o
downsream
ssues,
eadng
o
uceraons,
punarcs, and scemc aropy, or may provoke aneur ysm ormaon
monar y
arer y
(pumonar y
yperenson),
e
ear
(myocarda and
narcon),
appear.
he
and
e
dsease
rena
as
a
areres
varabe
(sysemc
course.
yperenson)
Some
cases
aso
rapdy
e
aendan
rsk
o
emorrage.
may
progress,
Clncal Features. Poyarers nodosa s more common n young adus
bu
can
ong
occur
weg
oss—are
vascuar
o
a
age.
reaed
proean
nvovemen
gasronesna
neurs,
he
cnca
ner vas.
nvovemen
puzzng,
arer y
era
any
sympom-ree
s
o
vared
and
may
esons;
abdomna
dfuse
predomnany
ypcay
and
be
suc
as
and
muscuar
are
epsodc,
boody
aces
moor
and
ner ves.
due
soos
pans;
Rena
and
and
dsrbued,
yperenson
w
ever,
nonspecc,
wdey
pan
afecng
s
sympoms—maase,
nlammaon
manesaons
and
course
Ina
e
eadng
o
rena
caused
and
by
perp-
nvovemen
s a major cause o dea. Unreaed, poyarers nodosa s usuay aa,
A
B
Fig.
7.11
flow
of
Takayasu
contrast
brachiocephalic,
tions
of
strating
circles
is
the
the
carotid,
right
marked
intimal
of
to
intimal
the
(A)
into
and
carotid
correspond
area
arteritis.
material
Aortic
the
arch
great
subclavian
artery
from
thickening
original
arteries
the
and
vessel
hyperplasia.
angiogram
vessels
wall;
the
showing
shown
(B)
in
narrowing.
inner
reduced
narrowing
(arrows).
patient
luminal
and
core
of
Cross
(A)
demon-
The
of
the
sec-
tan
white
tissue
Fig.
7.12
necrosis
vessel
MD,
ical
Polyarteritis
and
thrombotic
(upper-right,
Department
School,
of
Dallas.)
nodosa,
associated
occlusion
arrow)
is
of
a
small
uninvolved.
Pathology,
University
with
artery.
segmental
Note
(Courtesy
of
Texas
that
Sidney
fibrinoid
part
of
the
Murphree,
Southwestern
Med-
114
bu
CHAPTER
w
90%
o
Diseases
7
mmunosuppressve
erapy
of
remsson
Blood
or
cure
s
Vessels
aceved
n
cases.
res—probaby
smoke,
grene.
Kawasaki
Kawasaki
and
Disease
disease
childhood
sized
an
acute,
associated
febrile,
with
an
self-limited
arteritis
of
illness
large-
of
to
Smokng
vascuar
sgncance
sems
rom
requen
nvovemen
o
coro-
oer
on
a
he
seasona
rggers
an
cause
o
varaon
mmune
Kawasak
n
dsease
ncdence,
response
a
s
unknown.
suggesng
njures
a
areres
he
a
dsease
vra
are
he
vascus
aoug
brnod
resembes
necross
a
s
seen
usuay
secondary.
n
no
o
can
a
rem
vascus
nerves.
I
and
e
paen
progress
progresson,
w
smokng
prmary
cytopasmc
vascudes
agans
wo
varous
orms
reerred
o
as
o
over
bu
connues
me
once
o
o
gan-
esabsed,
absnence.
afec
antbody
are
sma
vesses.
Aoug
(1)
by
o
e
presence
neurop
an-proenase-3
dreced
consuen
(ANCA)–assocated
dened
componens
ANCA:
c-ANCA),
granue
agans
PR-3,
(PR3-ANCA);
and
o
granues.
ANCA
a
vascu-
auoan-
neurop
(2)
here
(ormery
azuro-
an–myeoperox-
poyarers dase
nodosa,
no
o
deveop
Vasculitides
orms
hese
bodes
nec-
pc
Morphology.
do
Antneutrop
tdes.
sows
may
er paogeness s ncompeey undersood, wo groups ave emerged:
•
areres.
Pathogeness.
nvovemen
absnence
esons
Small-Vessel
Many
cnca
o
uceraons
infancy
medium-
vessels.
Is
nar y
is
e
due
cronc
as
ANCA
(ormery
reerred
o
enzyme,
myeoperoxdase
as
p-ANCA),
dreced
agans
promnen. a
neurop
ysosoma
(MPO-ANCA).
Afeced vesses ave a dense ransmura nlammaor y nrae a Severa
orms
o
ANCA-assocaed
vascudes
are
recognzed
w
ncudes neurops and mononucear ces. I et unreaed, damage paray
caused
by
e
nlammaon
may
ead
o
aneur ysm
overappng
eaures.
hey
ncude
PR3-ANCA
posve
ormaon. granuomaoss
w
poyangs
and
MPO-ANCA
posve
mcro-
scopc poyangs. Bo are assocaed w gomeruoneprs and
Clncal Features. Kawasak dsease ypcay maness w conjuncva
pumonar y dsease, requeny eadng o emopyss. I s uncear
and ora eryema accompaned by bserng, eryema and edema o e
e
ands
presen
and
ee,
a
desquamave
ras,
and
cervca
ymp
node
enarge-
men. Approxmaey 20% o unreaed paens ave cardovascuar com-
pcaons,
wc
or
mos
may
sudden
noaby
rupure
dea.
(speccay,
or
he
e
deveopmen
rombose,
dsease
nravenous
o
eadng
responds
coronary
o
we
mmunogobun
arery
myocarda
o
aneurysms,
narcon
annlammaory
and
asprn),
wc
ANCAs
n
dagnosc
•
and/
agens
Thromboangiitis
strongly
I
egs,
and
Obliterans
obliterans
associated
prmary
and
with
afecs
oten
o
a
severe
tobacco
sma
produces
ampuaon
is
(Buerger
and
of
vasculitis
that
is
e
ses
scema,
o
uceraons,
e
arms
and
mmune
oberans
smokng
drecy
o
depend
s
oxcy.
mody
Ceran
e
on
uncear.
damages
drec
may
Bo
gangrene
ssues.
exposure
One
e
naon
dea
o
s
vesse
wa
HLA-ypes
obacco
a
endoeum
Aernavey,
a
some
and
more
smoke,
and
o
bu
e
o
vascuar
compound
nduce
suscepbe,
an
romboangs
e
componen
a
reacve
componens
are
progresson
precse
obacco
canges
n
obacco
mmune
conssen
w
roe
o
smoke
are
due
smoke
response.
a
roe
or
he
e
s
w
exampe
wa
n
dfer
In
e
be
vascuar
dependng
compexes.
and
on
e
sysemc
kdney
s
anbodes
ereore
hese
may
deposed
w
njur y
naure
upus
vascudes
o
e
e
o
upus
er ye-
cn-
auoanbodes
afeced
(see
o
mmune
resuan
er yemaosus
severey
are
drecy
par
sysemc
o
deposon
bnd
as
and
are
are
agens.
compemen
Anbodes
or
ese
and
mmunosuppressve
assocaon
o
bu
paens
vascutdes.
njur y.
vesse
dsrbuon
syndrome,
Infectious
Drec
and
vascuar
o
roe,
afeced
and
or
Good-
Caper
11).
and
Vasculitis
vascuar
parcuary
Pathogeness.
Treamen
by
o
ndngs
pasure
areres
o
sma-vesse
ca
smoking.
mdde-szed
severe
afeced
form
paogenc
mmunogobun
compexes,
Disease)
drec
racon
caracerzed
maosus.
Thromboangiitis
vaue.
componens
reduce e ncdence o sympomac coronary arery dsease.
a
g
Immune-compex,
a
sarpy
ave
a
ocazed
arers.
(e.g.,
bacera
may
arse
or
nvason
rysm)
arera
or
can
Vascuar
pneumona
rom
embozaon
weaken
by
Pseudomonas,
necous
nvason
or
was
nduce
o
spread
necve
usuay
and
can
adjacen
emaogenous
rom
agens,
Aspergus,
be
par
romboss
o
and
cause
spp,
a
or
ung,
may
ssue
or,
bacera
endocards.
suiceny
o
abscesses),
o
bacera
Mucor
cause
necon
ess
commony,
durng
sepcema
Vascuar
aneur ysms
necons
(mycotc
can
aneu-
narcon.
or
mmune njury. Ceran enc groups (Israe, Indan subconnen, Jap-
DISORDERS anese)
are
aso
a
greaer
rsk,
ponng
o
one
or
more
genec
Varcose
Morphology.
cronc
Caracerscay,
ransmura
vascus
o
ere
s
medum-
segmena
and
acue
sma-szed
cay
and
vens
reevan
nlammaory
n
e
exremes.
nraes,
wc
may
In
gve
e
rse
eary
o
sages,
mcroabscesses,
Varicose
are
and
adjacen
W
me,
srucures
romb
become
organze
encased
n
and
evenuay
brous
rombopebs
accoun
or
a
eas
90%
o
cn-
dseases.
Veins
e
veins
chronically
wall
no conguous vens and nerves (a eaure rarey seen n oer orms
vascus).
and
venous
mxed
accompaned by umna romboss. he nlammaon oten exends
o
VEINS
areres,
Varicose predomnany
OF
acors.
•
ssue.
abnormally
dilated
intraluminal
tortuous
pressures
veins
and
produced
weakened
by
vessel
support.
Venous
arery
are
increased
daon
can
occur
a
mupe
ses:
Varcose vens o e exremes occur n up o 20% o men and one
rd o women; obesy and pregnancy ncrease e rsk. hey mos
commony
Clncal
Features.
Paens
smokng
sory
more
ans
by
may
presen
exercse,
vascuar
or
o
w
usuay
20
Raynaud
superca
nsuicency
are
an
penomenon,
noduar
ends
o
younger
pack-years.
be
pebs
an
45
and
hromboangs
nsep
(venous
accompaned
by
oo
pan
ave
nduced
nlammaon).
severe
a
ober-
he
pan—even
a
afec
e
superca
vens
o
e
egs.
Varcose
daon
renders e venous vaves ncompeen and eads o ower-exremy
sass,
congeson,
and
secondar y
and
uceraons,
posed
edema,
scemc
necon.
wc
pan,
skn
oten
and
romboss.
canges
ea
may
poory
ead
and
Perssen
o
are
sass
prone
edema
dermas
o
superm-
CHAPTER
•
Esopagea
son
varces
secondar y
obsrucon
agea
or
varces
may
o
ver
epac
are
one
arse
n
crross
ven
o
e
seng
and
(ess
romboss
severa
ypes
o
o
pora
requeny)
(see
Caper
yperen-
pora
13).
porosysemc
•
ven
Esop-
suns
ncude
reca
perumbca
vens
ancu
or
ke
•
e
erm
vens
o
e
vens
(producng
e
because
somemes
aa
wa
magned
ead
sgncan
(emorrods,
o
upper
are
known
resembance
Medusa).
ey
s
descrbed
o
Esopagea
prone
o
as
caput
e
and
are
eadng
e
medusa,
daed
varces
rupure,
gasronesna
beow)
7.13A).
o
w
•
a
on,
juncon.
mos
resu
commony
Hemorrods
and
hey
panu
are
a
rom
massve,
due
source
o
o
pregnancy
beedng
pevc
or
and
sranng
are
prone
o
o
conges-
deecae.
esons
are
romboss
C avernous
deep
of
thrombophlebitis
Oer
ses
ac
venous
we
as
e
were
pexus
arge
veins
and
is
deep
n
n
the
source
venous
maes
vens
accounts
and
e
of
pevc
and
more
most
romb
e
sku
for
may
90%
pulmonary
orm
venous
e
than
dura
are
e
pexus
n
snuses
of
cases
emboli.
(especay
and
n
Kaposi
pesvirus-8
vera;
see
Caper
9)
may
ead
ypercoaguaby
o
pora
ven
(e.g.,
poycyema
romboss.
sarcoma
Vrcow
and
rad:
n
ong
venous
pane
romboss
aby
see
low
(e.g.,
(see
o
e
ncreased
Mae
sex
o
3).
exended
eg
one
or
more
endoea
Caper
(e.g.,
magnancy
3).
reaed
auomobe
(DVT)
Caper
w
sass
or
s
abnormaes,
ypercoaguaby
resus
or
hromboss
bed
res
rps)
ncreases
vens,
as
do
componens
njury
Proonged
n
e
deep
causng
nered
deecs,
suc
and
age
an
years
50
o
as
a
T-ce
and
•
sae,
venous
are
V
sarcoma
uncon.
rsks,
are
C a ss c
Je w s ) .
bu
Leden;
as
assocaed
rsk.
cases,
e
pan
ca
ever,
e
can
be
musces,
sympoms
absence
o
manesaon
preven
be
ncude
or
orced
are
ndngs
DVT
recurren
emporar y
eced
oten
o
or
edema,
by
pressure
dorslexon
absen,
does
s
DVT,
redness,
a
no
over
o
e
especay
excude
pumonar y
ancoaguan
eong,
sweng,
dependng
and
afeced
oo
n
In
reamen
e
vens,
(Homan
many
embosm
on
pan.
bedrdden
DVT.
(see
s
eoog y
In
BLOOD
VESSELS
AND
mas
sze
o
bood
(exremey
surround
monar y
and
common),
nrequeny,
neopasms
vesses
may
bood
arer y,
and
rare,
arse
and
ocay
gy
rom
vesses.
ympacs
e
sgn).
How-
e
Caper
and
cava)
umors
occur
o
rs
3).
wc
Endemc
bu
occur
vscera.
emango-
varees
o
emangomas
n
newborns:
are
o
red
a
peduncu-
beed
resembe
more
arge,
easy
exuberan
nrave,
excson
are
17),
one
requeny
be
hey
requred
componen
wc
bran
vascuar
emangomas,
regress.
may
n
daed
capar y
sponaneousy
neoplasm
known
mos
o
as
o
vascuar
sem,
nvove
may
n
be
some
von
Hp-
esons
rena,
caused
Kaposi
common
KS,
n
based
o d e r
by
are
pancreas,
human
sarcoma
ndvduas
on
men
Eu rop e an
s
her-
herpesvirus
w
popuaon
o
mpared
demograpcs
or
e
usu a y
Me d e r r an e an ,
d e s c e n
susp e c e d
p a qu e s
me
KS
and
s
( e sp e c a y
n
n o
n o du e s ,
e s on s
re m a n
ypcay
can
occurs
n
e
n d v du a s ,
pre s e n .
I
usu a y
m ay
M d d e
As ke n a z
a e c e d
o
e
m an e s s
on
n c re a s e
c on n e d
occurs
oow
n
seng
course
Lesons
bu
a
e
e
and
oten
rsk
AIDS-assocated
o
an
cdren
o
o
KS
n
e
n
ow e r
sze
sk n
HIV-negave
ndoen
oten
and
or
an d
an d
sub -
cdren
aggressve
organ
vruay
n
aways
and
course.
I
w
e
aa.
sod-organ
mmunosuppresson.
nvoves
regress
s
occurs
T-ce
ymp
aenuaon
nodes,
o
ranspan
I
pursues
mucosa,
an
and
mmunosuppres-
rejecon.
(epdemc)
mos
ncdence
vduas
angosarcomas.
Vascuar
era
or
ces
arge
a
vesses
nrequeny
suppor
(aora,
and
are
or
composed
of
recognzed,
ncudng
KS
common
s
an
AIDS-denng
HIV-reaed
ness
magnancy
and
wordwde.
and
w
an
aen
more
erapy,
bu
ncdence
popuaon.
an
KS
a
s
wdey
o
n
popuaons
occurs
1000-od
AIDS-assocaed
dssemnaes
80%
s
vscera
KS
n
an
nvoves
s
w
access
HIV-neced
ger
oten
eary
n
n
e
ymp
nd-
gen-
nodes
course.
pu-
mosy
blood-
ypes
as
anrerovra
measa-
Pathogenes s.
and
e
preerenay
are
Transpantaton-assocated
son,
vessels.
Severa
e
may
compeey.
mucosa
ey
o
and
ssue.
Afrcan
adus
a
tumors
skn,
growng,
ora
w
cerebeum,
n
sk n
e y
a
KS
proeraon
eukn
benign
or
m mu n o d e c e n c y
nu mb e r,
sroma
common
s
W
ve
are
regress
composed
no
e
orms
e x re m e s .
aggressve
may
Hemangiomas
lled
are
m mu n y
T- c e
recpens
To
sarcomas.
Hemangiomas
mos
rapdy
C ompared
do
E aser n
nvovemen,
•
DVT.
bengn
neopasms
endoeum
Prmar y
vena
magnan
as
e
LYMPHATICS
ncude
aggressve
bu
emangomas)
nvove
Mcroscopcay,
vascular
o cc urs
re d - pu r p e
he
Tumors
(Fg.
capares
7.13C).
also
(KS)
A e re d
remans
OF
kdneys
n-waed
n
ora
oten nvoves ymp nodes. A severe orm, w promnen vscera
•
TUMORS
a
Four
or
ov e r
young
squeezng
cases,
e
•
some
paens,
gven,
o
e
recognzed:
KS
c u an e ou s
Clncal Features. DVTs produce ew reabe sgns or sympoms. Loca
manesaons
is
(HHV-8,
E aser n,
ypercoagu-
acor
aso
e
dysuncon,
possurgca
rsk
acors
and
oder
or
o
mmobzaon
e
and
occur
o
[KSHV]).
Kapos
Pathogeness.
o
strawberry
gngva
(Caper
n
speen,
brs),
emangomas
ound
ese
Sarcoma
an
w
200
surgca
dsease
ver,
ype;
membranes
ver.
Kaposi
assocaed
e
115
as
e seng o necon or nlammaon). Peronea necons and cer-
condons
or
7.13D).
Cavernous
commony
perpros-
emaes,
(Fg.
and
common
mucous
composed
rapdy,
emangomas
pe-Lndau
n
manes
skn
desrucve;
mos
and
are
n
emangomas
srucures,
cases.
leg
ssue
as
(1
uceraed.
(Fg.
cavernous
Thrombophlebitis
deep
oten
e
Vessels
7.13B).
grow
e
Blood
(so-caed
common
on
are
ey
(Fg.
hey
of
ssues,
we
granuomas
cannes
uceraon.
of
are
granuaon
•
as
sroma
mupe.
ocay
Thrombosis
ps,
emangomas
P yogenc
and
vascuar
scan
aed
emorrages.
proonged
and
Hsoogcay,
Juvene
be
•
Hemorrods are varcose daons o e venous pexus a e ano-
reca
emangomas
subcuaneous
newborn
snake-
cncay
skn,
caves
a
may appear w pora yperenson; oer common ses o sun-
ng
Capary
e
Diseases
7
ces.
6,
as
sss;
w
hese
we
nerere
absence
as
w
o
me
magnanc y.
s
an
unusua
smuaed
ncude
vra
e
an
and
by
neopasm
acors
vra
acors
uncon
efecve
cona
a
omoogs
a
o
T-ce
o
begns
ce
may
s
as
HHV-8
suc
c yce
suppressors
response,
by
c yoknes
enance
umor
evouon,
key
produced
a
reac-
neced
as
ner-
progresson
suc
as
RB.
proeraon
progress
o
a
In
per-
u-ledged
116
CHAPTER
Diseases
7
of
Blood
Vessels
Pathogeness. Morphology. Cu aneous
esons
progress
roug
ree
(e.g., s ages:
patc,
paque,
and
nodue.
Paces
are
pnk,
red,
or
oowng
comp os ed
o
daed,
r reguar,
and
anguaed
ces.
ass o caed
Paques
daed
w
(Fg.
der ma
an
n rae
7.14A)
vas c uar
are
o
cronc
ee vaed
cannes
ndweng
corde
as
comp os ed
and
sur rounded
spnde
ces.
No duar
esons
are
ncre as ed
numb ers
o
pump,
over y
neopas c
w
s age
oten
nersp ers ed
s-ke
proera ng
spaces
(Fg.
n
e
seng
breas
o
cancer),
ympedema
radaon,
o
oregn
bodes
(e.g.,
srapne).
Hsorcay,
and,
poyv-
been
assocaed
w
angosarcoma
o
e
ver.
spnd e
7.14B).
he
In
e
skn,
angosarcomas
rs
appear
as
sma,
and
demarcaed,
red
nodues.
Advanced
esons
are
arge,
lesy
ces,
red-an oten
or
o
sarpy con an
arse
by
Morphology. pump
can
resecon
nlammaor y
esons
ned
node
bo o d ny
vess es
ymp
pur pe rarey,
mac ues
Angosarcomas
s equen a
o
gray-we
masses
(Fg.
7.15A)
w
-dened
margns
no duar
a bend mpercepby w surroundng srucures. he exen o s
accompaned
by
no da
and
vs cera
nvovemen,
dferenaon par c uary
n
e
A r can
and
AIDS-ass o caed
cannes
wou
Clncal Features. he
ca
and
seng.
Cassc
surgca
w
resecon
s
anrerovra
o
usuay
oten
erapy
KS
argey
mmunosuppresson,
mmunosuppresson
KS,
course
KS
s
vares
adequae
resoraon
s
wdey
resrced
efecve.
generay
s
o
o
accordng
e
surace
reamen.
T-ce
In
or
o
o
KS
uncon
Smary,
s
varabe,
rangng
rom
umors
a
e
e
7.15B)
dscernbe
o
bood
undferenaed
spnde
s
a
magnan
dened
mos
AIDS-assocaed
are
oten
nvove
aggressve
resecon
by
evdence
o
oten
e
umors
s
no
skn,
sot
a
ssue,
nvade
possbe,
and
breas,
ocay
curren
and
and
ver.
5-year
sur vva
30%.
endo-
A
B
C
D
7.13
Hemangiomas.
hemangioma.
and
D,
(C)
Courtesy
Brigham
Medical
and
John
Hemangioma
granuloma
Sexton,
Women’s
School,
(A)
Pyogenic
MD,
Hospital,
Dallas.)
of
Beth
Boston.
of
the
Israel
C,
the
lip.
tongue.
(D)
Hospital,
Courtesy
(B)
Histologic
Boston.
Thomas
Histologic
appearance
appearance
B,
Courtesy
Rogers,
MD,
in
in
cavernous
Christopher
University
of
juvenile
capillary
hemangioma.
D.M.
Texas
Fletcher,
Angosarcomas
measasze.
dferenaon.
Fig.
umors
Clncal Features. Oder adus are more commony afeced, and esons
reducng
beneca.
neopasm
vascuar
vesses.
Angiosarcomas
ea
ce
cn-
assocaed
by
(Fg.
body,
abou
Angosarcoma
orm
var ans.
(A
MD,
Southwestern
Compee
raes
are
ony
CHAPTER
A
7
Diseases
of
Blood
Vessels
B
Fig.
7.14
logic
Kaposi
view
spaces.
of
the
sarcoma.
nodular
(Courtesy
(A)
Characteristic
stage,
Christopher
coalescent
demonstrating
D.M.
Fletcher,
sheets
MD,
with
7.15
and
red-purple
proliferating
Women’s
macules
spindle
Hospital,
and
cells
plaques.
and
(B)
slit-like
Histo-
vascular
Boston.)
B
Angiosarcoma.
dense
plump,
Brigham
A
Fig.
cutaneous
of
clumps
of
(A)
Angiosarcoma
atypical
cells
lining
of
the
distinct
right
ventricle.
vascular
(B)
lumina.
Moderately
differentiated
angiosarcoma
117
8
Heart
O U T L I N E
Congenital
Heart
Malformations
Malformations
Heart
Angina
Chronic
Systemic
s
a
eadng
ease,
n
121
year
125
and
ever y
o
o
Uned
126
126
organ,
more
n
e
may
moray
o
body,
be
beang
an
mporance
dsease
e
s
severe:
wordwde
more
7500
L
an
o
crcuaor y
no
surprsng
accouns
or
m-
a
day.
sysem
Cardovascuar
and
40
bood
genetic
a
or
e
dsease
one
n
s
our
a
o
domnan
ser ve
e
esons
ocus
on
and
e
mos
acqured
common
orms,
and
orms
en
o
ear
ns
our
a
30%
of
all
ds-
Clncal
be
aure.
Congena
ear
genes
o
DISEASE
heart
or
year),
Deecs
as
aso
be
sages
caused
Srucura
(1)
wc
cardac
mpared
o
by
cardac
genec
anomaes
maormaons
causng
(3)
contribute
vessels,
which
to
afec
ranscrpon
deveopmen.
by
ransen
he
acors
uncon
envronmena
deveopmen,
gvng
rse
o
acors.
a
rg-o-le
maormaons
n
congena
causng
sun
causng
a
ear
dsease
e-o-rg
(cyanoc
sun;
congena
can
(2)
ear
obsrucon.
a
permis
bood
o
low
from
e
et
o
e
rig
side
of
congenital
account
for
ear
(or
vice
versa)
20%
Le-o-rg
suns
ncrease
bood
low
no
e
pumonar y
cr-
defects.
dsease
afecs
neary
1%
o
brs
(rougy
and
w
a
ger
ncdence
n
premaure
nans
compabe
w
ve
br
usuay
nvove
ony
expose
e
ow-pressure,
ow-ressance
pumonar y
40,000
and
o
ncreased
pressures
and
voumes,
resung
n
rg
svenrcuar
borns.
may
eary
o
o
A shunt is an abnorma communicaion beween cambers or bood
factors
great
and
crcuaon per
some
reguaors”
ose
Features.
caegorzed
cuaon
nans
muaons,
crca
maormaons
environmental
the
birth
136
136
“maser
smar
ds-
• to
as
same
sresses
e of
135
Failure,
Saes.
we
HEART
and
abnormalities
134
Mos snge-gene deecs a dsrup cardac deveopmen are auo-
soma
vesses Both
Disease,
135
Failure,
Heart
Tumors,
dseases);
CONGENITAL
Myocardial
Failure,
127
resen
e
of
Heart
Right-Sided
132
133
133
Heart
Left-Sided
Disease,
Cardiac
pumpng
congena
ear
Disease,
Heart
126
organ
ear
Heart
131
131
Cardiomyopathy,
Causes
Congestive
Hypertensive
Endocarditis,
Cardiomyopathy,
Myocarditis,
126
Disease,
and
Cardiomyopathy,
Restrictive
Hypertensive
128
130
Thrombotic
Hypertrophic
Disease,
Valve
caper,
w
Dilated
Disease,
Disease,
Cardiomyopathies and Myocarditis, 131
121
Heart
Disease,
Valvular
Endocarditis,
Nonbacterial
120
121
(Pulmonary)
o
ncudng
cusson
to
Infective
Other
cause
e
s
120
workoad
uncon
In
Shunts,
remarkaby
per
consequences
deas
Right-to-Left
Obstruction,
(Left-Sided)
s
mes
Gven
with
Leading
Heart
Heart
ear
Associated
Disease,
Degenerative
on
119
Infarction,
Right-Sided
he
Shunts,
125
Hypertensive
Valvular
Left-to-Right
Ischemic
Arrhythmia,
Rheumatic
with
Pectoris,
Myocardial
e
118
Associated
Ischemic
e
Disease,
Malformations
yperropy
and,
evenuay,
rg-sded
ear
aure
snge (cor
pulmonale).
ead
o
W
me,
ncreased
pumonar y
ressance
may
cambers or regons o e ear. Tweve enes accoun or 85% o cases
o
congena
ear
dsease;
er
requences
are
sown
n T abe
menger
• Pathogeness.
Congena
ear
dsease
usuay
arses
rom
W
durng
gesaona
weeks
3
roug
8,
wen
cases.
srucures
Known
deveop.
eoogc
he
acors
cause
ncude
s
unknown
acqured
n
amos
condons
rubea
necon,
eraogen
exposure,
maerna
and
ae-onse
cyanoss
(Esen-
because
suns,
dabees,
e
a
dusky
pumonar y
bueness
crcuaon
o
s
e
skn
bypassed
(cyanoss)
and
bood
eners
e
sysemc
poory
crcuaon.
90%
suc
S ome congenal anomales obsruc vascuar low, by narrowng e
as vaves,
or
major
bood
vesses.
A
maormaon
and erzed
genec acors suc as rsomes 13, 15, 18, and 21 and T urner syndrome.
118
et)
car-
cambers, congena
o
auy
major
• o
(rg
syndrome).
oxygenaed dovascuar
reversa
rg-o-le
resus embryogeness
sun
8.1
by
compee
obsrucon
s
caed
an
aresa.
carac-
CHAPTER
Table
8.1
Frequency
of
Congenital
Heart
8
119
Cardiac
a
Malformations Ao
Incidence
Malformation
Live
per
1
LA
Million
Births
Percentage PT
Ventricular
Atrial
septal
septal
Pulmonary
defect
42
4482
defect
10
1043
stenosis
LA
8
836
RA
Patent
ductus
arteriosus
7
781
L V RV Tetralogy
of
Fallot
Coarctation
of
aorta
Atrioventricular
5
577
5
492
septal
A
4
396
defect
Aortic
stenosis
Transposition
great
ASD
4
388
of
4
388
Ao arteries Ao
Truncus
arteriosus
1
136
PT Total
anomalous
pulmo-
1
120
PT nary
venous
connec-
LA
LA
tion
Tricuspid
atresia
RA
1
118
RA
L V TOTAL
9757
L V RV
Malformations
Let-o-rg
Associated
suns
are
with
assocaed
Left-to-Right
w
ara
sepa
Shunts
deecs,
RV
B
C
venrcVSD
uar
sepa
deecs,
and
paen
ducus
arerosus
and
are
e
Fig.
common
ype
o
congena
cardac
maormaon
(Fg.
8.1).
8.1
deecs
ypcay
ncrease
ony
rg
venrcuar
and
oulow
voumes,
wereas
venrcuar
sepa
deecs
and
arerosus
cause
ncreases
n
pumonar y
bood
low
and
o
e
Cyanoss
sun
rreparabe
repared
due
s
o
an
eary
pumonar y
cardac
beore
no
eaure
reversa
ese
yperenson
dysuncon
sun
o
hus,
occurs,
deecs,
can
cause
et-o-rg
usuay
w
bu
direction
septal
left
Septal
Aria
sepa
Defects
defecs
and
and
Patent
paen
Foramen
foramen
are
right
common
congenia cardiac anomaies diagnosed in adus.
Durng
and
et
cardac
ara
by
deveopmen,
e
foramen
paency
ovae,
s
wc
aer
cosed
beween
by
on
are
a
e
ssue
rg
laps.
sepa
In
w
low
sneezng
o
bood
embous
(e.g.,
or
sranng
pus
paens
rom
deep
rg-o-et
durng
a
eg
rsk
bowe
or
vens)
a
a
bood
low,
movemens.
paradoxca
eners
e
as
Suc
may
rg-o-et
embosm:
arera
occur
a
venous
crcuaon
o
Atrial
(C)
Patent
ventricle;
w
ormed
rom
grows
e
sunng
ear
s
e
septal
ductus
PT,
defect
( arrows
(ASD).
arteriosus
pulmonary
oer
by
ear
downward
poron
deecs
cdood.
transent
(A)
(B)
indi-
Ventric-
(PDA).
trunk;
RA,
Ao,
right
aorta;
atrium;
s
e
cardac
e
uson
apex
o
and
mee
se
o
a
maormaons.
o
a
muscuar
nner
ven-
a
membranous
par-
(Suppemena
approxmaey
he
rdge
eFg.
70%
o
8.1).
he
venrcuar
deecs.
Sma
foramen
aow
left
assocaed
upward
wa
may
(VSD).
L V,
sepum
80% o peope, ese sepa evenuay use. In e remanng cases, a patent
ovae
defect
membranous
mananed
s
flow).
ventricle.
Mos
grows
mos
blood
be
surger y.
e
shunts
and
mus
Ovale
ovae
of
atrium;
rcuar
Atrial
left-to-right
reversa
c yanoss
suns
of
bood RV,
pressure.
causes
paen LA,
ducus
congenital
pumoular
nar y
Common
Ara cate
sepa
PDA
mos
may
sepum
Larger
be
may
deecs,
compcaed
aure.
asympomac,
cose
Eary
by
surgca
and
deecs
sponaneousy
owever,
resu
pumonar y
correcon
durng
n
n
cronc
yperenson
s
e
mperave
muscuar
nancy
and
or
or
eary
et-o-rg
congesve
suc
esons.
va
Patent
Ductus
Arteriosus
an ara deec due o ncreased rg-sded ara pressures. hs may gve
rse o sroke due o odgng o paradoxca embo n vesses o e cenra
he
nervous sysem. In conras, an ara sepa deec s a xed openng n e
arer y
ara sepum a aows unresrced bood low rom et o rg arum.
Ara
sepa
deecs
wen
ong-sandng
oads
may
reversa.
cronc
evenuay
hese
usuay
asympomac
rg-sded
produce
compcaons
are
do
voume
pumonar y
no
occur
un
and
pressure
yperenson
w
paen
aduood,
and
oramen
over-
sun
ovae.
ducus
I
a
arses
o
e
perms
e
Septal
Defecs
in
are
mos
e
mos
cose
e
Defects
venricuar
common
o
sepum
congenia
sponaneousy
and
do
aow
et-o-rig
cardiac
no
come
anomaies
o
cinica
suning
a
bir,
aenion
and
bu
aora
rom
orgn
bood
e
o
consrcs
ssen
paen
suns)
cases
are
o
ungs.
E
2
e
n
1
arer y
o
2
vascuar
e
days
paogeness.
o
o
e
e
e
and
(e.g.,
gene
jus
ducus
causes
deecs,
o
nor-
oxygen-
decnng
due
ds-
e,
bypassng
arera
Known
ypoxa
aora
aora,
br,
ressance,
domnan
pumonar y
nrauerne
ncreased
pacena.
ncude
auosoma
jons
Durng
arer y
o
bewe en
bir
and
arer y.
response
rom
ink
ater
pumonar y
arerosus
ceran
coses
Wn
coses
derved
unceran
connecing
subcavan
pumonar y
ducus
and
a
pumonar y
et
rom
and
decreased
is
normay
et
e
low
prosagandn
et
a
unoxygenaed
may
aon,
Ventricular
and
areriosus
eves
o
per-
rg
bu
90%
o
o
CHAPTER
Supplemental
William
D.
eFig.
Edwards,
8.1
MD,
A
ventricular
Mayo
Clinic,
septal
defect
Rochester,
(membranous
Minnesota.)
type),
denoted
by
the
arrow.
8
Heart
(Courtesy
119.e1
120
CHAPTER
Sma
duca
suns
Heart
8
generay
cause
no
sympoms,
bu
arger Morphology.
deecs
evenuay
ead
o
sun
reversa,
cyanoss,
and
ear
T eraogy
dspacemen Paen
ducus
arerosus
creaes
a
g-pressure
et-o-rg
o
Fao
resus
rom
anerosuperor
aure.
sun
o
e
muscuar
sepum
a
separaes
e
pumonar y
a runk and e aorc roo (Fg. 8.2A). he ear s enarged and boo-
produces
a
ars,
“macner y-ke”
murmur.
Isoaed
paen
ducus saped
due
o
rg
venrcuar
yperropy ;
e
proxma
aora
s
requres surgca ner venon as eary n e as possbe o preven ese daed;
and
e
pumonar y
runk
s
ypopasc.
he
venrcuar
compcaons. sepa
deec
usuay
s
arge
and
s
overrdden
by
e
aorc
vave,
wc receves mos o e oupu rom bo venrces. Obsrucon
Malformations
Associated
with
Right-to-Left
Shunts
o
rg
venrcuar
oulow
may
be
due
o
narrowng
jus
beow
e
Cardac maormaons resung n rg-o-et suns gve rse o cyapumonar y noss
due
o
admxure
o
venous
bood
w
e
arera
mos
common
condons
assocaed
w
cyanoc
ses
dsease
(Fg.
are
eraog y
o
Fao
and
ransposon
o
or
pumonar y
vave
senoss
In
suc
cases,
a
paen
ducus
arerosus
or
daed
or
bronca
e
grea
provde
e
ony
roue
or
bood
o
reac
e
ungs.
ves-
8.2).
Cln cal
Tetralogy
of
Fallot
o
Feature s.
pu monar y
T eraog y of Fao is e mos common cause of c yanoic congenia
obs r uc on
ear
and
disease
he
common)
congena areres
ear
(mos
crcuaon. aresa.
he
vave
(⁓5%
eraog y
of
congenia
consss
o
e
cardiac
oowng
maformaions)
our
abnormaes:
pu monc
Venrcuar sepa deec
I
•
O verrdng o e venrcuar sepa deec by e aora
s o ae d
•
Rg venrcuar oulow rac obsrucon (subpumonc senoss)
e
•
Rg venrcuar yperropy
pu monar y
e
r g .
ds e as e
are
s e en,
s
as
emb o za on .
compc ae d
c aus e
e
e
e
r sk
C ompee
pu monar y
res
o
e
( due
surg c a
s
g rows.
o c c urs
rom
e ar
R g -o -
end o c ard s
rep a r
s
an
rom
c yano c
yp ox a).
ne c ve
a res a
e ar
proe c on
o
o
sun ng
ma or me d
res embes
sun ng
prov des
deg re e
pu mon c
e
cond on
s e qu e ae
or
e
r g -o -e
b e c aus e
o er
on
c as es ,
b e c aus e
as
p oyc y em a
ncre as es
mos
me
senoss
bu
d ep ends
In
m d,
d ee c ,
pu mon c
suc
a s o
o
w
exp and
s ep a
Te
sun ng
more
no
yp er ens on ,
p aradoxc a
s
enoug
obs r uc on
ven r c u ar
s e ver y
obs r uc on .
wors ens
do es
pu monc
o
cnc a
s e vere
w c
or ce
•
e
s
c yanoss,
Te
ou ow
and
p oss be
bu
pres en.
Ao
Transposition
of
the
Great
Vessels
PT
In
ransposiion
of
e
grea
vesses,
e
aora
arises
from
e
rig
venrice and e pumonary arery emanaes from e et venrice.
LA
I
s
ncompabe
w
posnaa
e
uness
a
sun
exss
a
dev-
RA
ers
oxygenaed
bood
o
e
aora
suc
as
a
venrcuar
sepa
deec
(one
rd o cases) (Fg. 8.2B; Suppemena eFg. 8.2). In ese cases, e rg
L V
venrce
s
sysemc
crcuaon,
yperroped
because
s
e
pump
or
e
g-pressure
RV
and
e
et
venrce
s
ypopasc
because
pro-
vdes bood o e ow-pressure pumonary crcuaon. In oer nsances,
suns are provded by a paen oramen ovae or ducus arerosus; ese
end
o
cose
soon
nervenon. Classic
A
tetralogy
of
he
ater
br,
domnan
and
suc
eaure
s
nans
requre
cyanoss.
emergen
Improved
surgca
surgca
ec-
Fallot
nques now perm repar, and paens oten survve no aduood.
Malformations
Leading
to
Obstruction
Ao Ao
Congena
vaves,
aer
PT
a
obsrucons
e
mos
eve
o
o
e
commony
bood
vaves,
nvove
low
or
e
can
occur
dsay
aora
and
proxma
wn
mer
a
a
o
grea
bre
e
ear
vesse.
he
dscusson.
PT
LA
Aortic
LA
RA
Coarctation
Coarcaon
RA
o
L V
L V
RV
as
emaes.
oer
here
•
are
An
c
VSD
Without
wo
B
Common
disease).
flow).
septal
(B)
(A)
congenital
T etralogy
T ransposition
defect.
Ao,
Complete
of
aorta;
of
RA,
right
may
the
LA,
right-to-left
great
left
vessels
atrium;
L V ,
dsa
shunts
(arrow
(cyanotic
indicates
with
left
and
atrium;
RV ,
right
ventricle;
VSD,
wc
o
dsease.
be
form
e
a
o
e
Maes
soary
mos
coarcaon
eaurng
beween
arerosus
without
ventricle;
PT ,
low,
congenital
direction
of
blood
ventricular
o
•
ventricular
e
aora.
and
e
An
s
e
(reerred
man
he
aora
are
s
a
common
afeced
deec
o
common
(Fg.
s
or
a
may
wce
be
as
orm
oten
as
bcuspd
assocaed
aorc
vave.
8.3):
crcumerena
et
“adut”
source
o
pumonar y
because
narrowed
subcavan
preduca).
narrowng
arer y
In
s
and
a
o
e
paen
aor-
duc-
e
rg
segmen,
form
(unoxygenaed)
crcumsance,
runk
sde
e
conssng
o
s
e
rg
o
daed
ear
due
o
devered
s
o
ncreased
peruses
venrce
rdge-ke
bood
e
e
e
bood
body
dsa
yperroped.
nodng
o
e
aora
pulmonary
adjacen
trunk;
consrcon)
ear
VSD
transposition
Fallot
o
orms
“nfante”
ducus
8.2
Coarcaon
deecs,
segmen
us With
heart
or
congena
RV
w
Fig.
(narrowng,
obsrucve
septal
o
e
gamenum
arerosum,
a
remnan
o
e
ducus
defect.
arerosus
(reerred
o
as
posduca)
(Fg.
8.4).
Proxma
o
e
CHAPTER
Supplemental
Rochester,
eFig.
8.2
Minnesota.)
Transposition
of
the
great
vessels.
(Courtesy
William
D.
Edwards,
MD,
8
Mayo
Heart
Clinic,
120.e1
CHAPTER
ISCHEMIC
Ao
Ao
Ischemic
HEART
heart
Heart
8
121
DISEASE
disease
encompasses
several
related
syndromes
caused by insufcient delivery of oxygen and nutrients to meet myo
PT
cardial
demand.
PT
I LA
s
mos
oten
due
o
coronar y
arer y
dsease,
e
ce
cause
o
LA
moray
RA
n
e
Uned
Saes
and
oer
g
ncome
naons.
Encour-
RA
agngy,
as
moray
decned
by
reaed
50%
o
scemc
snce
1963.
ear
hs
dsease
n
e
mprovemen
s
Uned
argey
Saes
due
o
L V L V
RV
ner venons
RV
a
ave
reduced
coronar y
arer y
aerosceross,
ncudng smokng cessaon programs, beer reamens or yperen-
son
With
PDA
Without
Coarctation
of
and
dabees,
advances
suc
coronar y
care
8.3
Coarctation
of
the
aorta
with
or
preductal
form)
a
patent
left
indicates
ductus
arteriosus
ventricle;
direction
PT,
of
pulmonary
blood
(PDA)
flow.
trunk;
RA,
uns,
o
coesero-owerng
efecve
arryma
angopasy,
and
drugs.
conro,
endovascuar
herapeuc
mprovemens
senng
ave
n
aso
(“adult”
Ao,
or
right
aorta;
postductal
LA,
atrium;
left
RV,
reduced
a
arge
bood
majory
low
o
caused
cases,
by
scemc
ear
aerosceross
dsease
o
e
sems
coronar y
form);
atrium;
right
In
and
areres, arrow
use
aorta
(“infantile”
rom without
and
more
conrbued.
PDA
Pathogeness. Fig.
as
oten
reerred
o
smpy
as
coronar y
arer y
dsease.
Aero-
coronar y
areres,
L V,
ventricle.
sceross
(see
sngy
n
or
Angina
Angina
any
can
afec
any
o
e
man
Pectoris
hree
varans
angna
cuar
is
intermittent
chest
pain
caused
by
reversible
ischemia.
Stabe
s
7)
combnaon.
pectoris
myocardial
•
Caper
eves
usuay
are
s
o
recognzed.
predcabe
exeron
assocaed
epsodc
or
w
ces
ncreased
sabe
pan
demand
assocaed
(e.g.,
aerosceroc
w
par-
acycarda).
paques
a
I
narrow
e umen o a coronary arery by 70% or more (crtca stenoss). he
pan
o
a
•
s
e
a
crusng
et
arm
vasodaor
Prnzmeta
onar y
o
or
squeezng
e
a
or
arer y
responds
or
et
jaw
ncreases
varant
spasm,
subserna
I
s
coronary
angna
vasodaors
suc
near
as
by
res
a
or
by
may
radae
nrogycern,
peruson.
occurs
ypcay
sensaon
reeved
a
res
and
s
aerosceroc
nrogycern
and
caused
by
paques.
cacum
cor-
I
aso
canne
bockers. Fig.
8.4
Coarctation
of
the
aorta,
postductal
type.
The
coarctation
is
a
• segmental
narrowing
of
the
aorta
(arrow).
Such
lesions
typically
Unstabe angna (crescendo angna) s caracerzed by ncreasngy
mani-
requen fest
later
in
life
than
preductal
coarctations.
The
dilated
ascending
even and
major
branch
vessels
are
to
the
left
of
the
coarctation.
The
lateral
ogy,
are
perfused
channels.
University
e
et
(Courtesy
of
coarcaon,
predominantly
Texas
e
s
Sid
arc
way
Murphree,
Southwestern
aorc
venrce
of
by
and
MD,
Medical
s
of
branc
dilated,
tortuous
Department
School,
vesses
of
coronar y
paque
Pathol-
be
daed
and
Features.
narrowng
•
Preducta
e
w
on,
•
and
e
hese
coarctaton
cyanoss
mos
depend
paency
n
afeced
o
wt
e
e
a
on
nans
e
ducus
patent
ower
do
a
no
a
poson
severy
o
rupure
Myocardial
e
and
sur vve
usuay
body.
e
presens
Wou
neonaa
eary
n
ner ven-
ncdence
e
ross.
presence
Men
gender
gap
are
aerosceroic
deveops
assocaed
roug
ncreased
bood
“nocng”
o
e
low
e
w
caudcaon.
nercosa
and
rbs
on
and
daon
o
radoogc
ypoenson
Coaera
nerna
ese
vesses
sudes.
e
ower
crcuaon
oten
mammary
can
n
areres,
produce
T reamen
progressvey
w
ess
severe
exeron
or
narrowng
o
>
90%
o
e
vesse
umen)
o
or
by
romboss.
Unsabe
angna
can
narcon.
is
necrosis
of
the
heart
muscle
resulting
o
o
myocarda
ncreasng
narcon
numbers
sgncany
w
rses
o
more
rsk
oten
progressvey
acors
an
or
w
age
aerosce-
women,
bu
s
age.
perod.
s
exremes
by
assocaed
supermposed
myocarda
afeced
romboic
reave
and
o
narrows
Pathogeness.
and
be
Infarction
eary n e and may reman unrecognzed no aduood. here oten
yperenson
may
(obsrucon
infarction
Postducta coarctaton wtout a patent ductus usuay s asympomac
upper-exremy
precpaed
I
ischemia.
he
e
arerosus:
ductus
o
and
s
res.
arer y
arbnger
Myocardial
yperroped.
from
Clncal
a
a
col-
Dallas.)
are
occurs
lower
a extremities
pan
aorta
w
and
vsbe
baoon
daon or surgca resecon generay yeds exceen oucomes.
he
Mos
paque
nang
ypcay
myocardia
obsrucion
sudden.
of
(Fig.
paque
a
infarcions
coronar y
due
caused
o
by
a
o
conan
myocarda
arge
narcon
pd-rc
cores
or
an
no
e
occusve
paque
can
rombus
of
an
(MI)
or
n overyng brous caps are parcuary vunerabe o rupure
orrage
acue
rupure
8.5).
dsrupon
Paques
are
arer y
cause
can
rapd
orm
paque
because
expanson
o
exposure
and
o
s
ave
Hem-
rupure,
coagen,
122
CHAPTER
Heart
8
and
Adventitia
Media
e
duraon
cardum,
and
o
e
e
occuson,
exsence
o
e
meaboc
coaera
demands
vesses.
Mos
o
e
narcs
myo-
nvove
Intima
e
et
ower
NORMAL
uson
An
venrce,
bood
durng
narc
bo
usuay
ner venon
e
because
pressure
narc
e
(and
dasoe
aceves
wn
wn
s
rg
us
and
s
crca
“error y
e
poson
(due
exen
wndow
a
s
reavey
meaboc
sysoe
u
e
venrce
ower
o
ower
wn
o
3
me
proeced
demands)
o
can
wa
6
and
by
per-
pressures).
ours.
essen
Cnca
e
sze
o
rsk. ”
Atherosclerosis
Dependng
on
and
degree
o
coronar y
arer y
obsruc-
Adventitia
on,
wo
paerns
o
narcon
are
seen:
Media
•
Transmura
nfarcts
ckness
e
resu
n
e
dea
o
myocyes
across
e
u
Intima
FIXED
CORONARY
o
myocardum,
excep
or
a
n
ayer
o
subendocar-
OBSTRUCTION
da
Lipids (Typical
myocyes
a
receve
er
oxygen
and
nuren
suppy
drecy
angina)
rom
Atherosclerotic
bood
n
e
venrces.
hese
narcs
are
generay
caused
by
plaque
compee
narcs
obsrucon
usuay
(ECGs),
ey
o
an
produce
are
aso
epcarda
eevaed
caed
ST
coronary
segmens
ST-segmen
vesse.
n
Because
suc
eecrocardograms
eevaed
MI
(STEMI).
Platelet
•
Endocarda
nfarcts
resu
n
e
dea
o
myocyes
n
e
nner
aggregate
poron
o
e
myocardum.
hs
ype
o
narc
may
be
caused
by
obsrucon o more dsa coronar y vesses or by severe, bu ncom-
pee,
obsrucons.
because
s
n
e
he
aer
dsa
may
preerenay
dsrbuon
o
e
k
endocardum
coronar y
areres
and
Healing
aso
er y
o
are PLAQUE
DISRUPTION
SEVERE
FIXED
s
exposed
bood.
caed
o
On
g
e
venrcuar
bass
o
non-ST-segmen
pressures,
common
eevaed
ECG
MI
wc
mpede
ndngs,
ese
dev-
narcs
(NSTEMI).
CORONARY
Myocarda
scema
aso
dsurbs
eecrca
conducance
n
e
OBSTRUCTION
(Chronic
ischemic
heart
disease)
ear,
ncreasng
e
rsk
o
arrymas.
Indeed,
aoug
myocarda
scema and narcon can resu n dea due o pump aure, n 80%
o
Thrombus
90%
o
cases
dea
ea
da
he
narcon
caracersc
necross;
(2)
Myocarda MURAL
WITH
THROMBUS
OCCLUSIVE
VARIABLE
THROMBUS
OBSTRUCTION/?
(Unstable
EMBOLI
angina,
or
(Acute
acute
transmural
infarction
or
myocardial
sudden
or
by
venrcuar
braon,
a
parcuary
acue
and
narcs
o
exposng
myocardum
o
cronc
an
more
o
age
appearance
e
morpoogc
en
ess
narcs
mcroscopc
e
12
va
3
canges:
od
ours
sans
(Fg.
a
can
8.7).
a
gy
coaguave
and
(3)
are
be
myocar-
s
(1)
usuay
od
o
here
nlammaon;
ours
an
njur y.
bross.
no
grossy
vsuazed
by
Mcroscopcay,
death)
eaures
o
coaguave
necross
become
deecabe
wn
myocardial
sudden
o
12
usuay
by CORONARY
o
narcon
(Fg.
8.8).
By
12
o
24
ours,
an
narc
sequential
can
rapped
be
grossy
bood.
dened
Necroc
by
red-bue
myocardum
dscooraon
ecs
acue
caused
nlammaon
SYNDROMES
(wc of
ours
death)
ACUTE
Diagram
and
on
sequence
bu
4 infarction
gross
depends
apparen,
ypca subendocardial
8.5
caused
arryma.
Morphology.
Fig.
s
Thrombus
progression
of
coronary
artery
ypcay
peaks
1
o
3
days
ater
narcon)
oowed
by
an
lesions
nlux o macropages, wc remove necroc myocyes and neuroleading
to
various
acute
coronary
syndromes.
(Modified
and
redrawn
p ragmens, and s mos pronounced 5 o 10 days ater narcon. from
Schoen
clinical
p.
FJ:
Interventional
correlations
and
basic
and
surgical
principles,
cardiovascular
Philadelphia,
pathology:
Saunders,
1989,
Durng
as
63.)
sot,
gy
on von
Webrand
and
aggregaon
acor,
and
ssue
acvaon
acor,
o
eadng
coaguaon
o
paee
acors
(see
are
cenra
o
rombus
ormaon
n
e
g
narcs
areas
o
become
a
by
granuaon
nlammaor y
ces
10
progressvey
o
14
ssue.
and
days
Heang
ngrow
o
beer
become
deneaed
rmmed
requres
new
e
vesses
by
mgra-
rom
e
adeson
Fg.
sear
margns,
and
arge
narcs
ake
onger
o
ea
an
sma
8.5).
ones. Paees
me,
vascuarzed
narc and
s
yeow-an
Evenuay,
over
a
perod
o
weeks,
brous
scar
repaces
e
sress
narced
ssue.
envronmen n areres. hereore, anpaee agens (e.g., asprn) are
useu
n
bo
Wn
n
e
o
40
orm
prevenon
o
myocardum,
meaboes
wn
e
seconds
a
(e.g.,
mnue
mnues
o
dsrbuon
so
causes
coaguave
morpoogc
adenosne
acc
or
e
acd)
o
e
reamen
o
a
accumuae.
onse
(see
o
vesse
myocarda
aerobc
rpospae
eves
Loss
o
scema.
damage
and
Caper
1).
myocarda
nvoved
o
obsrucon,
rreversbe
necross
eaures
o
and
vascuar
narc
(Fg.
8.6),
a,
and
myoc ye
dea
rae
on
o
occurs
asng
ocaon,
depend
ceases
noxous
conracy
Iscema
he
e
narcon.
gycoyss
n
sze,
e
sze
20
e
Clncal
severe,
neck,
jaw,
assocaed
In
a
ac.
Suc
and
dabecs
pan).
e
pan
s
o
o
or
et
paens,
narcs
myocarda
ces
perssen
“sen”
(due
cassc
subserna
epgasrum,
mnory
and
deveopmen
Features.
crusng
pan
arm.
and
s
or
In
no
conras
reeved
myocarda
are
auonomc
narcon
pressure
reavey
o
by
neuropaes
a
s
eraded
radaes
angna
may
n
e
pecors,
e
be
oder
bun
e
by
o
nrogycern
narcon
common
a
or
res.
asympom-
paens
and
percepon
o
CHAPTER
TRANSMURAL
INFARCTS
Heart
8
NON-TRANSMURAL
Restoration
of
flow
123
INFARCTS
(reperfusion)
Per manent T ransient/par tial occlusion
of obstruction
left
anterior regional
descending subendocardial branch infarct
Posterior
Per manent
occlusion
left
Global
of
hypotension
RV
circumflex
L V circumferential
branch
subendocardial
infarct
Anterior
Per manent
occlusion
the
of
Small
posterior
intramural
descending
branch
right
of
vessel
the
occlusions
coronar y
microinfarcts
ar ter y
Fig.
8.6
Dependence
Patterns
involved
from
dle),
of
with
partial
or
of
transmural
occlusion
or
of
transient
occlusion
of
myocardial
infarction
the
right
occlusion
small
infarction
resulting
main
(top),
on
from
coronary
global
intramyocardial
the
major
location
artery
(not
hypotension
vessels
and
coronary
nature
artery
of
the
diminished
occlusion.
depicted).
Right,
superimposed
on
The
right
Patterns
fixed
of
perfusion.
ventricle
infarction
three-vessel
Left,
may
be
resulting
disease
(mid-
(bottom).
and
s
ocaon
n
e
ear.
Serum
eves
o
proens
a
eak
rom
njured myocarda ces are useu n dagnoss. Cardac roponns T and
I
ave
g
More
acue
even,
oowng
•
speccy
an
90%
bu
and
o
sensvy
paens
neary
ree
compcaons
(Fg.
or
wo
myocarda
make
ours
o
a
damage
ospa
experence
one
or
(Fg.
8.9).
sur vve
more
o
e
e
8.10):
Contracte dysfuncton. Inarcs mpar et venrcuar pump unc-
on
n
proporon
o
e
voume
o
damaged
myocardum.
Severe
“pump aure” (cardogenc sock) occurs n rougy 10% o paens
w
o
•
ransmura
e
et
Papary
musce
nrequeny
o
•
bu
myocardial
infarct
of
the
posterolateral
left
s
w o
r upure
Acute
necrosis
by
a
lack
(arrow);
of
the
triphenyltetrazolium
absence
of
staining
chloride
is
due
to
cell
death.
staining
in
enzyme
(asterisk)
in
this
The
Note
the
anterior
is
myocardial
scar
(arrowhead),
due
patient
to
hemorrhage
ventricular
(specimen
is
rupture,
oriented
at
and
with
the
was
the
right
indicative
the
edge
acute
posterior
of
of
at
he
puse
and
usuay
nauseaed.
conracy
and
s
rapd
Dyspnea
dysuncon
and
s
o
weak
and
common,
e
paens
due
mra
o
vave
are
e
death
s
mos
dapo-
•
cardogenc
sock
deveops
due
o
pump
w
resu-
can
ep
o
deermne
e
ype
o
narcon
(STEMI
or
o
5
s ep a
and
days
cas es,
narc
w en
oten
papar y
are
o cc urs.
erapy.
usuay
musces
rupure
dysuncona,
I
L et
resung
amp onade
r upure
may
papar y
s
n
(Fg.
e
50%
me
consss
Arrytma.
ar
aure.
eadng
s
more
common
ven r c uar
n
rapd y
ree
a a
n
wa
(s ee
Fgs.
8.7
and
emo-
8.10A).
cre ae
mus ce
a
et-o-r g
r upure
may
sun
e ad
(s ee
o
s e vere
o
o
8.10C).
cas es
Rupure
dur ng
s ot,
braon)
responsbe
s
or
he
90%
rsk
greaes
e
n
e
r abe
Approxmaey
dsurbance.
and
or
e
majory
e ang
usuay
e
o cc urs
w n
o
paens
serous
weeks
n
muc
o
ssue.
deveop
and
wo
w en
arryma
our
deas
rs
pro cess
granuaon
rs
o
w n
some
(e.g.,
decnes
occurrng
orm
ereater.
pror
o
o
venrcu-
I
ospa-
zaon.
Caracersc eecrocardograpc abnormaes are usuay presen
and
cardac
regurg aon
rs
rym
an acue pumonar y congeson and edema. W massve myocarda
narcon,
a a
romb oyc
common,
and
8.10B),
90%
top).
myocarda
apparaus,
ey
infarct
of
the
oten
mpared
more
areas
e
rec
or
remote
the
cause
wall
40%
leakage
mra infarction.
damage
ventricle
Fg. after
a
regurgaon.
requen y
receve
Venr c uar of
Aoug
narcon,
mra
p er cardum demonstrated
ose
Myocarda r upture. Rupure compcaes on y 1% o 5% o narc-
os e
8.7
ypcay
dysfuncton.
ater
posnarc
ons
Fig.
narcs,
venrce.
NSTEMI)
•
Percardts.
orragc
Transmura
percards
narcon
due
o
can
ec
underyng
a
panu
myocarda
brnoem-
nlammaon
124
CHAPTER
Heart
8
A
B
C
E
D
Fig.
8.8
ulative
by
Microscopic
necrosis
edema
removal
ized
by
of
fluid.
(B)
loose
A
few
collagen
of
myocardial
fibers,
compared
neutrophilic
myocytes
connective
scar.
stains
features
wavy
Dense
necrotic
collagenous
which
and
by
tissue
infiltrate
phagocytic
and
residual
infarction
with
abundant
cardiac
and
adjacent
in
the
its
area
macrophages
capillaries.
muscle
cells
(E)
are
repair.
normal
of
(7
a
2-
to
(A)
fibers
to
10
Healed
present.
One-day-old
(right).
3-day-old
days).
(D)
and
(E)
infarct.
infarct
are
showing
cells
(C)
are
tissue
consisting
Masson’s
coag-
separated
Nearly
Granulation
myocardial
(D)
infarct
Necrotic
complete
character-
of
a
dense
trichrome
stain,
blue.
(see
40
Fg.
8.10D).
narcon
•
and
Percards
resoves
over
ypcay
e
nex
appears
ew
2
o
3
days
ater
days.
V entrcuar daton and aneurysm formaton. Because necroc mus-
)timil
ce
s
weak,
ere
may
be
dsproporonae
srecng,
nnng,
and
In Troponin
some
arge
ransmura
narcons,
s
eads
o
venrcuar
aneu-
I
rysms
(see Fg.
8.10F),
wc
are
prone
o
mura
romboss
and
are
CK-MB
assocaed
•
Myoglobin 20
Mura
and
w
arryma
trombus.
endocarda
Sass
and
due
damage
o
ear
aure.
dmnsed
osers
mura
Rupure
s
myocarda
romboss
uncommon.
conracy
(see
Fg.
8.10E),
fo selpitlum=(
evitaleR
reppu
n oi tartnecn oc
ecnerefer
daon o e narced regon (especay w anerosepa narcs).
30
w
•
rsk
or
Reper fuson
low
o
et-sded
njury.
scemc
As
romboembosm
dscussed
musce
may
n
Caper
paradoxcay
2,
resoraon
cause
e
o
dea
bood
o
va-
10
be
“a-rsk”
ncreased
myocardum.
producon
o
damaged
mocondra,
damaged
membranes,
he
precse
reacve
ncreased
and
mecansm
oxygen
upake
deeerous
speces
o
o
unceran:
rom
cacum
efecs
s
ces
no
w
ces
w
nlammaor y
ces
0
ave 4
20
he Hours
after
onset
of
chest
8.9
Increases
in
myocardium-derived
troponin
I,
myocardial
kinase
(CK-MB),
and
myoglobin
following
injury.
are
particularly
sensitive
and
specific
ong-erm
myocardial
acors,
o
conrbue
markers
of
e
prognoss
mos
ater
mporan
myocarda
o
wc
narcon
are
et
depends
venrcuar
on
unc-
and
e
severy
o
aerosceroc
coronar y
arer y
dsease.
he
infarction.
overa Troponins
proposed
cre-
on atine
been
pain
many Fig.
a
40
moray
rae
wn
e
rs
year
s
abou
30%,
ncudng
myocardial
deas
occurrng
beore
e
paen
reaces
e
ospa.
ereater,
CHAPTER
A
B
C
D
E
F
Fig.
8.10
rupture
with
a
Complications
(arrow).
infarct
aneurysm
cardiovascular
of
e
annua
narcon
moray
s
3%
o
William
rae
or
D.
of
septal
roughened
with
wall
(arrow).
pathology:
Edwards,
paens
myocardial
Ventricular
hemorrhagic,
anteroapical
tricular
(B)
(A
wo
epicardial
stretching
to
E,
clinical
MD,
surface
and
sufered
a
to
by
and
an
Chronic
thy,
is
Ischemic
ischemic
Heart
characterized by
myocardial
Disease
disease,
also
progressive
(A)
Anterior
rupture.
infarct.
mural
from
(D)
(E)
Recent
thrombus.
Schoen
FJ:
Philadelphia,
free
wall
Fibrinous
(F)
apical
Interventional
Saunders,
myocardial
pericarditis,
expansion
Large
125
and
1989;
F ,
of
left
an
ven-
surgical
Courtesy
Minnesota.)
Clncal
severe,
heart
acute
principles,
sodes
Chronic
rupture.
muscle
and
permission
Rochester,
myocarda
Cardiac
Papillary
(arrow)
basic
4%.
C)
(C)
overlying
thinning
Reproduced
Clinic,
(A
(arrow).
correlations
Mayo
ave
infarction.
rupture
Heart
8
Features.
Cronc
progressve
o
angna
ear
or
scemc
aure,
narcon.
ear
dsease
occasonay
Arryma,
s
assocaed
puncuaed
ear
aure,
by
and
new
w
ep-
nercur-
ren myocarda narcon accoun or mos o e assocaed morbdy
called
heart
ischemic
failure
due
cardiomyopa-
to
and
moray.
cumulative
damage.
ARRHYTHMIA
Pathogeness.
narcons:
or y
Usuay,
Cronc
mecansms
cardac
cronc
over
uncon.
o
myocarda
e
In
scema
ere
s
scemc
a
resdua
oer
cause
sor y
ear
o
dsease
one
myocardum
cases,
severe
wdespread
or
occurs
can
myocarda
wen
compensa-
no
coronar y
myocarda
more
onger
arer y
manan
dsease
dysuncon
Aberrant
ting
he
eecrca
propagaes
narcon.
scemc
ear
dsease
ypcay
resus
n
daon
and
yperropy,
oten
w
dscree
areas
rom
prevous
eaed
narcs.
Invaraby,
ere
s
severe
aerosceross
sows
pacy,
o
e
brous
coronary
areres.
ckenng,
and
he
mura
presen.
may
and
a
Mcroscopc
ses
o
pror
ndngs
ncude
myocye
is
arises
a
in
major
the
set-
cause
of
ce
e
sar
a
o
coordnae
ce
roug
snoara
node
o
any were
node
e
n
myocarda
gap
(e
n
a
wave
cardac
pacemaker)
o
venrces.
base
e
conracon
juncons
e
conducon
sysem
and
are
a
roug
Aberran
on
e
se
o
orgn,
eer
e
are
supravenrcuar
subd-
(ara)
can
myocardum.
manes
as
Arrymas
ryms
a
may
are
be
oo
susaned
sow
or
spo-
(bradycarda),
endocardum
romb
as
(tacycarda),
yperropy
rreguar,
or
a
precude
efecve
cardac
may (ventrcuar
ibraon
and
asysoe).
Ara
braon
and occurs
bross
rom
based
pumpng
be
sgnas
rom
venrcuar
oo
generay
and
moderae radc,
o
frequently
scarring
o or
scarrng
or
et vded
venrcuar
(arrhythmia)
ischemia
arovenrcuar
ryms
Cronc
rhythm
death.
ransmed
e
Morphology.
heart
myocardial
sudden
and
wou
of
wen
ara
myoc yes
become
“rrabe”
and
depoarze
nde-
narcon. pendeny
and
sporadcay
(as
occurs
w
ara
daon);
e
sgnas
126
are
CHAPTER
varaby
ransmed
Heart
8
roug
e
arovenrcuar
node,
eadng
o n
e
“rreguary
rreguar”
ear
rae
and
rym
o
ara
sze
(boxcar
ncudng I
e
arovenrcuar
node
s
dysuncona,
var yng
degrees
o
W
ragmenaon
aure,
and
oss
degenerave
o
myocye
canges
appear,
conrace
bers.
ear ere
bock
nuce).
braon.
oten
are
scaered
oc
o
nerceuar
bross,
represenng
occur ses
o
myocye
venrcuar Pat h o g e n e s s .
A c q u i re d
myocardial
diseases
and
of
ion
transport
a re
important
causes
dropou
due
becomes
o
sf,
scema.
mparng
Inay
dasoc
e
ckened
ng
and
et
eadng
inherited o
disorders
wa
of
et
ara
daon,
bu
w
progresson
o
congesve
ear
aure
rhythm venrcuar
daon
appears.
disorders.
Acqured
ncude
ceuar
mos
aed
acors
scema,
maera
da
eecrca
and
In
a
are
s
mos
o
myocarda
scarrng,
cases,
on
sgna
and
arer y
s
are
o
usuay
cannes
and
assocaed
be
myocardum.
and
o
exra-
amyodoss).
dsease
no
appears
conducon
deposon
cardac
ere
us
abnorma
common
cardac
(e.g.,
coronar y
arryma
ess
encode
or
myoc yes
acor
“rraby”
arrymas
genes
rsk
njur y.
narcon,
dsurb
beween
mporan
scemc
a
nlammaon
myocar-
rggered
Inered
due
(so-caed
o
e
assoc-
by
e
orms
muaons
by
used
a
muaon
medcaons
syndrome.
cay
n
a
rgger
Canneopaes
perormed
nonea
afecng
can
paens
poassum
are
n
dagnosed
w
a
amy
Many
paens
by
sor y
or
ong
esng,
an
Features.
suspeced
ncdenay
roed
yperenson
poenang
Efecve
yperenson
QT
yp-
unexpaned
Right-Sided
Right-sided
disorders
Ar ry m a
may
or
a
be
asy mpoma c,
rapd
e ar
rae,
be
or
re ae d
o
nade qu ae
c ard ac
oupu,
suc
as
e
rsk
dsease
o
venrcuar
conro
greay
asympomac
bood
yperropy.
or
ear
s
eevaed
scemc
aerosceross),
braon,
s ens e d
c aus e
(Pulmonary)
the
to
lung
rena
aure,
essens
pressure
Poory
ear
damage,
and
e
o
with
Hypertensive
heart
disease
parenchyma
left-sided
associated
cerebro-
sudden
rsk
o
con-
dsease
a
dea.
o
ese
ventricular
left-to-right
soaed
may
or
Heart
be
Disease
caused
vasculature,
failure
or
by
or
primary
may
congenital
occur
heart
dis-
shunts.
rg-sded
yperensve
ear
dsease
(aso
as
as
cor
pumonae)
ncude
dverse
dsorders
afecng
pumo-
sy mp-
nar y oms
coronar y
ara
hypertensive
of
secondary
(paptatons)
et
ear
dscover y
compcaons.
known b e as
e
ncreases
sroke,
Causes Features.
dscovered
vascuar
arryma.
abnor ma
yperensve
rom
(by
ease
Clncal
E ary
ony
commony
w
genec
or
s
o
canneopaes).
canne.
arrymas
and
n
e prooypca canneopay s e ong QT sy ndrome, caused mos
oten
Clncal
an ng
ar
excange
or
e
pumonar y
vascuaure
(Caper
10).
A
(sy n-
produce ncreased pumonar y vascuar ressance, eadng o yperencope).
Sudden
de a
c aus e d
by
ven r c u ar
br a on
or
asysoe
son, o cc urs
n
roug y
400,000
p e ope
e ac
ye ar
n
e
Une d
S aes.
rg
due
be
o
e
coronar y
rs
ar er y
ds e as e
manes a on
o
n
80%
coronar y
o
90%
ar er y
o
c as es
ds e as e.
and
In
venrcuar
ear
aure.
nona eros cero c
canneop a es,
congen a
c aus es
are
more
abnor ma es
common,
n
va ves
es,
o er
myo c ard s
and
and
myo c ard a
nl ammaor y
yp er ropy
ds orders,
s e cond ar y
o
younger
or
coronar y
ncude
ncreases
arera
congesve
e
vesses
dsease
of
ear
workoad
Caper
aure
and
dfuse
pumonar y
nersa
prmar y
vesses,
pumonar y
suc
as
bross
recurren
romboembosm
yperenson
and
•
Dseases afecng ches movemen, suc as kyposcooss and obesy
•
Dseases
causng
seep
pumonary
vascuar
consrcon,
suc
as
obsruc-
apnea
ear
embosm)
or
aure
may
may
appear
be
acue
sowy
and
n
onse
(e.g.,
nsdousy
w
pumo-
because
o
pro-
DISEASE
cardac
(see
rg-
are:
Dseases
onged
on
evenuay
•
Rg-sded
efecs
and
dsorders
Dseases of pumonary parencyma, suc as cronc obsrucve pu-
nar y
Hyperenson
8.11B),
suc
•
ve
HEART
(Fg.
common
c ardomyop a-
yp er enson
ac ors.
HYPERTENSIVE
mos
ncudng
and ar er es,
he
may
monar y p a ens,
yperropy
I
sded s
and
7).
aa
and
he
aso
as
cardac
arryma.
pressure
overoad
n
e
seng
o
cronc
pumonar y
dsease.
deeerous
compcaons
Aoug
e
et
VALVULAR
HEART
DISEASE
sde o e ear s mos commony afeced due o e requency o sys-
emc
aso
yperenson,
occur
n
some
rg-sded
dsease
yperensve
canges
(cor
pumonae)
sengs
Valvular
and/or
disease
results
insufciency
in
cardiac
dysfunction
(regurgitation
or
by
causing
stenosis
incompetence).
Senoss s e aure o a vave o open compeey, obsrucng or-
Systemic
Systemic
ular
the
(Left-Sided)
hypertens i v e
hypertrophy
absence
of
Hypertensive
hea rt
d is ea s e
s eco n d ary
other
to
is
Heart
Disease
d ene d
d o c ume nt e d
ca rdio v a scul ar
by
le f t
ward
v e n t r ic
hy per t e ns io n
pa t ho lo g y
(e . g . ,
in
v a lv ul a r
stenosis).
or
resus
e
(e.g.,
nduces
et
Even
venrcuar
workoad
agans
onged
severe,
or
md
yperenson
yperropy
ressance
e
ear
(Fg.
may
(>140/90
as
8.11A).
no
an
I
onger
Hg),
adapaon
e
be
mm
o
o
adap
proonged,
e
yperensve
abe
ncreased
sress
s
efecvey
pro-
and
amos
rom
eale
mon
aure
cusps
scarrng
on
e
sounds
et
as
a
vave
o
or
cronc
or
rom
o
e
cose
roug
murmurs;
or
o
rupure)
and
s
ocaon,
low
or
usuay
vaves
quay,
and
may
due
more
acqured.
Tabe
o
com-
Causes
o
8.2
produces
mng
srucures
nsdousy
muc
o
dsease
Insuicenc y
s
abnormaes
bood
rom
supporng
dsease
n
caccaon
Insuicency
aowng
resu
musces).
summarzed
dseased
can
e
(e.g.,
cusps.
compeey,
Vavuar
ear
severe
vave
nsuicenc y
corda
are
process
more
papar y
reracon.
he
a
one
endocards)
dsease
hrs.
o
Vavuar
cords
sde
low
caed
papaed
and
due
afecs
(e.g.,
(e.g.,
vavuar
Abnorma
may begn o a.
o
endnous
abrupy
acqured
a
(backlow).
vave
e
appear
aways
scarrng)
regurgae
o
Pathogeness.
low,
vave
abnorma
may
o
be
e
ear
exernay
murmur
are
Morphology. he ear s eavy and e et venrcuar wa s ckdeermned ened.
Mcroscopcay,
myocyes
and
myocye
nuce
are
by
e
vave
afeced,
e
efec
o
e
ncreased versus
senoss),
and
e
severy
o
e
deec.
eson
(regurgaon
CHAPTER
Heart
8
127
*
A
Fig.
8.11
Hypertensive
concentric
atrium
the
are
right
ulae.
Table
8.2
shown
diastolic
on
The
Etiology
thickening
ventricle
impaired
(shown
of
B
the
on
the
the
and
volume
Acquired
Heart
this
also
to
dilated
of
Systemic
the
Valve
wall,
left
left
atrial
atrial
and
(left-sided)
causing
four-chamber
the
leading
markedly
(A)
ventricular
in
Note
relaxation,
is
disease.
left
right
(arrow).
left)
shape
heart
of
view
volume
have
hypertensive
reduction
of
dilation
the
with
been
(B)
a
in
heart.
(asterisk)
overload.
hypertrophied
ventricle
a
Valve
Disease
Aortic
Stenosis
Postinflammatory
Aortic
scarring
Calcification
heart
of
mitral
(rheumatic
ring
Senile
Cacicaons,
Regurgitation
Abnormalities
of
Aortic
leaflets
and
aortic
of
commissures
a
The
ventricle
right
n
in
and
ventricle
trabec-
ventricle.
c ard ac
re qure
va ves
are
subs an a
re ae d
va ve
o
rep e ve
d eor ma on
T e
mos
common
d egenera ve
w
canges
•
Aeraons
wc
can
be
cuspa
(n
e
aorc
vave)
(Fg.
are:
8.12A
B)
or
annuar
n
e
(n
e
mra
exraceuar
vave)
marx.
(Fg.
8.12C
here
can
and
be
D).
ncreased
pro-
stenosis
and
dmnsed
brar
coagen
and
easn
(myxoma-
congenitally
degeneraon)
or
bross
and
scarrng.
valve
Regurgitation
Intrinsic
canges
left
hypertrophied
right
left
incidentally
disease)
ous
Mitral
and
enlarged
op enng .
•
eogycan
deformed
the
pulmonale.
wall
marked
and
scarring
heart
calcific
Calcification
the
present
of
is
ventricle
Stenosis
Postinflammatory
disease)
cor
free
s ress es
nor ma
and
(rheumatic
is
There
left
Disease
e ac
Mitral
The
stiffening
D egenera ve
Disease
Valve
to
Chronic
by
disease.
size.
pacemaker
thickened
me canc a Mitral
A
due
distorted
heart
lumen
valvular
disease
Postinflammatory
Calcific
Aortic
Calcic
aortic
Degeneration
degeneration
is
the
most
common
cause
of
aortic
be
scarring
stenosis.
Postinflammatory
scarring
(rheumatic
heart
disease)
Cacc Infective
endocarditis
Infective
enoug Mitral
valve
prolapse
Aortic
degeneraon
usuay
s
asympomac,
bu
may
severe
endocarditis
o
cause
senoss,
necessang
surgca
nervenon.
e
nc-
disease
dence ncreases w age, and mos paens presen a e age o 70 years “Fen-phen”–induced
valvular
Degenerative
aortic
dilation
or fibrosis
Syphilitic
Abnormalities
Rupture
of
Papillary
of
tensor
papillary
muscle
apparatus
muscle
Ankylosing
Marfan
a
spondylitis
Rheumatoid
dysfunction
o
arthritis
of
o
chordae
Abnormalities
of
An
dsorder
ree.
mporan
aorc
n
and/or
ventricular
senoss
s
bcuspd
aorc
1
o
2
vave
eary
conans
occurs
n
decades
e
n
bu
earer
wo
aorc
vave,
1%
s
uncona
a
congen-
o
2%
prone
an
o
o
a
cusps
ve
caccaon
norma
rcuspd
nsead
brs.
I
s
eadng
vaves.
left
ventricular
Rsk
acors
or
aorc
vave
degeneraon
and
cac-
annulus
ncude
mae
sex,
g
ow-densy
poproen
coesero,
enlargement
yperenson, (myocarditis,
acor
vave
tendineae
caon Left
rsk
e
asympomac
Pathogeness.
cavity
wc
Bcuspd
generay
syndrome
(fibrosis)
Rupture
greaer.
aortitis
dilated
and
smokng,
a
o
wc
are
aso
assocaed
w
a-
cardiomy-
erosceross.
e
accumuaon
o
poproens
nduces
oca
nlamma-
opathy)
on, Calcification
of
mitral
wc
vave, Fen-phen,
Data
Schoen
Hum
Pathol
FJ:
Surgical
18:558,
pathology
of
removed
natural
and
prosthetic
njur y
predsposes
Valve
cusps
Disease
a
aer
valve
disease
is
an
umbrella
term
that
in
the
valvular
extracellular
matrix
that
(Fg.
describes
o
function.
e
vave
negatively
affect
Heaped-up
prorude
senoss Degenerative
valve
exacerbaed
by
low
abnormaes
endoea
ce
(e.g.,
uncon.
e
bcuspd
resung
or
caccaon.
1987.
Morphology.
Degenerative
changes
be
yperenson)
Fenfluramine-phentermine.
from
valves,
may
ring
bross.
and
8.12A
caced
masses
mecancay
and
B).
e
on
mpede
cusps
e
oulow
vave
oten
sde
openng,
sow
o
e
causng
ckenng
due
128
CHAPTER
Heart
8
A
B
C
D
Fig. Fig.
8.12
Calcific
valvular
degeneration.
(A)
Calcific
aortic
stenosis
of
8.13
normal
valve
(viewed
from
above
the
valve).
Nodular
calcium
are
heaped
up
within
the
sinuses
of
Valsalva
hooding
(arrow).
the
atrium;
commissures
are
not
fused,
as
in
rheumatic
aortic
valve
Fig.
11.19C).
(B)
Calcific
aortic
stenosis
occurring
on
a
(arrow).
annulus
view.
the
valve.
(C
One
and
D)
(attachment
(D)
Cut
the
has
a
partial
of
the
myocardium.
the
Such
septum
with
mitral
demonstrating
interventricular
fusion
calcification,
margin)
section
underlying
near
cusp
Mitral
at
its
leaflets
impinge
on
called
nodules
(arrows).
extension
involvement
can
center,
calcific
of
the
of
the
in
the
this
a
o
30%
o
In
norma),
severe
cronc
dsease
oulow
(aorc
vave
(C)
Left
obsrucon
adjacent
into
structures
conduction
may
Clncal
et
o
20%
venrcuar
e
o
as
dysuncon,
es.
ear
ay
aure,
or
occurrng
syncope
wn
5
appears,
years.
he
e
aure.
Once
prognoss
reamen
s
s
angna,
poor,
surgca
w
congesve
dea
repacemen
Mitral
Valve
e
left
leaets
atrium
Prmar y
aon
more
o
an
and
of
the
mitral
prolapse,
valve,
ballooning
one
or
back
both
into
vave
o
ear
proapse
o
dsease;
s
a
orm
adus.
women
I
s
are
o
myxomaous
one
o
afeced
e
mos
amos
degener-
common
seven
mes
men.
he
due
s
manesaon
ear
As
o
a
usuay
connecve
dscussed
n
reflecting
long-standing
the
valvular
The
left
(Courtesy
ventricle
of
William
is
shown
D.
on
Edwards,
the
MD,
are
asympomac;
e
vavuar
abnor-
s
dyspnea,
cck,
usuay
usuay
requres
or
aypca
somemes
bengn,
(see
aer)
sgncan
oowng
repar
or
oug
and
ces
w
a
pan.
ere
s
an
approxmaey
mra
rupure
Auscuaon
regurgan
3%
regurgaon
o
e
repacemen
o
cordae
e
murmur.
ncreased
o
and
or
mra
rsk
paens
conges-
vave
ea-
vave.
Valvular
heart
acute
Disease
disease
is
the
cardiac
immunologically
manifestation
mediated
of
multisystem
rheumatic
inamma
unknown
(dopac).
Rarey,
Caper
ssue
6,
dsorder,
Maran
parcuary
syndrome
s
Maran
mos
that
occurs
after
group
A
β-hemolytic
streptococcal
rggerng
s
vavuar
dsease
necon
vruay
ypcay
aways
nlammaon
as
decned
n
nvoves
caused
and
by
scarrng.
many
pars
e
par ynx.
reumac
e
o
e
Mra
ear
ncdence
Wesern
se-
dsease,
o
s
reumac
word
over
e
pas severa decades, due o mproved socoeconomc condons, rapd
e
and
reamen
vruence
o
many
o
srepococca
srans
o
group
par yngs,
A
and
srepococc.
a
decne
However,
n
s ncome
counres
and
economcay
depressed
areas
n
e
Uned
synSaes,
drome.
view.
paens
endocards
aure,
dagnoss
eoogy
Mos
course
wc
o
ow a
an
e
n Pathogeness.
overload.
papaons,
disease
noss,
2.4%
dilated,
infections.
the
systole.
0.5%
vavuar
oten
“oppy”
mtra
afecng
orms
are
is
Disease
degeneration
during
promi-
into
Minnesota.)
mdsysoc
Rheumatic
tory
mitral
volume
Rochester,
Treamen
fever,
myxomatous
also
emodynamcay
ear
Rheumatic
Myxomatous
is
usu-
o
dseased vave.
In
a
necve
ve
ear
and
Features.
cnca
deveop
congesve
There
(arrow)
may s dscovered ncdenay on pysca examnaon. A mnory o
yperroped myocardum s prone o scema and sysoc and dasoc
o
atrium
four-chamber
Clinic,
pressures o 200 mm Hg or more, causng et venrcuar yperropy. he
eadng
valve.
leaflet
system.
reduced
rase
mitral
mitral
atrial
calcification
orce
the
the
dscoses
Features.
of
posterior
raphe
within
paens
Clncal
the
congenitally
Mayo bicuspid
of
stenosis
right (see
degeneration
prolapse
Note
insufficiency that
with
masses
left of
Myxomatous
a
nent previously
reumac
ear
dsease
s
an
mporan
pubc
ea
probem,
commony and
remans
e
mos
common
cause
o
acqured
vavuar
dsease
n
caused by muaon n e gene encodng brn. e
Morphology.
ere
s
baoonng
(oodng)
o
e
afeced
word.
mra Pathogeness.
eales
(Fg.
8.13),
wc
are
enarged,
redundan,
ck,
and
cocca ber y.
he
endnous
cords
are
eongaed
and
nned,
and
srans
On
soogc
myxomaous
(mucod)
examnaon,
e
vave
sows
cross-reac
agans
w
e
M
proens
proens
ound
n
o
e
ceran
srepo-
myocardum
and
may cardac
rupure.
Anbodes
rub-
deposon
vaves.
ese
anbodes
are
oug
o
cause
njur y
by
ac-
o vang
compemen
CD4+
T
and
Fc
recepor–bearng
ces
(e.g.,
macropages).
maera. ces
a
recognze
srepococca
pepdes
and
os
angens
CHAPTER
aso
appear
and
may
ec
cyokne-medaed
nlammaor y
Heart
8
129
responses. reumac
ear
dsease
w
vave
dysuncon
nvovng
e
mra
Ony abou 3% o paens neced w srepococc deveop reumac vave
n
95%
o
cases;
25%
o
ese
cases
aso
afec
e
aorc
vave.
ever, suggesng a os genec varans may nluence suscepby. Fbross
o
Morphology.
afecng
a
In
acue
varey
o
reumac
ssues,
ever,
ere
ncudng
a
are
ree
nlammaor y
ayers
o
e
oc
ear.
Percardts assocaed w a brnous exudae
•
Myocardts
n
e
orm
o
scaered
Ascof
bodes
wn
e
connecve
ssue;
paognomonc
Ascof
becomes
8.14A)
conss
o
coecons
o
ympocyes
scaered
(prmary
pasma
ces)
ces,
w
and
pump,
assocaed
acvaed
brnod
daed
Vavus,
rs
na
e
resung
nes
o
n
brnod
cosure,
necross
oten
vegeaons
and
(Fg.
o
senoss.
occur,
E)
eads
Fbross
urer
o
uson
and
uson
exacerbang
vave
pressure
overoad.
reumac
aso
occur
ever
s
n
adus.
mos
o
wo
Two
o
common
ree
n
weeks
c-
ere
s
one
conseaons
o
ater
sympoms:
macropages mos
and
assocaed
brn
w
commony,
by
a
mgraor y
cards;
or
(2)
arrs
n
abou
n
one
20%
o
or
more
jons
paens,
oten
neuroogc
deposon
sma
mos
noaby
Sydenam
corea
(S.
Vus
dance),
car-
romby
nvounar y
movemens,
musce
weakness,
and
emo-
8.14B). ona
Percards
mra
aso
8.14C
necross
acerzed boc
may
o
Acue
aacks
necon,
sympoms, aong
owng
Features.
bu
accompaned
•
severe
endneae
(Fg.
T
(1) (Ansckow
and
eales
e
e ces),
vave
bodes dren,
(Fg.
mra
commssures
cordae
Clncal nersa
e
dysuncon. W g mra senoss, e et arum progressvey
Acue cardac nvovemen may ead o one or more o e oowng:
•
e
o
o
myocards
may
ead
o
oca
scarrng
bu
dsurbances.
Fever
may
aso
be
seen
n
some
cases.
here
s
no varabe
nvovemen
o
e
skn
(ras
and
subcuaneous
nodues).
perssen abnormaes. In conras, vavus oten eads o cronc hroa
cuures
are
negave
wen
sympoms
begn,
B
A
C
D
Fig.
8.14
carditis;
cells,
there
etations
(B)
(C).
tion
the
of
(D)
(E)
the
visible
have
shortening
Surgically
cusps
of
of
leaflet
along
the
of
the
heart
line
fibrous
with
specimen
closure
thickening
distortion
From
Pathol
is
mitral
mitral
valve;
18:568,
the
left
note
stenosis,
FJ,
St
1967.)
of
central
leaflet
chordae
leaflets,
marked
aortic
Aschoff
body
in
wavy
the
disease.
(arrows).
as
demonstrating
John-Sutton
M:
(C
fusion
seen
inflammatory
chromatin
Small
Previous
tendineae.
dilation
rheumatic
inflammatory
(caterpillar)
heart
commissural
atrial
acute
mononuclear
rheumatic
valve
of
valve
Schoen
and
chronic
fusion
the
an
collection
nucleoli
on
the
and
of
rheumatic
(E,
Hum
of
There
rheumatic
of
fusion.
of
circumscribed
prominent
tendineae.
opened
disease,
a
appearance
superimposed
of
and
chordae
an
with
valvulitis
thickening
commissural
valvular
Microscopic
macrophages
mitral
removed
with
E
(A)
associated
caused
fibrous
Anterior
pathology
necrosis
activated
are
diffuse
and
disease.
rheumatic
valvulitis
with
thickening
(arrow).
some
Acute
rheumatic
heart
central
(verrucae)
stenosis
valve
is
including
(arrows).
of
Rheumatic
and
veg-
episodes
D)
Mitral
(arrows),
from
above
and
the
neovascularization
thickening
and
Contemporary
distor-
issues
in
bu
serum
ers
130
o
CHAPTER
anbodes
DNase)
da
rcon
ear
he
agans
usuay
rubs,
aure,
bu
dagnoss
on
n
are
s
cardac
acue
srepococca
1%
based
w
dsease
o
on
e
sgns
mra
paens
de
o
srepoysn
cards
addona
o
acue
pror
cnca
reacvaon
causng
(e.g.,
o
ncude
nsuicenc y,
evdence
ypca
subsdes,
necons,
angens
Cnca
daon,
an
made
conjuncon
Ater
srepococca
eevaed.
ess
Heart
8
reumac
descrbed
occur
njury
o
w
e
or
Sma romb a orm a ses o pacemaker nes, ndweng vascuar
caeers,
congesve
srepococca
eaures
may
and
O
percar-
seedng
ever.
necons
nec-
aso
arum
and
produces
ear
romboembosm.
e
pumonary
aure;
w
me,
rsk
Cronc
vascuar
rg
e
and
o
mura
pumonary
parencyma
venrcuar
ear
venous
canges
(cards)
vaves
n
e
et
congeson
o
and
are
caused
lora.
o
By
e
skn)
or repacemen o dseased vaves can oresa many o ese compcaons
ons
are
reeased
and as greay mproved e ouook or ese paens.
o
be
e
Seedng
may
occur
the
endocardium
of
thrombus
to
underlying
he
devces
ra
aora,
may
on
apy
that
presence
lead
to
of
heart
vegetations
varying
degrees
become
and/or
Subacute
and
sacs,
oer
neced.
o
bood
Mos
endocards
severy
n
a
valves
or
s
composed
o
Pathogeness.
we
as
nvove
s
e
vesses,
cases
are
cassed
cnca
prevousy
sgncan,
of
e
reers
even
onse
proraced
Acqured
s
w
as
and
e
more
aack
vrdans,
vruen
eay
as
a
componen
ear
acue
by
n
In
probaby
no
o
bood
w
obvous
o
drug
we
10%
as
o
n
ver y
w
dena
sma
mcrobes
or
occu
or
rva
s
norma
(com-
vaves
and
s
surgca
organsm
s
soaed
wn
vegea-
numbers.
e
proxmae
necon,
maera
njures.
predsposng
or
no
embedded
a
no
acors
cause.
dena
e
(e.g.,
or
hs
surgca
boodsream
Anboc
propyaxs
prosec
ear
procedures.
or
are
subacue
necons
ear,
over
weeks
anboc
vaves.
nous
usuay
and
o
o
nvovng
even
wen
mons.
o
o
ear
and
necve
endocards,
buky
and
poenay
8.15
Infective
myxomatous
mitral
Staphylococcus
abscess
(arrow).
endocarditis.
valve.
The
aureus
on
(A)
large,
(suc
users,
ear
n
wc
abscess
e
vaves
common
somemes
rom
e
Cln cal
senoss)
e
(rng
rabe
(Fg.
ses
8.15).
o
no
abscess)
e
(see
vegeaons,
e
necon
rcuspd
erode
deveopmen
bross
o
ecs
n
and
Feature s.
endo c ard s,
endocards.
a
Subacute
friable
endocarditis
vegetations
congenitally
bicuspid
desruc-
vave
s
aorc
excep
o
mra
nrave-
nvoved.
myocardum
8.15B).
eadng
n
requeny
underyng
Fg.
and
Sepc
sepc
o
embo
narcs
and
mycotc
ess
aneurysms
vavuar
(see
desrucon
Caper
and
s
7).
Sub-
assocaed
w ormaon o vegeaons, cronc nlammaor y nraes, and
paens
vaves
aorc
e
mos
endocards
vavuar
proapse,
predspose
o
acue
erapy.
vave
on
e
an
sed
ead
or
unreaed
Mos
acue
abscess ormaon were ey odge. Seedng o e vesse was may
vr-
scarred
drug
produce
er-
ow
are
Vegeaons
Morbdy
anboc
organsms
abnormaes
mra
vaves
by
presen
vaves
course.
norma
In
ve vegeaons conanng brn, neurops, and mcroorgansms
oder
bu
adu s),
caccaon.
Fe ver
may
n
s
be
w c
e
mos
abs en
on y
n
cons sen
sub ac ue
vague
are
caused
by
denoted
aortic
valve
Streptococcus
by
with
arrows.
(B)
extensive
viridans
Acute
sy mpoms
cuspal
on
a
previously
endocarditis
destruction
caused
and
sg n
ds e as e
B
by
e
aureus
deormed
cases,
organsms
conamnaed
users,
paens
undergong
abou
because
e
bood
an
njecon
Morphology.
bace-
A
Fig.
o
Stapyococcus
damage
prosec
caused
approprae
nsdous
srucura
senoss,
prosec
o
abnorma
approprae
mra
crca
are
prevousy
s
can
e
nravenous
vaves)
surger y.
ater
reumac
are
vaves.
course
recover
may
endocardts
deormed
e
a
abuse)
tissues.
Inecve
moray
uence
as
the
the
Acute endocardts reers o desrucve necons by gy vruen
and
as
organisms
empo
organsms
•
by
aneur ysma
aso
e
marked
cardiac
necons.
based
•
and
by
of
Streptococcus
cupr.
due
procedure,
Endocarditis
infection
drug
oucomes.
speces, oten commensa n e ora cavy, and even ung on occason
bood,
microbial
bacera
n necons occurrng n nravenous drug users. Many oer bacera
e
a
nravenous
bacera
o
et-sded
rom
is
and
afecs
or
rg-sded
prove
endocarditis
neuropena
adversey
so
responsbe or 10% o 20% o cases overa; aso s e major ofender
suscepbe o necve endocards. Mra vavuopasy or surgca repar
Infective
by
conras,
ear aure may ensue. In addon, scarred and deormed vaves are more
Infective
o
and
ere
he causave organsms var y dependng on e underyng rsk ac-
romb
yperropy
rsk
a
suscepby
ors. From 50% o 60% o cases o endocards o damaged or deormed
mon
ncreasng
secondar y
e
provde
Increased
earer.
eads
braon,
(e.g.,
endocardum
endocards.
subsequen
ora
ara
damaged
ensung
ncreases
and mra vave (mra senoss). W mra senoss, ara daon oten
o
or
and
ring
o
ne c ve
( p ar c u ary
suc
as
a gue,
CHAPTER
weg
oss,
and
endo c ard s
c s,
and
and
u ke
as
we a k ness .
e -sde d
bed
a
o en
esons.
re na
a
sy ndrome
sor my
Mur murs
are
M cro emb o
emor rages,
are
ons e
ound.
w
pres en
c an
n
g ve
p an ess
By
r ap d y
o
o
e ver,
p a en s
w
p ee c ae,
er y emaous
p a m
na
or
s oe
LA
LA
Ao
esons,
by
or
p an u
p os ve
bo o d
nger p
c u ures
no du es.
and
e
T e
d ag nos s
de n c a on
o
s
131
ac ue
de veopng
90%
r s e
con ras ,
Heart
8
Ao
con r me d
vege a ons
by
e co c ardog rapy.
he
prognoss
depends
on
Adverse
sequeae
e
necng
organsm
and
e
exen L V
o
compcaons.
o
rappng
ncude
gomeruoneprs
due L V
er
11),
o
sepcema,
myocardum
Let
angen–anbody
and
unreaed,
ong-erm
men
(6
necve
weeks
reduce
(e.g.,
necons,
cure
due
o
umaey
or
S.
raes.
For
aerobc
range
n
and
e
generay
cure
erapy
rae
60%
gram-negave
no
o
s
s
bac
aa.
nvovng
98%,
or
underyng
Approprae
vave
repace-
Nor mal
Dilated
cardiomyopathy
ow-vruence
and
or
owever,
ung,
Cap-
embozaon.
and/or
90%;
(see
e
sysemc
necons
rom
gomeru
nvason
anboc
v rdans),
raes
(rom
sysem),
endocards
more)
moray
organsms
ons
arryma
conducon
compexes
S.
aureus
w
a
o
nec-
paens
succumb.
LA
LA
Ao
Nonbacterial
Thrombotic
Ao
Endocarditis
Nonbaceria romboic endocardiis (NBTE) is caracerized by e
deposiion
of
sma
(1
o
5
mm),
serie,
nondesrucive
romboic L V
L V
masses on cardiac vaves
Prevous
occurs
on
vavuar
(Suppemena
damage
prevousy
s
norma
no
a
vaves.
eFg.
8.3).
prerequse.
Dseases
Indeed,
assocaed
ypcay
w
genera
deby or wasng are assocaed w an ncreased rsk or NBTE, as are
ypercoaguabe
saes
(e.g.,
cronc
dssemnaed
nravascuar
coaguHyper trophic
Restrictive
cardiomyopathy
cardiomyopathy
aon, yperesrogenc saes, and underyng magnances, parcuary
mucnous
adenocarcnomas)
and
endocarda
rauma
(e.g.,
ndweng Fig.
caeer).
he
oca
efec
on
e
vave
s
usuay
rva,
bu
embo
8.16
opathy
NBTE
esons
can
cause
narcs
n
e
bran,
ear,
and
oer
The
leads
esons
aso
ncrease
e
rsk
o
necve
endocards.
changes
ness.
CARDIOMYOPATHIES
These
that
diseases
may
cardiac
be
characterized
coned
to
manifestation
Incuded
are
are
among
necous,
AND
e
the
of
a
mmunoogc,
by
cardiac
systemic
disorder
dseases
meaboc,
myocyte
(primary)
a
and
ead
dysfunction
or
may
be
•
ose
myopaes,
a
wc
are
can
nonnlammaory
be
urer
in
Ao,
cardiomyopathies
atrial
aorta;
o
genec
myocye
a
no
subdvded
e
no
hose
caegory
ree
more
o
skeeon
a
resu
o
or
cardo-
ess
•
are
Hyperropc cardomyopay
dagnoss,
•
Resrcve cardomyopay
•
cardomyopay
eas
s
mos
common
and
Dilated
cardiomyopathy
dilation
and
contractile
is
•
characterized
by
progressive
gressed
o
by
dagnoss,
end-sage
myocarda
daed
A
dsease
conracy.
cardomyopay
envronmena
marked
he
can
as
L V,
in
diastolic
dilation
left
by
ear
naed
oows:
a
by
aure
as
usuay
secondar y
cumnaes
nered
n
o
pro-
poor
end-sage
abnormaes
or
n
and
dysfunction.
in
ventricular
Note
and
wall
the
thick-
ventricle.
over
domnan
•
commony
e
50
genes
ave
nerance.
nvoved,
B
and
myocardum
n
wc
cardomyopay
nlammaon
can
o
daed
suc
aso
or
unceran
cardomyopay
damage
be
exposures,
cardiomy-
restrictive
been
Genes
mpcaed,
a
encode
ypcay
by
muaons
a
s
oer
o
enerovruses
end-sage
necous
ave
been
are
daed
myocards
as
documened.
occason-
cardomyop-
By
progressed
e
me
o
absen.
as
cause
cardomyopay,
doxorubcn
daed
and
by
unknown
reaed
mecansms.
cemoerapeuc
cardomyopay.
Perpartum cardomyopaty. Daed cardomyopay occurs ae n
gesaon
cardiac
dysfunction.
daed
n
agens,
paens
Pathogeness.
Dilated
whereas
Acoo and oter toxns. Rarey, acoo abuse s assocaed w e
Toxc
common.
(systolic)
mos
deveopmen
and
Cardiomyopathy
Muaons
nsances
daed
drugs,
Dilated
atrium;
Coxsackevrus
•
cardomyopay
left
result
ventricular
auosoma
deeced
o
resrcve
cardiomyopathy.
dysfunction,
oss-o-uncon.
Infecton.
ay
ds-
n
ay,
daed
LA,
cases.
Daed cardomyopay
paerns,
and/or
w
•
ese
of
cyoskeea proens or proens a nk e sarcomere o e cyo-
dysuncon
dsorders.
50%
usuay
(secondary).
nc uncona and paoogc paerns (Fg. 8.16 and T abe 8.3):
O
forms
systolic
Inerted gene defects. Daed cardomyopay s eredar y n 20%
o
a
are nlammaory n naure are generay consdered orms o myocards,
wereas
to
MYOCARDITIS
myocardium
dverse
major
primarily
organs. hypertrophic
NBTE
three
rom
severa
and
may
weeks
be
sponaneousy
o
mons
muacora.
recover
posparum.
he
Approxmaey
norma
eoog y
a
o
s
ese
uncon.
Iron overoad. Daed cardomyopay can be seen n e seng o
eredar y
mupe
on
n
e
speces.
emocromaoss,
red
ce
ear
ransusons
and
cronc
due
o
ron-medaed
nefecve
njur y
emaopoess,
caused
producon
o
by
ron
reacve
or
depos-
oxygen
CHAPTER
8
Heart
t
C
A
Supplemental
botic
eFig.
vegetations
showing
bland
thrombus
is
8.3
along
thrombus,
only
Nonbacterial
the
loosely
line
with
of
virtually
attached
thrombotic
closure
to
no
the
of
the
endocarditis
mitral
inflammation
cusp
(arrow).
valve
in
(NBTE).
leaflets
the
valve
(A)
Nearly
(arrows).
cusp
(c)
or
(B)
the
complete
row
Photomicrograph
thrombotic
of
of
deposit
throm-
NBTE,
(t).
The
131.e1
132
CHAPTER
Table
8.3
Heart
8
Cardiomyopathies:
Functional
Patterns
and
Causes
Secondary
Functional
Left
Ventricular
Pattern
Ejection
Dilated
70
Here,
rey
dencaon
emaopoec
derved.
are
cnca
Saes.
we
numerous
norma
umors
a
crera,
enes
o
wde
abou
sysems
markers
recognzed
wc
are
moecuar
proen
dsorders
ave
occur
ere
Casscaon
compexy
(e.g.,
er
speen
acvae
nodes
magnances
w
mmuny
rsng
rauma,
nonmcroba
mporan
o
T-cell
a
n
wn
oten
aggregae,
dagnosed
e
neced
mos
expresson o vral proens and perss or e le o e paen. In paens
deecve
dagnoss
w
(e.g.,
vr-
magnan,
ese
maness
presenaons
vrus
he
nae
regons.
acvaed
o
neced
smuae
casscay
aypca
e
(3)
mnor
ces)
necross),
persss n aen orm. Severa EBV-encoded proens expressed n aeny
ces
and
resoves
NEOPLASTIC ons,
bu
ncrease
ympadens,
necons),
spreads
he
Mononuceoss
ympadens
bu
en
no
and
cancer
caseous
o
Lymphadenitis
Inecons
sava conanng vrus. EBV may rs nec oroparyngeal epelal cells,
neced.
gron
ympocyes.
ympadens,
mononuceoss
canges
T ransmsson
and
popuaon
mmune
seng ony abou 20% o ose wo are neced connue o sed e vrus.
Pathogeness.
aypca
(Monospo
angens.
Epsen-Barr vrus (EBV), a member o e erpesvrus amy, s ubq-
cdood
axary,
expanded
ures: (1) aypca ympocyoss; (2) a posve eerop anbody reac-
uous n uman popuaons. In ower-ncome counres, EBV necon n
eary
by
Features.
and
epas)
Infectious
cervca,
an
nec-
ous mononuceoss, wc gves rse o a dsncve syndrome assoc-
w
poseror
conan
T ces a may mmc ympoma. he speen s usuay enarged and
infection
eukema
e
nodes
virus)
nraed
enoug
n
brucellosis)
we
a
o
aberraons.
as
and
coun),
mmune
ocus
on
on
morpo-
neage-spe-
he
number
relecng
sysems
reavey
e
rom
common
148
CHAPTER
Table
9.6
Acute
Hematopoietic
9
Leukemias
Entity
B-cell
and
Cell
acute
lymphoblastic
of
Myeloid
and
Lymphoid
Neoplasms
Origin
Immature
B
Systems
Salient
cell
Pathologic
Marrow
leukemia
Features
replacement
blasts,
absence
of
by
Commonly
lymphoid
Auer
rods
form
(subset
acute
lymphoblastic
Immature
T
cell
Marrow
leukemia
replacement
blasts,
absence
frequent
Acute
myeloid
leukemia
Hematopoietic
myeloid
stem
cell
or
early
Marrow
progenitor
of
mediastinal
often
with
lymphoid
Auer
replacement
blasts,
by
rods,
of
molecule
rods
syndrome
Hematopoietic
myeloid
stem
cell
or
early
Dysplastic
progenitor
marrow
peripheral
blood
and
Genes
elements
myeloid
leukemia
Hematopoietic
stem
cell
Increased
marrow
precursors
and
leukocytosis,
granulocytic
vera
Early
myeloid
progenitor
Increase
in
all
myelofibrosis
Early
myeloid
progenitor
Increased
cytes,
aly,
or
cncopaoogcay
emaoogc
or
eary
marrow
pasms,
immature
elements,
Acue
(T-ce
(acue
o
enes.
orgnae
e
wc
acue
are
n
We
w
rs
emaopoec
eukemas
summarzed
and
n
are
a
diverse
hematopoietic
leading
to
eukemas
(B-ce
acue
o
arres
a
major
umor
eary
bock
n
bass.
o
B-
or
popuaon
n
T-
n
neoplastic
to
replace
dferenaon
presence
o
a
eas
mmunopenoypc
mas aso ave
B-ALL
dence
s
s
or
factor
genes,
(e.g.,
by
RARA);
signaling
genes
epigenetic
factors,
regulators,
and
transcrip-
factors
tyrosine
kinase,
fusion
in
the
form
of
in
the
JAK2
tyro-
in
the
JAK2
or
gene
elements,
atypical
marrow
Activating
sine
megakaryo-
fibrosis,
Activating
splenomeg-
tyrosine
leukoerythroblastosis
in
mutations
kinase
the
gene
mutations
kinase
CALR
genes;
MPL
mutations
gene
ces
neo-
ALL
ce
proliferations
normal
marrow
or
and
mmaure
ere
s
a
ssues.
B-ce
umors
myeod
umors
compee
In
no
T-ce
neopasc
dferenaon
of
marrow
failure.
B-ALL),
T-ALL),
he
nvoved
oten
mos
beween
ncompee
e
ng
sympoms
marrow
ages
and
cyopasm
man
sma
mos
nvoves
marrow
na
cay
e
and
ces
are
mauraon
bass
conras,
and
n
dagnoss
aure,
masses
nuceo
denca
o
as
more
due
2
and
o
o
(Fg.
an
o
bood.
are
AML
s
e
e
based
I
(weakness,
(necon).
w
w
amos
e
a
as
9.11
Acute
and
bass
ney
er
nc-
arses
resu-
rom-
mucosa
ave
scan
spped
cro-
9.11A).
as
a
o
bone
adoescence
marrow.
T-ALLs
nvovemen.
B-ALL
and
can
In
presen
Bass
ony
be
and
addon
w
are
oten
o
medas-
morpoog-
dsngused
occurs
oder
an
Unke
leukemia
TdT,
small
(ALL).
terminal
nucleoli,
and
Lymphoblasts
deoxynucleotidyl
scant
agranular
with
cyto-
transferase.
myeod
neopasm
myeodyspasc
prodrome
o
asng
marrow
bass
and
amouns
9.12A).
In
ave
a
(Fg.
mmaure
subse
bass
Lke
o
In
w
cases,
ey
oer
are
morpoogcay
ALL,
bass
ncusons
9.13).
myeoproerave
descrbed
croman,
c yopasm
a
a
years.
Myeod
ne
neede-ke
bass
or
aure.
o
(eer
syndrome,
end
ese
o
o
sympoms
be
arger
nuceo,
granues
are
neopasm
somemes
numbers
ake
o
e
and
dsngus
mmunopenoypng
or
a
ater
a
reaed
ympod
moderae
granues
e
bass
are
an
orm
paognomonc
nsances,
dcu
and
mos
dsnc
varabe
a
aer),
o
or
(Fg.
Auer
myeod
AML
rom
s
o
are
so
ympod
necessar y
or
dagnoss.
Pathogeness. Among e mos common drver muaons n a ypes o
rougou
60.
shown.
chromatin,
by
mmunopenoypng.
A ML
are
rods,
durng
e
plasm
nuclear
oows:
aways
ague),
lymphoblastic
on
euke-
peak
eemens,
skn
he
decae,
acue
eaures,
marrow
no
Beyond
myeod
eukema,
norma
presens
we
or
and
years.
beeds
nuce
ymc
ose
10
anema
[sma
commony
marrow
T-ce,
cncopaoogc
repaces
and
ymus,
e
cdood
neuropena
basopc
and
o
reaed
and
n
B-ce,
dsnc
(peecae
membranes]),
T-ALL
bass
common
e
wn
n
20%
dferences,
somewa
e
bocyopena
•
often
genes
splicing
BCR-ABL
basophilia
condensed
•
by
splenomegaly
marrow
Fig.
•
often
9.6
mmunopenoype
eukema,
AML).
Typcay,
sages
by
eukema,
or
of
often
related
ympobasc
eukema,
ce
that
subcassed
ympobasc
as
group
cells
symptoms
are
acue
myeod
reerred
e
genes,
signaling
consder
sem
myeod
Tabe
in
gene
Leukemias
leukemias
umors
a
progenors,
caracerscs
Acute
Acute
dsncve
magnances
and
fusion
by
kinase,
basophilia,
polycythemia,
Primary
ABL
megakaryocytes,
thrombocytosis,
Polycythemia
factor
encoding
RNA
tion
Chronic
BCR-ABL
translocations
progenitors
often
tyrosine
cases)
Transcription
molecule
Myelodysplastic
a
Genes
genes,
ABL
translocations;
myeloid
Auer
of
Transcription
involvement
by
factor
translocations;
the
T-cell
Mutated
T ranscription
e
ALL,
bu
s
AML
mos
oten
common
arses
n
rom
a
ndvduas
preexsng
acue eukema are gene rearrangemens and base par subsuons a
nerere
w
e
uncon
o
ranscrpon
acors
a
reguae
norma
CHAPTER
9
Hematopoietic
(>100,000
aways
ces/μL)
presen,
Neuropena
•
and
bu
and
s
Lymphoid
e
w
cyomer y.
somemes
paee
coun
norma.
usuay
149
Anema
s
beow
s
amos
100,000/μL.
common.
Immunopenotypng.
ormed
s
Systems
Denve
anbodes
For
o
exampe,
dagnoss
neage-specc
deecon
o
rees
on
angens,
ermna
sans
usuay
per-
by
deoxyrbose
low
rans-
erase (TdT) s useu or denyng earer B and T ce progenors.
Hsocemca
seen
•
n
acue
Cytogenetcs.
subypes
deny
•
o
sans
aso
be
used,
eukema.
Specc
ransocaons
acue
eukema,
erapeuc
Moecuar
may
myeod
ave
ncudng
are
myeoperoxdase,
assocaed
prognosc
w
parcuar
mporance,
and
may
are
now
arges.
Genetcs.
Ceran
orms
o
acue
eukema
dened by e presence o drver muaons n specc cancer genes.
Mos
acue
eukemas
sequencng. Fig.
9.12
nuclear
Acute
myeloid
chromatin,
leukemia
prominent
(AML).
nucleoli,
and
Myeloblasts
fine
with
azurophilic
are
o
are
em
curreny
are
evauaed
dscussed
by
argeed
DNA
aer.
delicate
cytoplasmic
Clncal granules
Some
Features.
Acue
eukema
s
an
aggressve
dsease.
In
addon
shown.
o
sympoms
opena,
•
reaed
ere
B one
pan
may
o
marrow
repacemen
and
e
aendan
pancy-
be
resung
rom
marrow
expanson
and
nraon
o
e
subperoseum
•
Lympadenopay,
mon
and
more
In
T-ALL
C enra
w
promyelocytic
leukemia,
abnormally
a
variant
coarse
and
of
AML.
The
numerous
dfer
and
T-ALL
characteristic
finding
is
a
cell
in
the
center
of
the
field
Auer
wo
of
rods
(arrow).
Pathology,
(Courtesy
University
of
of
Dr.
Texas
Robert
with
W.
mos
caracersc
o
AML
w
sysem
compresson
manesaons
eadace,
acue
ALL
are
nvovemen,
o
arge
vesses
medasnum
eukema
w
and
cured.
vomng,
and
vares
combnaon
AML.
Hgy
More
resung
ner ve
rom
accordng
o
cemoerapy
an
efecve
80%
o
argeed
menngea
pases
subype.
usng
cdren
erapes
Mos
regmens
w
are
B-ALL
avaabe
moecuar
subypes
by
e
o
acue
presence
o
a
eukema:
BCR-ABL
(1)
BCR-ABL–postve
uson
gene
(descrbed
multiple
dea
under
cronc
myeod
eukema)
and
(2)
acute
promyeocytc
McKenna,
Southwestern
a
dsncve
subype
o
AML
caracerzed
by
e
presence
o
Medical
a School,
as
o
dened
eukema, Department
gums,
neo-
n needle-like
ymc
reaed
or
and
granules.
B-ALL, A
are
skn
e
ner vous
a
or have
n
suc
Treamen
paens
e
com-
dferenaon
ar ways
spread,
Acute
o
more
AML
Inraon
•
promyelocytes
epaomegay,
an
Tescuar enargemen due o eukemc nraon
and
9.13
and
ALL
•
•
plastic
n
•
monocyc
Fig.
spenomegay,
pronounced
(15;17)
ransocaon
a
creaes
a
PML-RARA
uson
gene
encodng
Dallas.)
an
aberran
orm
o
e
renoc
acd
recepor
a
bocks
ermna
d-
erenaon o promyeocyes. hs orm o acue eukema s now amos
emaopoec ce dferenaon. hese muaons ypcay nvove ac-
aways cured w argeed reamen conssng o a-trans renoc acd,
ors
a vamn A anaog a bnds e PML-RARA uson proen, combned
a
reguae
e
neage
o
wc
e
eukema
beongs.
For
exam-
pe, B-ALL oten conans muaons n ranscrpon acors requred or
w
eary
reamen
sages
arres
ead
o
genes
o
and
o
B-ce
accumuaon
grow
o
sgnang
ncudng
severa
hese
mmaure
acor–ndependen
encodng
RAS,
dferenaon.
bass.
sgnang
moecues
grow
muaons
a
acor
ac
cause
Muaons
and
n
mauraon
oer
genes
proeraon. RAS
upsream
recepors,
are
and
and
downsream
oten
muaed.
arsenc
neurops,
a
combnaon
•
he
o
Mor poog y.
marrow,
gy
and
compemenar y
Bass
aoug
dagnoss,
are
dagnoss
can
bopsy
parcuary
varabe.
be
he
n
subypng
acue
eukema
requres
n
o
ssue
a
T-ALL.
ce
e
mass
he
coun
bood
may
perpera
may
be
be
and
bone
requred
bood
markedy
or
e
degradaon
rapdy
reamen
de,
o
o
mmaure
cearng
B-ALL
e
w
o
PML-RARA.
ces
neopasc
cyooxc
T
hs
presumaby
cone.
ces
A
no
recen
bearng
c-
ces
expressng
responses
e
n
B-ce
angen
CD19.
reapsed/reracory
hs
B-ALL
erapy
n
as
cdren
produced
and
adus,
bu a e cos o permanen oss o norma B ces and somemes severe
or
perpera
s
cause
dferenaon
merc angen recepors (CARs) engneered o speccay recognze and
k
ess:
seen
we
o
wc
e
wc
deveopmen
dramac
Pathology.
sas,
nduces
even
aa
acvaed
oxcy
njeced
Caenges
ndngs
rangemens
eevaed
encodes
an
o
T
caused
ces
reman.
e
by
Inane
KMT2A
epgenec
producon
(cyokne
acue
gene
reguaor,
o
cyoknes
by
e
massvey
sorm).
eukemas
(prevousy
ave
a
poor
assocaed
known
as
prognoss.
w
MLL),
he
rear-
wc
prognoss
150
or
CHAPTER
adus
or
w
paens
kema
w
BCR-ABL–negave
w
remans
parcuary
TP53
poec
AML
poor,
subypes
caengng
ce
probem
wc
ALL
oer
parcuary
muaons,
sem
Hematopoietic
9
n
s
ave
s
guarded,
an
adus
e
acue
oder
sma
dsma
and
and
e
prognoss
promyeocyc
an
subse
oucomes
Lymphoid
o
age
60
acue
even
eu-
years.
A
Systems
argeed
cay
erapy.
dsnc
prmar y
s
a
arge
emao-
dene
AML
ons).
hese
(>20%
I
(MPNs;
afecs
n
myeod
bass
and
a
syndrome
dscussed
abou
ncreasng
o
neopasms
myeodyspasc
pasms
Syndromes
group
Chronic
Myeloid
Chronic
myeloid
15,000
specc
no
aer).
as
wo
(MDS)
e
ack
e
AML-denng
and
per
a
broad,
MDS
paens
requency
derived
neopasms
e
s
n
popuaon
drver
as
e
common
Uned
a
ABL
mua-
groups,
myeoproerave
neary
year
eaures
overappng
dscuss
CML
and
wo
neopasms,
oer
cncopaoog-
poycyema
vera
and
myeobross.
liferative
here
w
eukemas
w
ranspanaon.
Myelodysplastic
We
myeoproerave
as
Saes
e
neo-
he
e
neoplasms
from
gene
(CML)
by
portions
on
o
e
is
the
of
BCR
ave
DNA
smar
of
gene
a
on
from
other
BCR-ABL
myelopro-
fusion
chromosome
22
gene
and
the
9.
breakpons
BCR-ABL–posve
bu
distinguished
presence
the
chromosome
posons
and
ways
Leukemia
leukemia
B-ALL
downsream
n
cronc
(descrbed
myeod
earer)
eukema
dfer
n
sub-
consequences.
AML.
and
s
ages.
Pathogeness.
proen
n
he
wc
BCR
e
ABL
ABL
gene
ound
yrosne
n
knase
CML
becomes
encodes
a
cmerc
consuvey
acve
because o uson o par o e BCR proen and mmcs sgnas produced
Pathogeness. MDS s caracerzed by mauraon deecs assocaed w
by
nefecve
dferenaon, e eary dsease course s marked by excessve producon
emaopoess
and
a
g
rsk
o
ransormaon
o
AML.
he
marrow s pary or woy repaced by e cona progeny o a ransormed
mupoen
neage
sem
ce
a
dferenaon.
demonsraes
he
marrow
s
nefecve
and
yperceuar
or
dsordered
cdren
muaed
ng
cancer
agens
appears
and
or
o
be
young
gene
or
onzng
caused
adus,
exposure
radaon).
by
MDS
o
In
sporadc
s
oten
muagens
adus
muaons
n
e
acor
recepors.
Because
BCR-ABL
does
no
nb
o reavey norma bood ces, parcuary granuocyes and paees.
normoceuar,
bu
Morphology. he eukocye coun s eevaed, oten exceedng 100,000
due
(e.g.,
over
grow
mu-
e perpera bood sows one or more cyopenas.
In
acvaed
o
erapeuc
age
cancer
nerance
o
60
genes.
o
a
akya-
years,
MDS
T ransorma-
ces/μL,
due
eosnops,
as
o
e
and
meamyeocyes
aso
requeny
and
o
ncreased
we
as
myeocyes
eevaed.
(Fg.
marrow
s
numbers
o
9.14).
he
orms
paee
yperceuar,
and
and
oer
sgnang
moecues.
In
addon,
rougy 10% o MDS cases ave oss-o-uncon muaons n TP53; ese
be
spenc
emaopoess.
e
I
suc
coun
s
speen
suppy canno keep up w e massve spenomegay, e resu may
RAS
exrameduary
neurops,
granuocyc
s
n
by
he
earer
suc
muaons
enarged
as
on o AML s assocaed w addona muaons a drve ce grow,
as
markedy
presence
basops,
e
bood
narcs.
paens ave parcuary poor cnca oucomes.
Clncal
Morphology.
a
he
exb
marrow
s
popuaed
dsordered
“megaobasod”
megaobasc
emaopoec
dferenaon
eryrod
anemas,
by
precursors
eryrod
(dyspasa),
resembng
orms
precursors
w
ron
ose
ncudng
seen
deposs
n
wn
e
er
are
Features.
nonspecc.
ura
sor y
o
cases,
crss
e
bas
B-ALL,
granues
mupoen
nucear
mauraon,
and
sma
megakaryocyes
w
snge
sma nuce or mupe separae nuce.
onse
varabe,
ransormaon
mocondra (rng sderobasts), granuocye precursors w abnorma
or
s
he
wc
o
Spenomegay
s
bu
acue
CML
may
unreaed
eukema
resembes
conssen
emaopoec
s
be
s
(so-caed
e
n
and
eares
CML
AML;
w
sem
nsdous
e
dea
evenuay
bas
e
na
CML
he
aa
crss).
remander,
a
sympoms
sympom.
In
na-
due
o
70%
o
resembes
orgnaes
rom
ces
T argeed erapy as dramacay aered e dsease course. Tyrosne
knase nbors a arge e BCR-ABL uson proen nduce susaned
remssons
Clncal
Features.
cyopenas,
ss
rees
on
Mos
necons,
e
paens
anema,
presence
o
are
and
50
o
70
beedng
cyopenas
and
years
are
o
age.
As
common.
caracersc
a
he
resu
o
ease.
he
and
preven
bas
crss,
BCR-ABL–posve
cone
parcuary
persss,
n
and
paens
paens
w
mus
eary
be
ds-
reaed
dagno-
morpoogc
and genec ndngs. Cyogenec sudes oten revea cona abnorma-
es;
oss
o
common.
a
majory
o
MDS
s
panaon.
dcu
and
poron
o
o
cromosomes
sudes
rea;
mos
w
me
does
paens
T ransormaon
survva
assocaed
a
sequencng
5
deny
and/or
drver
7
s
parcuary
muaons
n
e
cases.
cemoerapy,
medan
or
DNA
o
ranges
ncreased
are
AML
rom
marrow
no
oo
respond
od
occurs
9
o
29
bass,
o
n
we
o
undergo
10%
mons
o
40%
and
cyogenec
convenona
sem
s
o
ce
rans-
cases.
worse
n
he
cases
abnormaes,
or
TP53 muaons.
Myeloproliferative
The
common
Neoplasms
pathogenic
feature
of
myeloproliferative
neoplasms
is the presence of mutated, constitutively activated tyrosine kinases
or
other
acquired
aberrations
in
signaling
pathways
that
lead
to Fig.
growth
factor
9.14
Chronic
myeloid
leukemia:
peripheral
blood
smear.
Granulo-
independence. cytic
forms
at
various
stages
of
differentiation
are
present.
(Courtesy
of
hese dverse myeod magnances are rare bu are noabe because Dr.
o
e
remarkabe
response
o
cronc
myeod
eukema
(CML)
o
Robert
W.
Southwestern
McKenna,
Medical
Department
School,
of
Dallas.)
Pathology,
University
of
Texas
CHAPTER
or
e.
Reapses
somemes
occur,
oten
due
o
ougrow
o
cones
9
Hematopoietic
n
BCR-ABL
a
preven
nbors
rom
bndng.
In
remssons
can
be
obaned
by
swcng
o
dferen
a
he
s
marrow
seen
are
acve
agans
parcuar
muaed
orms
o
BCR-ABL.
151
appearance
occasonay
s
ae
denca
n
e
o
e
course
spen
o
oer
nbors myeoproerave
a
Systems
some pase
nsances,
Lymphoid
w Morphology.
muaons
and
For
neopasms
suc
as
PCV .
Inay,
e
marrow
s
oers, yperceuar
and
mdy
dsored
by
bross.
Megakar yocyes
are
emaopoec sem ce ranspanaon ofers a cance o cure. arger
an
marrow
Polycythemia
Vera
Polycythemia
vera
s
norma
exrameduar y is
a
myeloproliferative
disorder
marked
production
of
all
myeloid
lineage
cells
and
markedy
to
increased
red
cell
mass
and
n
cusers.
dfusey
emaopoess
In
advanced
broc,
occurs.
he
and
cases,
e
compensaor y
abnorma
(Fg.
9.15).
Red
perpera
ces
exb
bood
bzarre
smear
sapes,
symptoms and
related
presen
by s
increased
and
ypoceuar
nuceaed
er yrod
precursors
are
commony
seen,
aong
(polycythemia). w
a
mmaure
we
combnaon
o
ces
ndngs
(myeocyes
reerred
o
and
as
meamyeocyes),
eukoerytrobastoss.
Pathogeness. Poycyema vera (PCV) s assocaed w acvang pon Abnormay muaons
n
e
yrosne
knase
JAK2,
a
sgnang
moecue
n
arge
paees
are
oten
presen.
Marked
spenomegay
paways due
o
exensve
exrameduar y
emaopoess,
oten
assocaed
downsream o e eryropoen recepor and oer grow acor recepw
subcapsuar
nfarcts,
s
ypca.
he
speen
may
weg
up
o
ors. he JAK2 muaons reduce e dependence o emaopoec ces on 4000 g, rougy 20 mes s norma weg. Moderae epatomegay, grow acors or grow and survva, eadng o excessve proeraon o aso
due
o
exrameduar y
emaopoess,
s
commonpace.
eryrod, granuocyc, and megakaryocyc eemens.
Clncal
Features.
Prmar y
myeobross
usuay
occurs
n
ndvduas
Mor pholog y. he marrow s yperceuar due o ncreased numbers oder
o
er yrod,
myeod,
and
megakar yocyc
orms.
Marrow
an
60
years
seen
n
10%
o
paens
a
dagnoss.
hs
can
progress
o
a
were
e
marrow
s
repaced
by
brobass
and
bood
o
voume
many
and
vscosy
ssues.
Paees
due
are
o
poyc yema
oten
may
be
dysuncona,
eadng
o
romboss
are
oten
ncreased
n
e
perpera
and
norma
Sympoms
oms,
PCV
ncude
cyanoss,
emaemess,
areres
and
can
appears
and
ead
o
nsdousy,
eadace,
meena.
sroke,
dzzness,
myocarda
n
ae
mdde
gasronesna
may
nvove
narcon,
and
age.
symp-
vens
or
pumonary
embosm. Epsaxs s common, and e-reaenng emorrages occur
n
5%
n
5%
o
10%
o
paens.
Because
o
e
g
he
10%
o
ce
urnover,
gou
s
greaer,
on
o
W ou
w n
ab ou
or
10
ye ars
o
n
mos
AML
are
leads
a
sp en
a er
re a
bu
of
and
gou
sudes
by
due
sow
o
a
a
g
rae
moderae
are
o
o
eukoer yrobasoss.
mdy
coun
rombocyopena
he
reduced
s
romboss
n
5%
o
oten
myeobross
medan
sur vva
and
20%
spenomegay
o
s
4
beedng,
cases.
and
ranspanaon
requen
and
com-
ce
urnover
severe
are
normocyc
bu
can
he
be
we
eevaed
ce
coun
eary
n
usuay
norma
or
eevaed
a
e
dagnoss,
s
super venes
more
o
5
and
JAK2
years.
be
e
o
o
ransormaon
are
dsease
rea
hreas
nbors
consuona
may
as
dcu
an
e
o
PCV
and
ncude
AML,
efecve
sympoms.
progresses.
a
CML.
necon,
wc
occurs
decreasng
Hemaopoec
sem
e
ce
curave.
Lymphomas
and
Chronic
Lymphoid
Deec-
o
comp c a ons
me
emao c r
as
o
ner va
pas e
a
and
b as
re quen y
s
ne ar
e ad
cr s s
an
nor ma
a
hese
common
10
o
by
pomas
rom
and
are
Fig.
9.15
derved
pasma
maure
and
emaoogc
are
ce
maure
neopasms
ympocyes,
dscussed
magnances
rom
bu
and
ave
ncude
ympod
reaed
unque
a
wde
ces.
enes
varey
Hodgkn
are
aso
cncopaoogc
o
ym-
derved
eaures
aer.
myeo -
ye ars .
JA K2
mprovemen
den c a
n
o
a
prop ens y
pr mar y
o
o c c urs
nc re as e d
re ve a e d
res emb ng
average
Leukemias
neopasms
sur v va
sur v v a
sp en
ess
rombocyoss.
vas c u ar
pas e
an
e
muc
primary
brosis,
cytopenias
ncrease
acor
sweas
o
a
o
CML.
Myelofibrosis
Pathogeness.
a
e
Trans or ma on
o cc urs,
marrow
to
o
o
and
dagnoss.
me d an
Proonge d
aer)
us e d
hallmark
erative
o
e
rom
e
ower ng
e vove
p a ens.
a s o
Primary
The
by
basopa,
d e a
owe ver,
(des cr b e d
n bors
w
conrms
re a men,
p eb oomy.
PCV
bross
muaons
mon s;
rep e ae d
ng
paens.
granuocyoss
JAK2
and
seen
Common aboraor y ndngs ncude a emaocr a s oten 60%
or
or
paee
Non-Hodgkin o
oss,
bood.
usuay
hromboses
anema
beedng.
Prmar y
Features.
weg
Laboraor y
accompaned
usuay
bu
Clncal
o
arge
course.
Basops
reaed
cause
abnormay
s
and
Fague,
Hyperurcema
seen.
anema
congeson
sympoms
coagen. oten
Increased
w
spent pans.
pase,
presen
bross spenomegay.
s
wo
and
Prmar y
he
reduces
extensive
sgnang,
mos
requen
is
the
development
marrow
a
o
s
caused
paway
ese
of
oblit-
hematopoiesis
extramedullary
myeobross
JAK/STAT
recepors.
myelobrosis
which
by
varous
muaons
downsream
are JAK2
and
hematopoiesis.
o
grow
muaons,
wc
are presen n 50% o 60% o cases. I s no known wy JAK2 muaons
are
n
assocaed
oers.
w
Fbross
PCV
s
n
some
caused
by
paens
and
prmar y
pro-brogenc
acors
myeobross
suc
as
grow
acor
and
TGF-
a
are
eaboraed
by
Primary
precursors
megakar yocyes.
TGF-
promoes
angogeness
as
we
as
bo
o
wc
are
promnen
n
myeobroc
peripheral
several
blood
smear.
teardrop-shaped
red
Two
cells
nucleated
are
myeloid
cells
were
present
in
other
fields.
An
evident.
identical
histo-
coagen logic
deposon,
and
neopasImmature
c
myelofibrosis:
paeerythroid
e-derved
marrows.
and
picture
fibrosis.
can
be
seen
in
other
diseases
producing
marrow
distortion
152
CHAPTER
Hematopoietic
9
and
Lymphoid
Some genera aspecs o magnances o maure ympod ces bear
empass:
•
e
erms
sue
eukema
nvovemen.
apparen
n
Leukemas
perpera
refer
ypcay
bood,
o
arse
wereas
e
n
usua
bone
ympomas
paerns
marrow
presen
of
s-
and
are
as
Wesern
masses
e
CLL,
word.
Pathogeness.
paen
wc
For
s
dagnosed
uncear
CLL/SLL
“ympomas”
and
nvovemen.
n
ve
n
for
dagnoss
o
e
s
as
perpera
masses,
based
umor
on
ces,
bood
wou
e
nvove-
perpera
morpoogc
regardess
o
er
and
oca-
neopasms
sysem;
oten
dsrup
mmunodecency
e
and
funcon
of
e
auommuny
s
mos
an
w
o
or
acqured
neopasms,
mmunodeicences
parcuary
ose
are
assocaed
at
unema
EBV
pocyes
sowy
s
ess
ympoma
recrcuae
by
a
umors
because
oten
ke
are
are
appears
norma
dagnoss.
erapes
B-ce
o
be
ocazed,
ympocyes
hereore,
w
and
ew
neopasc
umors
are
umor
and
Many
ons
he
excepons,
ym-
a
ony
muc
muaons
use
pod
eukemas
mned
by
secons,
common
and
an
muaons
mporan
enes
ncrease
n
B-ce
mmunogobun
o
T-ce
reaed
consders
presence
w
o
ocus
vra
on
(summarzed
a
e
or
umors,
o
o
cnca
a
Tabe
ave
oc
eac
mos
We
bre
acvaon.
o
ransoca-
Chronic
Lymphocytic
Cronc
ympocyc
bood
(SLL)
are
aso
and
ce
o
and
eny.
cronc
orgn
w
e
n
n
e
Asa.
wc
9.7
eukema
e
(CLL)
ouc
because
on
o
dferng
perpera
Characteristics
lymphocytic
Follicular
red
of
ony
bood
sma
ew
e
e
yrosne
NF-κB,
oten
resung
15%
or
knase
o
o
n
(BTK)
and
conrbues
ces.
CLL/SLL
ces
ypogammagob-
deveop
Wen
auo-
presen,
n
e
exen
ympocye
of
o
an
Mature
B
nvoved
an
Features.
s
cell
are
are
a
o
are
caed
sma,
efaced
areas
sma
(see
marrow,
In
w
maure-ookng
and
caed
he
wc
and
ver
CLL,
ere
ympocyes.
requeny
smudge
sees
9.16B).
ceners,
speen,
paens
by
conanng
ympocyes
Fg.
proferaon
he
cases.
are
he
cyopasm
rage
ey
dfusey
-dened
9.16A).
CLL/SLL.
ces
o
aso
he
bood
dagnoss
and
ces
g
can
ymp
course.
s
I
s
based
conrmed
expressng
expressed
prognoss
ndoen
dsruped
on
ces.
on
s
generay
T
kappa
or
good
e
ympocyes
cyomer y,
and
suc
In
wc
as
cona
ambda).
or
CD20,
surace
SLL,
lymphoma
Naïve
mature
B
cell
CD5
mmu-
ssue
bopsy
CLL
usuay
paen
s
oows
a
ver y
asympomac,
marginal
zone
lym-
Mature
B
and
Chronic
in
Lymphoid
Leukemias
Characteristics
older
adults;
blood;
Translocations
Translocations
cell
usually
involves
lymph
nodes,
marrow,
spleen;
and
indolent
involving
BCL2;
presents
with
generalized
lymphadenopathy;
involving
Arises
at
sites
of
the
cyclin
moderately
chronic
D1
gene;
presents
with
generalized
aggressive
inflammation;
very
indolent
phoma
Diffuse
large
B-cell
lymphoma
Germinal
minal
Burkitt
lymphoma
center
center
Germinal
or
B
center
post–ger-
cell
B
Heterogeneous,
translocations
cell
Usually
all
Hairy
cell
leukemia
Mature
B
cell
arises
cases;
Spleen
and
at
may
arise
involving
at
extranodal
subset
of
marrow
extranodal
BCL2,
BCL6,
sites;
cases
and
MYC;
variably
most
with
involving
EBV;
cases
associated
with
aggressive
translocations
associated
involvement;
sites;
MYC
in
virtually
aggressive
have
BRAF
mutations;
indo-
lent
Adult
T-cell
leukemia/lymphoma
CD4-positive
T
cell
Usually
presents
ciated
Peripheral
T-cell
lymphoma
Mature
T
cells
Epstein-Barr
virus;
HTL V-1,
human
T-cell
lymphotropic
with
virus
1.
with
HTL V-1
Heterogeneous;
from
EBV,
e
omac paens are reaed w anbodes agans CD20, nbors o
lymphadenopathy;
Extranodal
n
reveas
dagnoss.
because
wen
ncreased
markers
ces),
requred
dagnosed
on
low
B-ce
norma
(eer
node
by
medan sur vva s greaer an 10 years, even wou reamen. Symp-
Occurs
B
(Fg.
scany
ces
ympocyoss
preparaons;
enarged
Associated
center
n
crcuang
popuaon
peripheral
Germinal
and
acve
nodes
scaered
ces
nuce
mocay
perpera
he
ym-
Lymphomas
cell
and
dvdng
round
absoue
(wc
exceeds
Origin
ymp
amos
a
or
perpera
coun
Invoved
or
Lymphoma
leukemia
lymphoma
cell
e
oerance.
indolent
Mantle
by
sgnas
CLL/SLL
o
paens
paees.
BCR
wc
sur vva
pro-
generaed
BCR).
accumuaon
ces
mmune
paognomonc
e
rare
unusua
ympocyc
Non-Hodgkin
lymphoma/
lymphocytic
Lymphocytic
mpar
aso
Clncal
cncay
a
o
nogobun
and
Cell
chronic
acor
sgnas
or
ce
(e.g.,
oowng
and
ces
acvey
soogc
(deer-
genoype
In
common
menon
Leukemia/Small
Entity
Small
Bruon
approxmaey
own
ympocyes
dark,
hese
ym-
caracerscs.
denca,
nvovemen;
Table
er
are
recepor,
promoe
uncon,
are
o
poma
a
mecansms,
are
s
proooncogenes.
eaures,
o
are
9.7).
conss
sma
arger,
proba-
doube-srand
oncogene
ympomas
morpoog y,
deser ve
normave
rsk
genes
genomes)
ose
n
nevereess
paogencay
e
magnances
non-Hodgkn
mmunopenoypng),
we
genes
B-ce
agans
caed
ranscrpon
Paradoxcay,
CLL/SLL
o
more
cass-swcng)
casscaon
kar yoype,
o
uncear
Morphology.
sys-
curave.
ransocaons
drver
a
e
mporance
B-ce
umor
cr-
n
usuay
DNA breaks n mmunogobun genes (durng somac ypermua-
on
crca
(e
an
e
adus
common
growng
mporan
cases
o
auoanbodes are made by nonmagnan bysander B ces, ndcang
wdespread
emc
o
nermedar y
norma
anbodes
necon.
Aso
on
expresson
hroug
ger
w
an
urn
suppresses
nered
ympod
Atoug
roug
e
coexs
nsances.
w
apoposs.
mmunogobun
more
Mos
eukema
CLL/SLL
ndoen,
s
CLL.
common
reasons,
sur vva
surace
low
adap-
ce
nbs
umaey
ympod
Paens
rsk
he
ave
presen
body.
mmune
some
may
caracerscs
e
Maure
occasonay
“eukemas”
umor
s
e
eraon per se. CLL/SLL ces express g eves o BCL2, a proen a
on
•
or
absoue:
moecuar
•
ces/μL,
era
ncreased
bood
•
ympoma
5000
n ymp nodes and oer ssues. However, ese dsncons are no
men
•
and
Systems
cytokine
lymph
node
infection;
often
associated
release;
and
blood
frequent
with
aggressive
involvement;
hypercalcemia;
systemic
uniformly
asso-
aggressive
symptoms
stemming
CHAPTER
B-ce
recepor
sgnang,
and
BCL2
anagonss.
he
presence
o
9
Hematopoietic
and
Lymphoid
Systems
153
TP53 Morphology.
Lymp
nodes
are
usuay
efaced
by
a
dsncy
muaons porends a worse prognoss. Cure may ony be aceved w noduar emaopoec
sem
ce
ranspanaon,
wc
s
reser ved
or
proferaton
wo
a
convenona
erapes.
A
sma
racon
o
ransorm
o
aggressve
umors
resembng
dfuse
ces
(Rcer
ransormaon);
once
arge
ransormaon
sur vva
me
s
ess
an
1
occurs,
e
predomnan
so-caed
a
centrocytes,
ave
ces
anguar
sgy
“ceaved”
arger
an
nuce
and
near
nodngs,
coarse
condensed
w
croman,
and
e nuceo
(Fg.
9.17B).
Cenrocyes
are
mxed
w
varabe
year. numbers
severa
o
centrobasts,
nuceo,
cenrobass
Follicular
commony,
B-ce
ndsnc medan
are
ympocyes
ndenaons ympoma
Mos
CLL/SLL resng
cases
9.17A).
younger neopasc
paens
(Fg.
and
arger
modes
predomnae,
ces
amouns
a
w
o
eaure
vescuar
cyopasm.
a
croman,
Uncommony,
correaes
w
more
Lymphoma
aggressve cnca beavor. he umor ces express e B-ce marker Follicular
lymphoma
is
strongly
associated
with
a
(14;18)
transloCD20,
cation
that
increases
the
expression
of
the
antiapoptotic
BCL2
and Focuar
ympoma
consues
approxmaey
25%
o
cases
germna
o
g
eves
ympoma
n
e
Uned
Saes,
makng
e
mos
o
B-ce
BCL2.
markers,
Because
surace
BCL2
s
no
mmunogobun,
expressed
n
norma
adu germna
non-Hodgkn
cener
gene.
cener
B
ces,
sans
or
BCL2
ep
dsngus
ocuar
comympoma
rom
ocuar
yperpasa.
mon “ndoen” non-Hodgkn ympoma. Lke CLL/SLL, occurs ess re-
queny n Asan popuaons. he ce o orgn s a germna cener B ce.
Clncal
Pathogeness.
ersc
18
o
14,
(14;18)
e
(see
genes
an
85%
ransocaon
IGH
resung
oss
More
o
a
ocuar
uses
(mmunogobun
n
“overexpresson”
Caper
encodng
1).
In
abou
a
e
eavy
o
rd
o
BCL2
can)
BCL2
sone-modyng
ympomas
gene
ocus
proen,
cases,
proens
an
ave
on
on
carac-
usuay
Features.
Focuar
maness
as
ympoma
paness
afecs
generazed
adus
oder
an
ympadenopay.
50
he
and
mar-
cromosome
row s nvoved a dagnoss n approxmaey 80% o cases. Aoug e
cromosome
naura
nbor
addona
are
a
o
apop-
muaons
n
sor y
buky,
proonged
sympomac
anbodes
seen.
s
(overa
medan
sur vva
s
approxmaey
10 years), e dsease s no curabe; erapy s reser ved or paens w
o
agans
paens,
dsease.
CD20,
ocuar
Treamen
and
BCR
ympoma
ncudes
sgnang
progresses
“gene”
nbors.
o
dfuse
cemoerapy,
In
30%
arge
o
B-ce
40%
ym-
poma (DLBCL). DLBCL arsng rom ocuar ympoma as a worse
prognoss
Mantle
Mantle
an
Cell
cell
location
I
a
increases
ce
are
ces
5).
RB,
A
rom
aso
n
men
Cycn
e
been
or
G
1
marrow
n
an
nvoved
rom
a
50
e
aer.
S
by
e
ympod
trans-
naïve
B
oces.
ympomas
ormng
RB,
o
a
a
compex
promong
e
Addona
and
ce
varey
cyce
e
o
(see
brakng
drver
w
progresson
Cap-
efec
muaons
sgnang
o
ave
moecues,
reguaors.
efaced
by
he
ympocyes
cases
(11;14)
gene.
resembng
norma
over wems
paerns.
nuceo,
an
D1
non-Hodgkn
pase
D1
are
norma
mos
ces
o
grow
encodng
nodes
with
cyclin
years.
epgenec
noduar
n
o
grow.
genes
and
nconspcuous
s
o
the
nacvang
cycn
ce
Lymp
6%
an
and
o
of
zones
smuaes
pase
vaguey
arger
nuceus,
descrbed
associated
derved
mane
oder
D1
acors,
Morphology.
sgy
s
knases
dened
dfuse
strongly
e
ympoma
ranscrpon
n
n
Overexpresson
drvng
DLBCL,
expression
approxmaey
many
cycn-dependen
er
is
ympoma
ound
Pathogenes s.
o
dfuse
Lymphoma
consues
occurs
novo
lymphoma
that
Mane
ces
de
and
and
and
scan
e
umor
umor
ces
ces
ave
an
cyopasm.
perpera
growng
usuay
are
rreguar
he
bood
n
bone
abou
20% o cases. he umor ces express surace IgM and IgD, e B-ce
angen
ndng
Clncal
CD20,
a
s
and
Features.
ay
and
are
row,
speen,
CD5,
and
dagnoscay
Mos
ound
ver,
o
and
ave
paens
ave
g
presen
generazed
(oten)
eves
o
cycn
D1
proen,
a
epu.
e
w
ague
dsease
and
nvovng
gasronesna
rac.
ympadenop-
e
hese
bone
mar-
umors
are
B
moderaey
Fig.
9.16
Chronic
lymphocytic
leukemia/small
lymphocytic
aggressve
and
ncurabe.
T reamen
nvoves
e
use
o
ow-
lymphoma:
dose cemoerapy, anbodes agans CD20, and drugs a nb B-ce
lymph
node.
(A)
Low-power
view
shows
diffuse
effacement
of
nodal
recepor sgnang. he medan survva s 4 o 6 years. architecture.
appearance
(B)
of
At
high
small,
power,
round
a
majority
lymphocytes.
of
A
the
tumor
cells
have
“prolymphocyte,”
a
the
larger
Extranodal cell
(A,
sity
with
a
centrally
Courtesy
of
Texas
of
Dr.
placed
José
nucleolus,
Hernandez,
Southwestern
Medical
also
is
present
Department
School,
of
Dallas.)
in
this
field
Pathology,
Marginal
Zone
Lymphoma
(arrow).
Univer-
Extranodal
that
arises
marginal
within
and
zone
is
lymphoma
sustained
by
is
an
chronic
example
of
a
cancer
inammation.
154
CHAPTER
Hematopoietic
9
and
Lymphoid
Systems
B
A
Fig.
9.17
out.
(B)
outlines
Dr.
Follicular
At
high
lymphoma:
magnification,
(centrocytes)
Robert
W.
are
McKenna,
lymph
small
mixed
node.
(A)
lymphoid
with
Department
a
of
Nodular
cells
with
aggregates
condensed
population
of
Pathology,
University
Exranoda margna zone ympoma s an ndoen umor derved rom
larger
•
angen-smuaed B ces. I occurs mos commony n organs w epe-
a
nngs,
suc
as
e
gasronesna
rac
(so-caed
MALT omas
cells
of
with
B CL6.
pon
sa-assocaed ympod umors]), savary gands, ungs, orb, and breas.
nlamed
due
Hasmoo
gasrs).
o
ympoma
yrods)
o
secreed
by
oug
a
e
H.
or
o
umor
H.
pyor
ces,
dsease
subsequen,
oten
w
begns
as
s-unknown
or
a
on
er
Hecobacter
erapy
grow
oten
and
mmune
muaons,
a
a
are
•
reacon,
neopasc
I
be
o
drve
angen,
grow
suc
as
H.
and
survva.
pyor
Hence,
proens,
wdrawa
causes
umor
o
e
s
MYC.
ssues
he
and
he
cona
coec
cyopasm
dferenaon.
n
may
he
B
ces
sma
be
nrae
abundan
umor
ces
e
aggregaes
In
ons
and
express
epeum
o
nvoved
esons).
pae
e
or
exb
B-ce
pasma
angen
addon
mes
B
en
as
Features.
swengs
ncdenay
n
o
Exranoda
e
e
savary
seng
o
gand,
H.
zone
ympomas
yrod,
or
orb,
pyor–nduced
or
ypcay
are
gasrs.
pres-
dscovered
Unke
oer
non-Hodgkn ympomas, wen ocazed ey are oten cured by smpe
excson
dsease)
oowed
may
by
aso
radoerapy,
compeey
or
regress
(n
n
e
case
response
o
o
H.
pyor-assocaed
anboc
Large
Diffuse
large
phoma,
Dfuse
in
the
arge
common
smuaed
a
Cell
B
ces
demonsrae
genoypc
fo r
adus
and
is
the
mo s t
ap pro xi ma te ly
Un i ted
B-ce
n
c o m m on
35%
of
t y pe
of
States .
ympoma
oder
an
encompasses
subsana
he
o
are
cromosoma
era
dferen
10%
o
a
aberraons
B
ave
resu
ranscrpona
n
reg-
ces.
a
(14;18)
overexpresson
DLBCLs
ave
ranscrpon
ransocaons,
and
a
afec
ransocaon
o
e
anapo-
rearrangemens
acor
numerous
varous
ranscrpon
neopasc
resng
B
ces
a
oer
reguaes
drver
epgenec
acors
are
ympocyes;
Ces
w
dsnc
(Fg.
vescuar
arge,
a
a
owever,
ova
nuceo,
predomnae
muobae
mua-
reguaors,
ave
mporan
nucear
and
eas
ere
or
nuceus,
e
one
our
dspersed
amouns
ces
or
o
consderabe
conours,
modes
9.18),
ree
s
o
may
wo
pae
ave
a
promnen
e
umor
ces
are
anapasc
and
ncude
umor
gan
ces resembng Reed-Sernberg ces, e magnan ces o Hodgkn
ympoma
and
(descrbed
many
suc
as
•
(DLBCL)
50
a
Severa
caegor y
aer).
express
BCL2,
years.
I
occurs
s
derved
eerogeneous
morpoogc,
a
a
ages
rom
group
o
bu
s
he
umors
surace
BCL6,
and
IgM
express
and/or
MYC
are
e
IgG.
varaby
B-ce
angen
Oer
proen
expressed.
EBV-assocated
persons.
neopasms
begn
and
In
as
regress
•
e
mos
ransocaons
oncogenes,
common
a
ncudng
ead
e
drver
o
e
muaons
n
DLBCL
overexpresson
oowng:
o
sev-
cncopaoogc
Human
DLBCLs
mmune
n
e
ty pe
wc
s
may
peroneum.
encodes
8
s
seng
ranspan
poycona
uncon
[KSHV])
wc
n
posranspanaon
er pesv rus
or
HHV8,
e
arse
(e.g.,
EBV-drven
y mphomas,
dum,
subypes
are
ncuded
n
e
DLBCLs.
mmunosuppresson
angen-
mmunopenoypc,
dsncve
o
erpesvrus
Among
ese
severa
Occasonay,
ly m-
n on - Ho dg k in
varaon.
Pathogeness.
n
ave
BCL6,
Lymphoma
l y mp h oma
accountin g
lymphomas
mos
B
B-cel l
o
encodng
dened
may
or
markers
Diffuse
cener
umors
resus
Bo
o
racon
cenray paced nuceo, and abundan pae or basopc cyopasm.
CD20,
erapy.
a
5%
gene
varaon.
croman,
margna
gene
ger
mporan
germna
o
rearrangemens
even
ces.
sze
cyopasm
Clncal
a
moecues,
n
e
round
o
been
soogc
and
surace mmunogobun, usuay IgM.
BCL2
n
30%
an
promoer.
an
of
Dallas.)
ave
and
proen,
expresson
MYC,
Morphology.
ce
CD20
e
BCL6
BCL6
Approxmaey
ave
sgnang
(ymphoepthea
o
e
School,
DLBCLs
3q27,
nuclear
Courtesy
efec.
uncons
Morphology.
n
(A,
many aspecs o grow-promong meabosm, suc as e W arburg
cone
nvouon.
o
through-
cleaved
Medical
rd
Approxmaey
nvovng
and
respons-
one
gene
present
or
(centroblasts).
cromosome
eves
are
ocuar ympomas, wc vruay aways ave e (14;18).
•
emerges a remans dependen on angen-smuaed T-eper ces or
sgnas
o
BCL2.
cells
irregular
oc B CL2 proen. Some o ese umors may represen “ransormed”
o
cyoknes
survva.
on
nvovng
pyor
eads
Abou
ncreased
syndrome,
nlammaory
poycona
drver
ssues
Sjögren
(e.g.,
anboc
depend
ces
n
(e.g.,
necon
wc
T
mos
dsorders
cronc
pyor–specc
e
arses
auommune
Eradcaon
regresson
ater
hs
and
Southwestern
muaons
uaor
Pathogeness.
lymphoma
nucleoli
Texas
ocaed
[muco-
of
chromatin
o
AIDS,
recpens),
seng,
B-ce
ese
and
arogenc
n
edery
umors
proeraons
a
oten
may
resored.
(HHV8,
assocated
arse
hese
aso
w t
wn
umors
proens
e
are
caed
rare
Kapos
peura
cavy,
aeny
omoogous
sarcoma
prmar y
o
euson
percar-
neced
severa
w
known
CHAPTER
Fig.
9.18
have
tesy
Diffuse
large
of
Texas
Dr.
nuclei
large
B
with
Robert
W.
Southwestern
cell
open
lymphoma:
chromatin
McKenna,
Medical
lymph
and
Department
School,
node.
The
prominent
of
tumor
nucleoli.
Pathology,
9
cells
(Cour-
University
of
Hematopoietic
Fig.
9.19
nuclei
high
fairly
level
“starry
Dallas.)
Burkitt
are
of
sky”
of
ncudng
c ycn
D1.
Mos
afeced
paens
Dr.
Robert
a
Systems
node.
by
and
at
a
lower
Department
155
tumor
cells
prominent
lightly
their
Note
the
nucleoli.
staining,
magnification.
of
and
appearance.
interspersed,
appreciated
McKenna,
The
monotonous
(arrowheads)
produced
better
W.
lymph
giving
activity
pattern
is
Lymphoid
lymphoma:
uniform,
mitotic
macrophages
oncoproens,
and
Pathology,
The
normal
(Courtesy
University
of
are Texas
Southwestern
Medical
School,
Dallas.)
mmunosuppressed.
•
Medastna
women
ymc
B
caons
a
proens
an
•
arge
and
B-ce
appears
ces.
hs
ead
PD-L1
mporan
o
roe
orgnae
umor
e
and
ympoma
o
requeny
s
mos
an
o
suggesng
oten
unusua
as
overexpresson
PD-L2,
n
occurs
rom
n
cromosoma
e
a
young
popuaon
mmune
mmune
o
amp-
ceckpon
evason
pays
paogeness.
BCL2.
and
he
a
MYC
combnaon
srong
exb
an
nvovng
ver y
and
o
prosur vva
aggressve
convenona
anoer
a
poen
oncogene,
progrow
oncogene
beavor
IGH
ces;
gene
varan
on
cromosomes
o
eac
s
proen.
e
In
2
w
(BCL2)
mos
mos
oncogene
yeds
subsanay
pays
n
(MYC)
umors
worse
a
e
oucomes
DLBCL.
round
a
or
Paens
mass
a
ypcay
one
or
presen
severa
gasronesna
ses.
Exranoda
are
and
λ
obser ved.
he
overexpresson
abou
20%
o
acve
g-can
ne
o
sporadc
n
oc
B
on
resu
e
MYC
cases,
e
o
cdood
enargng,
oten
presenaons
are
ympomas.
sympomac
common;
Wou
nensve
compee
uncommon
reamen,
combnaon
remssons
approxmaey
50%
a
DLBCL
nvovemen
are
s
aceved
ree
o
e
bu
ces
and
are
wo
o
nermedae
ve
dsnc
n
sze
nuceo
and
(Fg.
ave
9.19).
conans
IgM,
and
numerous
a
e
ssue
creae
B-ce
sma,
pd-ed
apoposs
a
vacuoes.
caracersc,
macropages
“starry
marker
are
sky”
CD20,
conanng
pattern.
and
Ver y
e
Tumor
germna
g
aer
raes
ngesed
ces
cener
o
assocaed
nucear
express
B-ce
surace
markers.
e
ver,
speen,
dagnoss.
n
and
and
rapdy
an-CD20
60%
o
dsease
o
dsease
aggressve
cemoerapy
reman
o
se,
umor
nuce
30%
s
ympoma),
exranoda
unceran.
cdren and young adus: Burk ympoma accouns or approxmaey
marrow
common
s
pomas
ocuar
mos
and
and
Clncal Features. Bo e endemc and nonendemc orms afec many
bone
e
15%
rapdy
aso
κ
can arse n vruay any organ or ssue. Unke e more ndoen ym-
and
s
a
cases
ranscrponay
Ig
DLBCL
(e.g.,
rac
w
abou
he
ova
oten
debrs
consues
respecvey,
endemc
s
e
here s a moderae amoun o basopc or ampopc cyopasm
w
wc
dysreguaon
paogeness
Morphology.
occur
age;
22,
e
14,
nvovng
commony
Clncal Features. Aoug mos common n oder adus, DLBCL can
any
and
same:
proeraon
a
cromosome
ransocaons
umor ces are aeny neced w EBV , bu e precse roe a EBV
D oube-t ympoma reers o unusua umors a ave dua rans-
ocaons
e
80%
and
o
aa.
W
mmunoerapy,
paens;
appear
o
be
o
ese,
cured.
For
as
cdood
usuay
maxary
nvovng
Burk
or
e
non-Hodgkn
arses
a
mandbuar
bowe,
ympoma
s
ympomas
exranoda
ses.
masses,
wereas
reroperoneum,
gy
aggressve;
n
e
Endemc
and
n
Uned
umors
Nor
ovares
owever,
more
very
he
manes
Amerca,
are
w
Saes.
oten
umors
common.
nensve
ce-
moerapy regmens, a majory o paens can be cured.
oers, oer aggressve reamens (e.g., emaopoec sem ce rans-
panaon)
ofer
ope.
Other
Neoplasms
Among
Burkitt
Burkitt
MYC
Lymphoma
lymphoma
gene
that
Hea
is
result
associated
in
with
translocations
overexpression
of
the
MYC
involving
the
transcription
e
eaures
Burk
ympoma
s
endemc
n
pars
o
Arca
and
occurs
sporad-
cyopasmc
muaons
e Arcan and nonendemc dseases are denca, aoug ere are cn-
sream
ca and vroogc dferences. he ce o orgn s a germna cener B ce.
ons
s
Pathogeness.
MYC
gycoyss),
Caper
umor.
o
casscaon,
are
wory
o
a
Cells
ympod
severa
bre
neopasa
w
n
dsncve
e
or
Word
cncay
dscusson.
Hary ce eukema s an uncommon, ndoen B-ce neopasm w a
cay n oer geograpc areas, ncudng e Uned Saes. Hsoogcay,
(see
Lymphoid
orms
dsncve morpoogy caracerzed by e presence o ne, arke
factor.
obc
Mature
oer
Organzaon
mporan
•
of
many
Mos
5).
a
s
a
maser
cancer
Burk
reguaor
amark
ympoma
ransocaons
use
e
o
Warburg
assocaed
may
be
MYC
e
gene
w
meabosm
rapd
ce
ases-growng
on
(aer-
o
n
uman
sensve
8
w
I
rom
Vruay
a
serne/reonne
occurs
many
nraon
enarged.
o
n
e
Pancyopena
cases
knase
oder
bone
s
seen
are
assocaed
w
BRAF ,
wc
maes,
and
s
and
speen,
marrow
n
more
an
acs
drver
down-
manesa-
a
o
wc
cases.
Scaered “ary ces” can be dened n e perpera bood smear
grow
cromosome
e
RAS.
resu
usuay
projecons.
n
mos
BRAF
cases.
o
he
dsease
ceran
nbors.
s
progressve
cemoerapeuc
he
overa
prognoss
unreaed
agens
s
and
exceen.
bu
s
exremey
responds
we
o
156
•
CHAPTER
Hematopoietic
9
and
Lymphoid
Systems
Mycoss fungodes and Sézary syndrome are umors o neopasc CD4+
T
ces
a
are
ound
n
e
skn,
and
are
ence
grouped
under
cua-
neous T-ce ympoma. Mycoss ungodes usuay maness as a ras
a
by
progresses
sysemc
appearance
and
s
ey
over
produced
nrae
caracerzed
presence
o
dagnosed
years,
me
o
dssemnaon.
by
umor
w
wereas
by
e
paques
he
marked
upper
a
(Sézary
eary-pase
paens
T
and
ces
o
e
ces)
n
umors,
ave
e
oowed
cerebrorm
membranes,
Sézary
syndrome
eryroderma
perpera
ungodes
umor-pase
a
nucear
epderms.
exoave
mycoss
w
cuaneous
nodng
derms
generazed
ces
and
neopasc
oten
dsease,
and
bood.
survve
e
Paens
or
many
dssemnaed
ds-
ease, or Sézary syndrome survve on average or 1 o 3 years.
•
Adut
T-ce
caused
by
HTL V-1
and
eukema/ympoma
a
rerovrus,
necon
W es
Arca,
s
uman
endemc
and
(ATL)
T-ce
n
occurs
s
a
neopasm
eukema
souern
vrus
Japan,
sporadcay
o
CD4+
ype
e
1
T
Carbbean
esewere,
ces
(HTL V-1).
basn,
ncudng
n
e
Fig.
9.20
berg
soueasern
Uned
Saes.
he
roe
o
e
vrus
n
ympogeness
cell
Hodgkin
with
surrounded
uncear
bu
key
nvoves
ceran
vra
proens
and
susaned
lymphoma:
large,
lymph
inclusion-like
node.
nucleoli
A
binucleate
and
abundant
Reed-Stern-
cytoplasm
is
s
by
lymphocytes,
macrophages,
and
an
eosinophil.
(Cour-
proertesy
of
Dr.
Robert
W.
McKenna,
Department
of
Pathology,
University
of
aon o neced T ces. Adu T-ce eukema/ympoma s assocaed Texas
w
skn
esons,
ympadenopay,
ma,
and
varabe
ympocyoss.
epaospenomegay,
Mos
cases
are
very
Southwestern
Medical
School,
Dallas.)
ypercace-
aggressve
and
respond poory o reamen. he medan survva me s ony 8 mons.
•
Perpera
umors
genera,
Hodgkin
Hodgkin
tive
rom
even
ese
e
o
umors
are
sympoms
wen
10%
a
umors
reaed
umor
a
eerogeneous
non-Hodgkn
o
o
respond
poory
uncona
T
s
reavey
o
ces,
umor-derved
burden
group
ympomas.
o
In
erapy.
paens
nlammaor y
ow.
Lymphoma
giant
Hsorcay,
cells
are
characterized
known
Hodgkn
ympomas
appearance
e
Aoug
and
e
as
e
by
was
presence
comprse
ony
cells
consdered
dagnosc
Hodgkn
the
Reed-Sternberg
ympoma
because
dsncve
umor.
encompasses
abou
aggressve
lymphomas
tumor
Hodgkn
are
up
because
sufer
producs,
ympoma
make
ese
Moreover,
oten
T-ce
a
a
apar
ympomas
racon
are
now
distinc-
variants.
rom
Reed-Sernberg
sma
of
and
ces
o
e
non-
ave
ces
undersood
o
a
n
be Fig.
umors
o
B-ce
or g n ,
e y
con nue
o
be
ds nguse d
9.21
Hodgkin
low-power
o
er
unque
bo og y
and
resp ons e
o
subypes
sceross,
(2)
depeon,
e
o
mxed
and
(5)
eaures
ogeer
under
ces
sare
(descrbed
e
ympoma
ceuary,
ympocye
Reed-Sernberg
noypc
Hodgkn
rubrc
(3)
are
ceran
cassc
recognzed:
ympocye
predomnan.
aer),
In
rc,
e
as
Hodgkn
a
(4)
rs
morpoogc
and
resu
(1)
ympocye
our
and
noduar
ert
A
subypes
o
Hodgkn
western
Medical
are
umped
e
caused
by
mos
bae
commony
upreguaed
by
varous
acor
a
muaons,
suppors
and
B-ce
genes
School,
survva,
encodng
s
o
ces,
nuceus,
mmune
wc
cases
o
EBV
e
s
ound
n
e
mxed-ceuary
Reed-Sernberg
subype
and
a
ces
n
smaer
as
many
racon
ces
o
•
oer “ cassc” orms o Hodgkn ympoma.
he
Reed-Sernberg
sne
ce
qua
(Fg.
non
9.20),
o
a
cassc
very
Hodgkn
arge
ce
ympoma
w
an
s
ave
abundan
a
CD30
cyopasm.
caracersc
and
angens,
do
or
no
mmunopenoype:
express
T-ce
Reed-Sernberg
CD45
angens.
hey
(eukocye
Dferences
ces
and
express
common
n
e
er
varans
CD15
angen),
appearance
and
B-ce
o
e
or
into
nodules.
Pathology,
e
o
ssue
lymph
node.
acellular
(Courtesy
University
response
cassca
young
sma
cyes,
•
nodues
reacve
drawn
sroma
oder
o
Hodgkn
adus.
I
s
A
collagen
of
of
Dr.
Texas
Rob-
South-
ese
ces
denes
ympoma:
dened
varans
nuceo
he
sc
n
are
9.21).
by
n
and
w
by
a
e
presence
snge
abundan,
50
and
Reed-Sernberg
eosnops,
pasma
and
ympoma
caracerzed
by
muo-
pae-sanng
produced
ces,
s
comprses
ces
by
varyng
pro-
macropages,
Reed-Sernberg
and
are
mos
penu
conanng
25%
o
wn
sma
n
cases
a
e-
ympo-
macropages.
rare.
presence
common
abou
ympocyte-depeted
bo
are
and
ssues.
nrae
are
e
presen
ympoma
years
nlammaor y
Aso
eosnops,
cyoknes
nvoved
Hodgkn
ympocyte-rc
Hodgkn
(Fg.
ympocyes,
ces
an
Cassc
erogeneous
enormous
muobae nuceus, exceponay promnen ncuson-ke nuceo,
and
cells
of
Reed-Sernberg
Mxed-ceuarty
overa.
e
o
are
and
paens
Morphology.
type:
pink,
cyopasm, and coagen bands, wc dvde nvoved ssues no
PD-L1
porons
response.
and
mupe
crcumscrbed
o
of
Dallas.)
subypes
adoescens
acunar
eads o er overexpresson and eps Reed-Sernberg ces evade e os
70%
tumor
varans
common
and PD-L2, wo mmune ceckpon acvaors, are oten amped, wc
as
sclerosis
bands
Noduar sceross Hodgkn ympoma oten nvoves e medas-
num
drver
ympoma.
ranscrpon
the
Department
Reed-Sernberg
o
a
nodular
well-defined
mmunope-
ese
are
subdivided
McKenna,
muaons n cancer genes; ese are bes caracerzed n cassc Hodgkn
NF-κB,
shows
subypes,
ympoma.
ympoma
have
W.
•
Pathogeness.
view
er apy. that
Fve
lymphoma,
b e c aus e
o
As
e
subypes
names
unusuay
o
mpy,
cas-
ey
promnen
or
sparse nraes o reacve sma ympocyes, respecvey. he
CHAPTER
9
Hematopoietic
he Reed-Sernberg
ces
and
varans
resembe
ose
seen
n
ceuary
Se
apar
rom
cassca
mmune
Hodgkn
ympoma
s
e
and
dened
by
subtype,
e
wc
accouns
or
abou
5%
o
S evera
presence
o
ymposocyc
(L&H)
e
deeerous
kdney,
a
o
efecs
wc
on
e
conrbue
skeeon,
o
morbd-
acors
ead
ces
popped
w
corn
a
decae
(popcorn
muobed,
ce).
L&H
pufy
varans
o
produced
by
myeoma
ypercacema
and
ces
cause
paoogc
bone
resorpon
racures,
mos
re-
varan n
e
spne
and
emur.
nuceus
• resembng
and
cases.
queny Reed-Sernberg
sysem,
moray :
and s
ave
157
ympo-
• cyte-predomnant
I
ces
Systems
subype. y
•
pasma
Lymphoid
e e
mxed
proerang
and
are
Myeoma
causes
deecs
n
umora
mmuny,
ncreasng
e
rsk
ound or
bacera
necons.
wn arge nodues conanng many sma B ces admxed w
•
Myeoma
eads
o
rena
aure
owng
o
(1)
obsrucve
proen-
varabe numbers o macropages. Unke e Reed-Sernberg varaceous ans
n
cassc
Hodgkn
ympoma,
L&H
varans
express
cass
comprsed
o
precpaed
Bence-Jones
proens;
B-ce (2)
g-can
deposon
n
e
gomeru
or
e
nersum,
markers (e.g., CD20) and do no express CD15 and CD30. eer Regardess
o
subype,
e
dagnoss
s
based
on
e
Reed-Sernberg
ces
or
varans
n
e
approprae
amyod
background
deydraon
and
ces.
Ces
resembng
Reed-Sernberg
ces
near
deposs;
(3)
ypercacema,
may
be
rena
sones;
and
(4)
requen
wc
bous
o
eads
bacera
o pyeoneprs
reacve
or
dencaon o
o
as
seen
due
o
deecve
umora
mmuny.
n
oer cancers and some reacve condons; us, mmunopenoypng
Morphology.
s oten requred or dagnoss.
desrucve
Mupe
skeea
myeoma
esons
a
usuay
mos
maness
commony
w
nvove
coumn, rbs, sku, pevs, emur, cavce, and scapua Clncal
Features.
Hodgkn
ympoma
usuay
maness
as
or,
w
e
noduar
sceross
subype,
verebra
Radoogcay,
paness e
ympadenopay
muoca
e
bone
esons
appear
as
punced-ou
deecs
1
o
4
cm
n
dameer
sympoms (Fg.
9.22A).
he
ces,
ypcay
marrow
conans
ncreased
numbers
o
pasma
reaed o e presence o a medasna mass. he sysemc efecs o cyo-
knes
cause
anema
o
cronc
nlammaon,
eukocyoss,
and
more
an
30%
o
e
ceuary
(see Fg.
9.22B).
Rena
so-caed nvovemen (myeoma nepross) s assocaed w proenaceous cass
B
sympoms
(ever,
weg
oss,
ng
sweas).
Sagng
gudes
erapy
and a
deermnes
e
prognoss.
Y ounger
paens
w
more
avorabe
obsruc
e
dsa
convoued
ubues
and
e
coecng
ducs.
subypes Oten, epea ces adjacen o e cass become necroc or aropc
end
o
presen
w
ow-sage
dsease
and
are
ree
o
so-caed
B
sympbecause
Bence-Jones
proens
are
oxc.
Oer
common
paoogc
oms, wereas paens w more exensve dsease are more key o ave processes B
sympoms
and
anema.
Ina
reamen
s
w
cemoerapy,
nvovng
e
kdney
ncude
measac
caccaon,
g-
somecan (AL) amyodoss, and bacera pyeoneprs.
mes w nvoved ed radoerapy or arge umor masses.
he overa ouook s exceen. he 5-year survva rae or paens w
ow-sage
dsease
s
over
90%.
Even
w
wdespread
dsease,
e
overa
Clncal
Features
he
dagnoss
5-year dsease-ree survva rae s around 50%. Immune ceckpon nb-
monocona
mmunogobun
ors
and/or
eves
ave
produced
exceen
responses
n
paens
w
reapsed,
reracory
dsease and may soon be added o ronne erapeuc regmens.
or
e
g
urne;
marrow ;
Plasma
These
Cell
B-cell
plasma
cells
globulin
or
Neoplasms
and
abou
15%
mporan
virtually
are
o
pasma
o
e
ese
ce
deas
Related
Entities
composed
always
immunoglobulin
Coecvey,
or
and
proliferations
secrete
entirely
a
or
in
monoclonal
part
of
immuno-
fragments.
neopasms
caused
neopasms,
by
reaed
ympod
mupe
dsorders
neopasms.
myeoma,
s
dscussed
mos
nex.
aure
varabe.
s
sur vve
oped
more
are
may
unoded
a
nduce
adomde-ke
new
cases
are
dagnosed
n
e
Uned
Saes
eac
myeoma
and
wc
n
peope
usuay
s
he
IgG
o
cans.
a
are
ng
mos
n
Ony
pasma
rarey
are
are
ree
esons
(20%
o
produce
IgM,
IgD,
excess
g
n
prncpay
e
g
o
ony
cans
n
κ
IgE
e
or
λ
as
Once
marrow
skeea
by
myeoma
Even
eavy
secreed,
mporan
15%
n
mmunogobun
e
protens.
ces
o
s
20%
g
myeomas
cans
cans,
resu-
As
ree
g
descrbed
n
efecs.
angens
Other
A
use
e
e
IGH
cycn
been
Myeoma
ocus
D1
gene.
descrbed.
cyokne
on
A
oten
wde
6
cromosoma
varey
Proeraon
nereukn
as
cromosome
(IL-6).
o
14
o
o
oer
myeoma
ransocaons
proo-oncogenes
drver
ces
s
a
muaons
suppored
as
ave
by
e
sem
arge
e
o
be
many
a
ces
aby
o
dsposes
are
Bsposponaes,
o
CAR-T
1).
o
w
n
e
and
progno-
rarey
“smoder-
receny
sress
a
acva-
o
e
proens,
erapes.
he
acvy
agans
ubqun
gases,
markng
and
by
Inbors
as
ceran
deve-
mmunogobun
efecve
em
a
m
proongs
ces
he
msoded
dr ugs
racures
ranspanaon
Tras
ce
aso
ereby
serum
unreaed,
severa
cause
and
e
ces
years.
Caper
acvae
ubqun,
Msoded
and
(see
serum
Hypercacema
paens
aceved,
ces
a
myeoma)
n
pasma
presenaon.
wereas
o
or
cans
o
esons,
enadomde
paoogc
ce
o
oucomes.
response
g
ndngs.
bony
or
deecon
proen,
number
me
mons,
organee
s
e
M
e
or
nb
pro-
bone
ypercacema.
bu
recognze
as
no
pasma
ye
ce
ongong.
Cell
Neoplasms
mmunogobuns,
•
ye
w
curave.
umors
B
12
myeoma
o
reduce
Plasma
producng
suc
be
are
ese
mer
Morphology.
o
a
myeoma
degradaon.
Hemaopoec
proven
o
a
asympomac
n
on
radoogc
mproved
proens
resorpon,
o
mupe
compound
because
ag
easoma
g
sma
paoogc
and
sysem.
mmunogobun
produced.
Bence-Jones
ave
e
remanng
mmunogobun
cans.
urne
e
produced
25%);
or
nvoves
rougou
mmunogobuns,
n
unpared
oowng,
IgA
ces
compee
excreed
yc
I
mmunogobun
by
syneszed
ree,
cans
e
e
orgn.
w
requen
oowed
produce
oten
Arcan
assocaed
(60%),
cases,
o
o
proen
apoposs
year. he medan age a dagnoss s 70 years. I s more common n maes
6
ceuar
Approxmaey
w
ave
ave
Mupe myeoma s one o e mos common emaoogc magnances:
20,000
be
accumuae
proeasome,
common
an
rees
so-caed
mmunogobun
caracersc
cures
erapes
e
ree
Paens
myeoma”
cans
Myeloma
or
o
dencaon
aso
Aoug
ng
Multiple
e
ss
accoun
he
and
rena
ng
and
e
(a
are
and
assocaed
markng
ympocyes
em
or
Related
w
as
pasma
Entities
e
producon
cona
ces.
o
proeraons
hree
umors
monocona
o
n
anbody-
s
group
dscusson.
Monocona gammopaty of undetermned sgnicance (MGUS) s seen
n
paens
wou
sgns
or
sympoms
wo
ave
monocona
mmu-
nogobuns n er bood. MGUS s very common n oder adus, and
abou 1% o cases ransorm no a sympomac neopasm, mos oten
mupe myeoma, eac year.
158
CHAPTER
Hematopoietic
9
and
Lymphoid
Systems
as
ver y
rare
wereas
socyc
oers
exremes
e
Langerans
a
are
group
ce
sarcomas,
bengn
o
are
reacve
umors
stocytoses,
gy
comprsed
wc
magnan
yperpasas.
mer
a
o
neopasms,
Beween
ese
Langerans
bre
wo
ces,
e
descrpon.
Pathogeness. A orms o Langerans ce socyoss are assocaed w
drver muaons a acvae e serne/reonne knase BRAF . BRAF s a
componen
on
n
and
a
o
e
survva.
dferen
RAS
sgnang
T umors
paway
wou
serne/reonne
BRAF
knase
a
suppors
muaons
caed
ceuar
oten
MAP2K1
ave
a
proera-
muaons
acs
down-
sream o BRAF , urer mpcang s paway n e paogeness.
Morphology.
Proerang
Langerans
ces
ave
abundan
cyopasm
and vescuar nuce, smar o a o ssue macropages (aso known
as
socyes);
eosnops
proen
ence,
are
caed
oten
e
erm
admxed.
angern
and
can
stocytoss.
Langerans
be
dened
Numerous
ces
by
express
sanng
reacve
a
or
unque
angern
and CD1a.
Clncal
severa
•
Features.
Langerans
cncopaoogc
ce
socyoss
can
be
grouped
no
enes.
he mos common subype s unfoca unsystem dsease, n wc e
A proeraon s conned o a snge se n a snge organ sysem, mos
commony
I
may
be
racures.
•
bone
I
Mutfoca
maness
o
deecs,
aso
s
ndoen
unsystem
w
nvovemen
eads
bu
asympomac
and
e
dabees
dabees
neous
a
usuay
maness
ons
and
he
and
are
n
cuaneous
requeny
eads
o
oca
excson
In
sak
e
younger
a
s
an
2
mmc
ypcay
50%
o
o
bone
as
e
spona-
cemoerapy.
aggressve
years
o
dsorder
age.
seborrec
epaospenomegay,
cases,
cavara
reerred
w
an
gu.
rradaon.
and
experence
efecvey
or
paoogc
ypoaamus
o
s
paens
dsease)
or
abou
o
skn,
and
cdren
masses.
Some
esons
ung,
combnaon
reaed
cdren
e
exopamos
(Letterer-Swe
occurs
w
bony
as
enderness,
afecs
puar y
trad.
oers
by
usuay
nspdus.
dsease
suc
pan,
cured
poseror
nspdus,
regressons;
Mutsystem
s
erosve
Hand-Scüer-Crstan
•
ssues
cause
dsease
mupe
o
sot
or
I
skn
oten
erup-
ympadenopay,
B pumonary
Fig.
The
(B)
9.22
Multiple
sharply
Bone
plasma
punched-out
marrow
cells,
nucleoli,
myeloma.
and
bone
aspirate.
including
(A)
defects
Normal
atypical
cytoplasmic
Radiograph
marrow
forms
droplets
are
of
the
most
obvious
cells
with
skull,
are
largely
multiple
containing
in
lateral
the
nraon
by
Beeding
es,
ces.
n
a
marked
•
pasma
ce
componen
ypervscosy
by
nnus,
secrees
syndrome
vsua
monocona
(W adenström
mparmen,
and
IgM
a
oten
macrogobunema)
neuroogc
dysuncon.
or
Tabe
vesse
evan
disorders
9.8).
wa,
o
may
coaguaion
As
descrbed
paees,
emosass
and
macyc ympoma s responsve o agens used or oer ndoen B-ce
peced
coaguopaes
ympomas
•
nbors
o
B-ce
recepor
sg-
paees.
he
paways.
o
VII,
ave
over
he
o
because
Histiocytic
erm
deposed
mupe
popuaon
ease
are
e
ces
bu
a
syness
o
(see
Caper
oers
ave
nevereess
a
paogenc
4).
ony
causes
Some
a
dsorders
s
o
an
•
mnor
sgncan
Parta
dendrc
ces
desgnaon
or
or
macropages.
a
varey
Some,
o
suc
and
by
abnormaiies
or
Caper
and
in
3,
acors.
of
vesses,
combinaion
norma
e
nvoves
ess
a
caracerze
ess
or
pae-
(summarzed
cong
Laboraor y
unconay
mporan
proonged
PT
prorombn;
tme
coaguaon
decences
or
A
X;
trombopastn
rombn;
ds-
are
e
re-
coaguaon
nvesgaon
o
sus-
o
(PTT).
hs
paways.
acors
V ,
can
or
resu
rom
decences
brnogen.
es
assesses
Proongaon
VIII,
IX,
X,
o
XI,
e
nrnsc
PT T
and
can
XII;
be
pro-
brnogen.
•
Pateet count. he norma reerence range s 150,000 o 450,000/μL.
•
T ests of pateet functon. No snge es provdes an adequae assessmen
o
“umbrea”
V ,
common
caused
cona
mmunogobun.
acors
and
paens
Neoplasms
stocytoss
proerave
amyod
myeoma,
pasma
o
as
Exensve
predspose
Protrombn tme (PT). hs es assesses e exrnsc and common
coaguaon
a
esons.
and
ncude:
Prmary or mmunocyte-assocated amyodoss resus rom a mono-
cona proeraon o pasma ces producng mmunogobun g
n
mos
nang). e overa survva me ater dagnoss averages 4 o 5 years.
cans
pancyopena
from
aone
cong
quany
and
CD20,
sem
facors,
acors
agans
o
DISORDERS
Evenuay , nvovemen o e marrow eads o cyopenas. Lympopas-
(anbodes
ead
bone
immunoglobulin.
composed o a mxure o sma B ces and varabe numbers o pasma
he
may
oseoyc
W nensve cemoerapy, 50% o paens survve 5 years.
Lympopasmacytc ympoma s a B-ce neopasm o oder adus a s
causes
desrucve
prominent
BLEEDING
•
and
paen o recurren necons. he dsease s rapdy aa unreaed.
calvaria.
replaced
nuclei,
marrow
view.
esons,
paee
uncon.
Aggregaon
ess
a
measure
e
response
o
paees o ceran agonss and quaave and quanave ess o von
Webrand acor (descrbed aer) are bo used n cnca pracce.
CHAPTER
Table
9.8
Bleeding
9
Hematopoietic
and
Lymphoid
Systems
159
Disorders
Mechanism
Causes
Vascular
Vitamin
fragility
Clinical
C
Systemic
Chronic
deficiency
(scurvy)
amyloidosis
connective
skin
and
mucous
mem-
branes
glucocorticoid
Inherited
Features
Ecchymoses,
use
tissue
disorders
Vasculitis
Platelet
dysfunction
Thrombocytopenia
Petechial
Immune-mediated
Consumptive
Marrow
(DIC,
HUS,
TTP)
underproduction
Prolonged
(tumors,
other
infiltrative
disorders,
aplastic
minor
anemia)
Qualitative
Drugs
factor
other
platelet
defects
(von
Willebrand
disease,
Glanzmann
A
Hemophilia
B
cal
Delayed
inhibitors
specc
ence
o
cong
acors
crcuang
and
ess
brn
msceaneous,
and
sites
bleeding
subject
to
mechani-
joints)
after
surgery
(e.g.,
K
deficiency,
liver
disease)
Bleeding
drugs)
in
deep
soft
tissues
(e.g.,
psoas
muscle)
used
o
measure
producs
or
o
e
assess
eves
e
o
pres-
Table
9.9
Causes
Decreased
of
Production
Thrombocytopenia
of
Platelets
ancoaguans.
o
vesses
a
uncommon
coaguaon
in
(e.g.,
(DIC)
are
sp
(vitamin
(antibodies,
Generalized Abnormaes
trauma
circumcision)
Consumptive
specazed
from
thrombasthenia,
Hemorrhages
Hemophilia
Underproduction
more
bleeding
syndrome)
Acquired
Addona
immediate
trauma
inhibitors)
Inherited
Factor
skin
Menorrhagia
Bernard-Soulier
deficiencies
and
neoplasms
Inherited
Coagulation
mucosae
defects
(aspirin,
Myeloid
bleeding,
Epistaxis
acors
are
ead
o
dsorders,
reavey
beedng
wereas
ncude
dsorders
a
range
o
Bone
Marrow
Dysfunction
o Aplastic
anemia:
congenital
Marrow
infiltration:
and
acquired
paees leukemia,
disseminated
common. cancer
Selective
Impairment
of
Platelet
Production
Thrombocytopenia
Drug-induced:
alcohol,
thiazides,
cytotoxic
drugs
hrombocyopena s dened as a paee coun o ess an 150,000/μL.
Infections:
Excessve
are
posraumac
reduced
unkey
rom
o
un
sma,
eccymoses
20,000
couns
e
o
beow
bood
skn,
s
seen
50,000/μL,
a
superca
n
beedng
e
ony
and
5000/μL.
vesses
and
mucous
wen
e
paee
sponaneous
Beedng
produces
membranes
peecae
o
s
occurs
or
arge
e
gasrones-
eared
compcaon
Ineffective
and
urnar y
racs,
and
oer
ses.
he
mos
infection
Megakaryocytopoiesis
Megaloblastic
Decreased
anemia
Platelet
Immunologic
na
HIV
couns
beedng
ypcay
measles,
Survival
Destruction
Autoimmune:
o
rombocyopena
s
emorrage
no
e
cenra
ner vous
sysem, Primary:
wc
s
uncommon
bu
may
be
immune
Secondary:
Maj or
c aus es
o
romb o c yop en a
are
se d
n
Tabe
9.9.
B-cell
mp or an
pro duc on
depress es
bu
n
or
and
o
s e
d o es
con ras,
a
ncre as e d
abnor ma y
b e c aus e
no
n
a e c s
s
o
e
be
p aee s .
cnc a y
ce
o
and
by
a
o
sg n c an
due
o
may
mer
a
be
a
re duc e d
Sp enomega y
p aee s
romb o-
probem
g ranu o c ye
p aee s
ds orders
c aus e d
s e qu es ra on
genera y
re d
d es r uc on
s e vera
o
c aus e
pro duc on
a s o
may
d es r uc on
couns
R e duce d
emaop oess
ae d
ncre as e d
p aee
c yop en a.
In
romb o c yop en a
w
pro duc on .
s e en
br e
as
tumors
an
s o -
ds c uss on .
infections
Isoimmune:
autoimmune
(infectious
Thrombocytopenic
Purpura
by
anibodies
opsonizaion
of
e
a
bind
paees
paee
and
eir
surface
remova
proeins,
from
e
lymphocytic
eading
o
(systemic
mononucleosis,
quinidine,
and
lupus
HIV)
neonatal
heparin,
sulfa
compounds
Nonimmunologic
Disseminated
Thrombotic
Destruction
intravascular
Hemolytic-uremic
Dengue
Immune rombocyopenic purpura (ITP) is an auoimmune disease
caused
purpura
chronic
disorders
posttransfusion
Drug-associated:
coagulation
syndrome
thrombocytopenic
Microangiopathic
Immune
(e.g.,
C nleukemia);
c a y
thrombocytopenic
aa.
hemolytic
purpura
anemia
fever
Sequestration
Hypersplenism
circuaion Dilutional
by macropages. Multiple
he
dsease
as
wo
cnca
subypes.
Acue
ITP
s
a
HIV,
orm
seen
reavey
mosy
n
common
cdren
dsorder
ater
a
vra
mos
necons.
oten
afecs
transfusions
(e.g.,
for
massive
se-med
Cronc
women
ITP
s
a
beween
human
immunodeficiency
virus.
blood
loss)
erythematosus);
160
e
CHAPTER
ages
paee
o
20
and
anbody
IgG-coaed
soaed
40
years.
he
speen
producon
and
e
paees,
dsorder
Hematopoietic
9
so
a
spenecomy
mus
be
s
an
major
s
mporan
se
o
beneca.
dsngused
and
rom
Lymphoid
se
o
desrucon
Cronc
an-
o
ITP
secondar y
e
s
ITP
an
due
o oer condons (e.g., sysemc upus er yemaosus, drug exposure,
HIV
necon,
he
onse
peecae,
mnor
rare,
o
and
o
easy
Serous
occur.
he
rs
and
reaed
rapdy
responses,
ce
w
erapes
drugs
are
Heparin-Induced
hs
speca
menon
ype
because
bocyopena
reamen
and
ress
e
or
on
an-CD20
a
cnca
o
erapy.
deciencies
Acqured
•
oers,
anbodes),
e
e
Mos
paens
produce
are
o
drug-nduced
s
cnca
n
eparn.
3%
are
I
s
o
caused
K
syness
paens
by
IgG
o
ater
1
o
anbodes
2
weeks
a
o
bnd
vamn
he
ver
many
epac
o
decences
med
Heredar y
dened.
O
o
a
o
snge
rea.
Bo
marked
o
mbs)
paee
venous
and
arera
rombocyopena,
and
dea.
acvaon
condon
romboses
and
Cessaon
and
e
may
o
occur,
cause
eparn
a
eparn
even
severe
n
e
morbdy
erapy
breaks
s
used
o
seng
o
e
o
syness
and
a
severe
o
or
pro-
coagua-
acors.
severa
coaguaon
coaguaon
acors
dseases
are
acors
rom
e
common
and
crcu-
causes
o
ese,
acors.
ony
o
many
von
coaguaon
Webrand
acors
dsease,
aso
ave
emopa
been
A,
and
emopa B are suceny common o warran urer consderaon.
o
as-
(e.g.,
by :
acor.
decences
disease
romboss,
eparn-dependen
K-dependen
mupe
tive
exacerbang
a
X
caused
seng
maabsorpon,
nadequae
and
e
Autoantbodes agans coaguaon acors cause acqured decen-
ereby
n
nesna
IX,
oten
n
acquired
•
Disease
membranes
mos
occurs
or
clotting.
Dssemnated ntravascuar coaguaton (DIC; dscussed aer) oten
Willebrand
paee
are
for
dsorders.
Willebrand
on
n
VII,
parencyma
coaguaon
Von
4
resus
acvaed
Von
acor
erapy,
syneszes
on. Anbody bndng acvaes paees and nduces er aggregaon,
paee
and
usuay
acors
congenital
required
common
hs
and
either
are
•
bre
rom-
us,
compex
eads
severe
more
cong
o
dsease.
removes
ces
Moderae
from
that
anboc
nuron,
aon;
an–B-
a
are
and
aso
susaned
mers
result
factors
deicency.
rombn
Lver
uncon
rombopoen-ke
rombocyopena
5%
decences
mpared
e
•
rombocyopena.
mporance.
o
protein
on deec. Wararn s an ancoaguan drug a acs by nbng
presence
spenecomy,
and
ater
Thrombocytopenia
o
Disorders
disorders
of
Vtamn
ncude
emorrages
macropage
somemes
For
ndngs
emorrages
eaures,
nb
and
conrong
and
subaracnod
e
wc
coun
Common
beedng,
response
paee
deveops
w
gum
dsconnuance.
efecve
Coagulation
broad-specrum
nsdous.
nracerebra
e
ater
(e.g.,
oten
s
gucocorcods,
correc
even
ITP
epsaxs,
dagnoss
rombocyopena,
Coagulation
magnances).
cronc
brusng,
rauma.
bu
B-ce
Systems
oss
cyce
o
or
quantitative
Von
rom
or
Webrand
mucous
surger y,
is
dsease
membranes,
and
a
defects
bleeding
in
s
von
caracerzed
excessve
menorraga
disorder
Willebrand
I
s
by
beedng
more
caused
by
qualita-
factor.
sponaneous
ater
prevaen
dena
n
beedng
procedures
persons
o
Euro-
pean descen and s beeved o afec approxmaey 1% o peope n e
consumpon.
Uned Saes, makng e mos common nered beedng dsorder.
Thrombotic
he
erm
Microangiopathies
trombotc
Von
mcroangopates
encompasses
a
specrum
o
cn-
ca syndromes a ncude romboc rombocyopenc purpura (TTP)
up
and emoyc-uremc syndrome (HUS). her causes are dferen, bu a
um,
are
•
caracerzed
e-rc
and
romb
anema.
In
by
abnorma
n
e
conras
paee
acvaon
mcrocrcuaon,
o
DIC,
acvaon
and
eadng
o
deposon
o
o
pae-
coaguaon
acors
s
no
o
20
MDa
were
vWF
•
vWF
ay norma or ony sgy deranged. Because bo dsorders promneny
e
nvove e kdney, ey are dscussed n Caper 11
o
o
s
many
syneszed
e
(Fg.
prmar y
aso
as
a
s
(see
Fg.
coacor
and
ound
wo
X
enancng
acor
IX,
dever y
o
Collagen
Clotting aggregated
cascade
VIII
Platelet
Fibrinogen
GpIIb/IIIa
GpIb Platelet
Subendothelial
Fig.
9.23
circulate
takes
Structure
as
part
adhesion
a
in
of
complex.
the
vWF
and
vWF
coagulation
platelets
to
Endothelial
function
also
of
is
factor
present
cascade
by
subendothelial
VIII–von
in
the
collagen,
Willebrand
factor
subendothelial
activating
endoea
factor
primarily
X
by
means
through
defect
(vWF)
matrix
the
of
of
complex.
normal
factor
IX
glycoprotein
Factor
blood
(not
Ib
VIII
vessels.
shown).
(GpIb)
subendoe-
o
and
ser ve
as
paees
a
o-
9.23).
or
platelets
Factor
e
vWF
emosass.
Activated,
with
n
uncons:
coagen
Xa
vWF
n
major
aowng
subendoea
damage
VIII,
crcuaon
I
vWF
gycoprotens,
beween
factor
9.23).
VIII
vWF
Circulating
(vWF)
coagen.
pateet
endoea
bnds
n
to
“gue”
Endothelium
Factor
acor
weg
bnds
bnds
owng
a
n
moecuar
rombocyopena
promnen eaure o HUS or TTP; consequeny, e PT and PTT are usu-
Webrand
ces and megakar yocyes and exss n e pasma as arge mumers o
and
vWF
Factor
vWF
platelet
VIII
causes
receptor.
ncreasng
acor
s
VIII
o
a-
ses
CHAPTER
Von
Webrand
paee
uncon
cnca
brand
ndngs,
dsease
he
an
auosoma
measurabe
ave
and
n
us
rare
severe
mos
acor
dsorder
cncay
assocaed
ony
paens
common
domnan
bu
s
coaguaon;
excep
wo
cassc
dsease
and
e
w
VIII
varan
w
nsgncan
w
deecs
paee
deec
omozygous
n
9
bo
produces
von
We-
arge
or
he
causng
sma
quaave
vWF
von
reduced
decrease
dagnoss
deecs
mumers,
s
reaced
by
n
vWF
prevenng
measurng
as
a
“oregn”
erapy
greay
angen.
usng
a
Webrand
crcuang
n
acor
dsease
vWF
VIII
s
and
eves
a
a
a
norma
e
ead
o
prmary
quany,
abnormay
Hemophilia
Severe
IX
sze,
and
uncon
son
o
o
cump
Disseminated
(aggunaon),
an
many
lation
A
caon
ing,
dsorder
cases
are
amy
a
caused
sor y.
decences
cences
o
may
disorder
afeced
by
new
Severe
acor
ony
caused
ndvduas
muaons;
emopa
VIII
manes
ater
n
A
(acvy
by
are
s
deciency
maes.
e
remander,
1000
(chronic
g)
myeloid
leukemia,
primary
myelofibrosis)
Lymphoid
fetus
abortion
Amniotic
Splenomegaly
(weight
Complications Myeloproliferative
Abruptio
of
Coagulation
leukemias
(chronic
lymphocytic
leukemia
and
hairy
cell
leukemia)
embolism
Lymphoma
Toxemia
Infectious
Storage
diseases
diseases
(e.g.,
(e.g.,
malaria)
Gaucher
disease)
Infections
Moderate Sepsis
(gram-negative
and
Mountain
Chronic
spotted
(weight
500
to
1000
g)
gram-positive)
Meningococcemia
Rocky
splenomegaly
fever
vein
congestive
splenomegaly
(portal
hypertension
or
splenic
obstruction)
Histoplasmosis
Acute
Aspergillosis
Hemolytic
leukemias
anemias
nohemolytic
(hereditary
spherocytosis,
thalassemia,
immu-
anemia)
Neoplasms
Amyloidosis Adenocarcinomas
of
pancreas,
prostate,
lung,
and
stomach Niemann-Pick
Acute
promyelocytic
Chronic
Massive
Tissue
disease
leukemia
Injury
infections
(tuberculosis)
Sarcoidosis
Trauma
Mild
splenomegaly
(weight
80%
10%
(coinfection);
100%
Detection
of
serum
Detection
antibodies
of
antibody
for
HBsAg
to
or
ELISA
HBcAg;
HBV
for
antibody
detection;
DNA
HCV
PCR
Detection
for
IgG
Double-stranded
ssRNA,
2005,
quence
o
o
HBV
onger
HBeAg
HBcAg,
rsk
o
hepatitis
B
infectious
cronc
n
muaons
and
and
ncreased
core
antigen;
diseases
encodes
necon.
cronc
acqured
regeneraon
genome
HBsAg,
hepatitis
B
of
the
liver.
In
RNA
core
proten
poypepde
(epas
surface
RNA
antigen;
Iacobuzio-Donahue
o
durng
sur vvng
severa
he
epas,
e
rsk
or
key
as
CA,
epao-
he
conse-
an
proonged
perod
deeced
epaocyes.
proens
a
ave
o
paogenc
Be
(HBcAg,
w
a
epas
precore
and
B
core
core
angen)
regon,
serum
usng
sympoms
necons,
and
desgnaed
in
IgM
and
serum,
in
D
liver
hosts
Detection
HDV
IgM
or
of
and
only
serum
IgG
antibodies;
biopsy
antigen;
HEV
ELISA,
PCR
angen)
enzyme-linked
immunosorbent
Gastrointestinal
and
liver
pathology,
e
HBsAg
w
HBV
requred
paogeness
or
o
vrus
repcaon
HBV-assocaed
and
ver
as
been
cancer
Subclinical
oowed
peaks
Sma
ess.
durng
ypcay
HBsAg
persss
o
s
e,
monorng
HBV
DNA
beore
dsease.
undeecabe
deeced
or
by
o
appears
sympomac
decnes
anbody
and
cncay
amouns
soon
ater
provdng
In
eves
12
HBsAg
proecon
(ndcave
an-HBc
HBsAg
and
s
o
persss
DNA
IgM
epaocye
repaced
n
and
by
e
IgG
an-HBc
IgG
njur y).
serum
or
an-HBc
s
Over
an-HBc
more
an
anbody.
dagnosc
o
e
nex
anbody.
acue
6
In
ew
mons,
hus,
mons,
e
necon,
Acute
presence
wereas
disease
hepatitis
20
40%
Chronicity
Cirrhosis
scarring
per
without
year
years
liver
failure
30% (~20%
of
chronic
~1.5%
126 mg/dL
cronc
yperpospaema.
a
Adipose
cema
cases
a
•
or
resung
mon
•
wc
paraneopasc
In
be
or
dsease,
o
dsease.
umors,
a
esmaed
PTH
mu a ons
seng
s
ncude
c arc noma.
ass o c ae d
es
e
ns anc es ,
may
dabees.
organs.
com-
exc ess ve
p ara y rod
parayrod
ncreases
ng
more
cum eves, and e cnca probems are reaed many o e rena
a
an
Saes;
enoug
Insulin
occurs
and
g
dsorder
c aus e d
re ar rangemen s
bood
Many
ypercacema,
muc
Uned
dabec, and a one rd o ese peope are unaware o er dsease.
reeasng
bood
MEN1
excreon
overacvy
Compensaor y
o
sen
ess.
common y
gene
gene
depresses
pospae
cncay
yp er p as a
o
aure.
common y,
are
cacum
decen
common
ne ary
L ess
genes
suppress or
Hypercacema
as
(by
cacum;
eevae
prmar y
rena
ad enoma
16. 6).
wo
a
or
as
o
producon.
bood
yper paratyrodsm
decreased
urn
n
umors:
umor
S econdary
men
p ara y ro d
Abnor ma es
y rod
n
a
o
roune
p ara y ro d
( Suppemen a
g andu ar
an
s
cause
durng
rom
o
sm-
wc
reeasng
cacum
ser ve
cacum
cacum
(PTH),
breakdown
PTH
cronc
bood
converson
excessve
sem
o
requen
women
c aus e d
o
may
e
reguae
reabsorpon
ncreases
acves
w
o
o
ereby
ncreases
urer
secondar y
deeced
n
ese
assocaed
be
ubuar
wc
y per paraty rodsm
e
usuay
orm;
s
ormone
excreon,
ncreases
A
Hyper paratyrodsm
or
rena
kdneys,
rac;
are
concenraons
ncreases
e
gands
parayrod
pospae
cacum.
parayrods
gands
parayrod
pospae-bound
acve
cum
o
producon
ncreases
More
GLANDS
uptake
caccaon.
Lipogenesis
Hypoparatyrodsm
remova
o
s
parayrod
rare
and
gands
s
mos
durng
oten
yrod
caused
or
by
oer
nadveren
neck
Lipolysis
surger y.
he mos requen cnca manesaons are ncreased neuromuscuar
rraby
(eany)
ENDOCRINE
Mos
o
dgesve
e
a
ac
pancreas
o
produce
e
e
poypepde,
nsun
cardac
arrymas.
PANCREAS:
enzymes
componen
and
s
no
composed
e
pancreas
eac
s
e
sets
nsun,
secreed
or
o
duodenum
ormones
producon
DIABETES
uncon
by
a
exocrne
(see
of
13).
Langerans,
gucagon,
dsnc
causes
gands,
Caper
wc
he
wc
somaosan,
popuaon
dabees,
wc
o
s
secree
endocrne
conan
and
ces.
one
o
ces
Insulin
pancre-
Decen
e
grea
medca scourges o e modern word and e ocus o e dscusson a
oows.
Overview
of
Diabetes Liver Striated
Diabetes
mia,
is
a
resulting
metabolic
from
disorder
defective
characterized
production
or
by
inadequate
action
of
insulin.
e
because
Glucose
uptake
Glycogen
ncdence
one
o
o
e
s
wo
dsease
major
as
rsen
orms
o
aarmngy
dabees
n
recen
(ype
2
years,
Protein
aer)
s
assocaed
w
obesy,
an
ncreasng
Gluconeogenesis
synthesis
Glycogen
synthesis
synthesis
Lipogenesis
dabees, Fig.
dscussed
muscle
hyperglyce
probem
16.7
muscle,
Insulin
adipose
physiology.
tissue,
and
Metabolic
liver.
actions
of
insulin
in
striated
CHAPTER
16
Endocrine
System
B
A
Supplemental
is
delineated
variation
ogy,
in
eFig.
from
nuclear
University
of
16.6
the
Parathyroid
residual
size
and
Chicago,
adenoma.
normocellular
occasional
Chicago.)
follicle
(A)
gland
In
on
this
the
formation.
low-power
upper
view,
right.
(Courtesy
Dr.
(B)
a
solitary
hypercellular
High-power
Nicole
Cipriani,
detail
adenoma
shows
Department
minimal
of
Pathol-
272.e1
CHAPTER
Ora
uaes
by
nake
nsun
ceran
acs
a,
va
bood
e
ood
ormones
e
us
o
rases
producon
nsun
gucose.
I
degradaon
e
aso
o
eve
se
(ncretns)
recepor
provdng
e
rom
o
smuaes
and
gucose
ces,
reeased
ncrease
subsrae
pds
o
or
e
an
n
rom
gucose
upake
so
o
s
bood
a
s
nesna
upake
generang
proens,
e
efec
amno
ne
ces.
no
energy
nsun
wc
Insun
eves
ay
nbs
anaboc.
e
ver,
urer
nsun
are
ces
pancreac
n
reducng
couneraced
ses.
gycogen
breakdown
n
gucose.
bood
eves
acae
syness,
n
bood
gucose
gucagon,
he
major
Durng
asng
gycogen
aemp
o
a
eves.
n
saes,
e
o
a
ow
we
e
s
and
o
o
o
by
α
smuae
an
g
ncrease
gucagon
decreasng
bood
efecs
produced
eadng
nsun
norma
o
s
gucagon
ver,
breakdown
manan
Many
ormone
uncon
(gycogenoyss)
epac
an
by
gycogen
gucose.
of
•
are
s
a
nlammasome
(suc
reduced
sae
n
(see
as
secrees
promoe
o
ces
e
n
2),
e
and
we
and
sensng
smuang
nereukn-1),
some
sensvy
ressance;
acvae
Caper
c yoknes,
nsun
obesy
epn
273
wc
o
o
epn
(3)
ree
paway
e
produc-
nduce
nsun
β ce dysfuncton. ce uncon may ncrease eary n e deveop-
men o T2D, n response o ncreased bood gucose, bu umaey,
deecve
men
ay
e
o
ce
over
acds
uncon
dabees.
dened
(wc
raer
an
o
an
or
essena
genec
be
gucose
deecs;
an
conrbuor
dysuncon
or
efec
o
may
se
nsun-reeasng
may
s
s
s
(pooxcy)
producon
poory
Diabetes
eves
ere
accumuae
c yoknes
ssue
epn)
System
ressance.
od
Pathogenesis
e
o
a
adpose
and
ncreased,
acds
on
(2)
adponecn
are
caed
In
addon, nsun reduces e generaon o gucose rom gycogen sores
n
sgnang;
(adponecn
ssues;
and
reducng
and
are
sm-
musce
and
acds
efecs
and
augmened
Endocrine
16
be
o
due
e
o
(gucooxcy);
ormones
rom
repacemen
o
ong-sandng
ses
ree
deecs
e
se
deveop-
excess
n
nesne;
w
amy-
dysuncon
cause).
The two major forms of diabetes, type 1 (accounting for 5% to 10% of
cases) and type 2 (90% of cases), are caused by different mechanisms.
Type
1
Type
1
attack
As
and
Diabetes
diabetes
and
n
e
uaon
mos
are
sysem
s
an
ces
no
a
e
varans
an
HLA
A
a
e
reason
genes
ncreased
II
or
in
genes.
which
of
wy
or
se
n
e
wy
envronmena
cells
Abou
5%
ces
dsease,
ore-
reguaon
s
afecs
acors,
s
reg-
o
and
of
Diabetes
cases
are
arbuabe
expressvy
a
o
oow
snge
gene
deecs
Mendean
w
g
nerance.
he
pen-
mos
common o ese s maturty-onset dabetes of te young (MODY), wc
may
as
mmune
Deecve
bu
T
insulin.
oerance
own
nvoved
rsk
ypoess,
roe
disease
deciency
ndvdua’s
n
cass
popuar
known.
in
dseases,
w
beng
s
autoimmune
resulting
aacks
dferen
ese
T
is
cells,
assocaed
among
ses
β
auommune
Many
reguaor y
e
(T1D)
mmune
unknown.
Forms
erance
destroy
oer
Other
resu
rom
muaons
n
one
o
severa
genes
nvoved
n
ce
uncon. Congenta eary-onset dabetes, wc s usuay deeced n e
neonaa perod, s caused by muaons n e nsun or nsun recepor
gene
or
genes
a
afec
recepor
expresson
or
sgnang.
Dabees
may
aso appear durng pregnancy (gestatona dabetes), especay n women
by
ony
ncudng
Obesity
necons
bu
no
cear
and
mcrobome
esabsed.
a
paens.
T
and
Muc
ympoc yes,
desrucve
are
e
useu
B
o
Regardess
ces
e
wc
a
ce
k
markers
s
or
o
reac
e
ces,
s
and
e
dsease,
se
by
CD4+
specc
bu
er
T
s
are
CD8+
ces,
or
suspeced
mecansm,
angens
caused
by
Anbodes
mcrobes),
underyng
w
damage
se
nlammaon.
desrucon
(commensa
s
ce
conrbuon
Vasculature
n
c yooxc
wc
se
presen
T
Adipocytes
nduce
angens
o
ce
unceran.
FFAs
Adipokines
Type
2
Diabetes
Type
2
diabetes
resistance
in
(T2D)
is
peripheral
a
complex
tissues
disease
(failure
to
resulting
respond
to
from
insulin
insulin)
and
β Insulin
cell
for
dysfunction
the
plasma
T2D
glucose
remans
env ronmen a
(Fg .
manifested
a
as
insulin
secretion
that
is
resistance
inadequate
level.
p o ory
ac ors ,
und erso o d
and
d s e as e
n amma on
a
n
w c
s e em
o
gene c s ,
p ay
a
Pancreatic
ro e
β-cell
β-cell
compensation
failure
islet
16.8).
β
•
Inflammation
Genetcs.
80%
o
T1D).
Genec
90%
acors
are
concordance
Despe
many
ceary
n
sudes
nvoved,
denca
and
e
as
wns
evdenced
(even
more
dencaon
o
by
cells
e
an
n
dozens
o
Insulin
genec
poymorpsms
a
are
sascay
assocaed
w
T2D, secretion
an
undersandng
o
ow
genec
varans
cause
nsun
by
or
•
ce
dysuncon
remans
Increased
Normal
Decreased
ressance β
cells
eusve.
Obesty. Obesy s assocaed w e deveopmen o nsun ress-
Blood
Normal
to
impaired
Type
2
Normal
ance,
a
even
and
s
n
e
absence
ocaon
(cenra
o
ypergycema.
more
an
e
perpera)
amoun
o
nluence
body
e
glucose
deveopng
T2D.
s
assocaon
as
ed
o
e
erm
or
e
combnaon
o
vscera
obesy,
16.8
gucose
with
Pathogenesis
obesity
cardovascuar
dsease,
and
abnorma
pd
proes.
meaboc
promoe
uar
nsun
syndrome
ressance
rgycerdes
and
are
by
a
g
mupe
producs
o
rsk
or
T2D.
mecansms:
ay
acd
of
type
induced
by
2
diabetes.
adipokines,
Insulin
free
resistance
fatty
acids,
and
associ-
chronic
in
adipose
tissue.
Pancreatic
cells
compensate
for
insulin
Indvduresistance
as w
is
noerinflammation
ance,
diabetes
metaboc ated
syndrome
tolerance
rsk Fig.
o
glucose
Obesy
(1)
may
nrace-
meabosm
nb
by
hypersecretion
compensation
free
fatty
is
acids.
resistance
and
followed
by
(Reproduced
pancreatic
of
insulin.
-cell
with
-cell
However,
failure,
and
permission
failure.
J
Clin
at
some
diabetes
from
Invest
point,
ensues.
Kasuga
M:
116:1756,
-cell
FFA,
Insulin
2006.)
274
CHAPTER
Endocrine
16
System
wo are aready predabec; pregnancy-assocaed ormones avor nsu-
e
n
ve oxygen speces, ncreased procoaguan acvy o endoeum,
ressance.
In
rare
cases,
dabees
may
resu
rom
desrucon
pancreas by cronc pancreas or emocromaoss,
exocrne
pancreas
a
secondary
afecs
e
o
e
or a umor n e
producon
proeraon
ses.
marx.
bu
Clinicopathologic
The
morbidity
complications
he
cassc
(requen
Features
associated
of
with
of
hyperglycemia
cnca
urnaon,
Diabetes
diabetes
and
presenaon
due
o
e
the
o
osmoc
is
og y,
mainly
resulting
T1D
efec
n
due
to
chronic
vascular
s
e
o
gucose
rad
o
n
•
injury.
toxc
bood
depees
o
o
conras,
bdy
o
bo
s
mos
dscovered
orms
resus
ndvduas
on
roune
rom
e
w
T2D
are
aboraor y
cronc
asympomac;
esng.
compcaons
he
o
mor-
areres;
sma
ckenng,
he
ve
e
•
mos
o
bood
wereas
severey
dsrupon
ssue
njur y
vesses
arger
afeced
o
e
nvoves
deveop
areres
organs
bood
a
deveop
are
a
(Fg.
ree
basemen
acceeraed
ose
suppy
eas
dfuse
are
16.9).
paogenc
he
by
•
membrane
gucose-derved
proens,
a
o
a
process
recepor
caed
nlammaor y
vascuar
a
ces
smoo
s
moecues
acceeraed
RAGE
(recepor
(macropages
musce
ces.
suc
by
o
or
and
Bndng
as
gyoxa
AGE)
T
a
ces),
or
AGEs
s
bnd
expressed
endoeum,
o
RAGE
on
ceuar
AGEs
on
and
eads
o
te
conrbuors
s
no
because
requre
meabozed
coacor
an
a
s
vascular
In
o
e
dened
cs
n
paways,
as
an
undened
marx
we
afecng
ncreased
os
and
vascuar
roe,
pao-
ncrease
ssues
or
(ner ve,
gucose
n
or
a
and
ens,
upake,
reacon
e
a
regeneraon
(see
dscuss
TGF-
some
due
o
o
Caper
Cataracts
infarct
Atherosclerosis
Islet
cell
loss
Insulitis
Amyloid
(type
(type
Nephrosclerosis
Glomerulosclerosis
Ar teriosclerosis
Peripheral
Pyelonephritis
vascular
atherosclerosis
Gangrene
neuropathy
Infections
neuropathy
complications
of
diabetes.
acor
o
e
wc
smuaes
producon
1).
o
act-
severa
grow
(wc
ac-
smuaes
neovascuarzaon
(wc
e
In
smuaes
1)
2)
mos
serous
addon
necons.
reduced
abnormay.
Myocardial
o
organs.
suscepby
deenses
dacygycero,
enzyme
grow
Glaucoma
Chronic
exraceuar
produc-
proens).
dferen
mmunoogca
to
ncreased
Retinopathy
16.9
gucose
sorbo
hs
infarcts
Fig.
of
some
anoxdan
conrbung
renopay)
secon
reduced
o
C.
endoea
Hyper tension
Autonomic
o
reac-
pysoogc
e
nsun
o
converted
knase
proeraon,
exraceuar
nex
aso
eadng
vascuar
dabec
esons
sow
relecs
s
proten
Hemorrhage
Peripheral
a
o
requred
mporan
Microangiopathy
Cerebral
ser ve
concentratons
hs
do
s
a
gucose
enzyme
suc
seen
and
syness
acves
o
sress.
endoea
paways.
ypergycema.
vesses)
guaone,
oxdave
ors
Advanced gycaton end-products (AGEs) are ormed by neracons
beween
ntraceuar
gucose
Intraceuar
sgnang
sens-
deveopmen
major
and
generaon
aer.
NADPH,
reduced
vates
aerosceross.
parcuary
are
ces,
ese
acors,
hese ces ereore ave ncreased suscepby o damage caused
poory
conroed bood sugar, parcuary damage o sma and medum-szed
grow
and, n e seng o ypergycema, nraceuar gucose eves rse.
Inraceuar
By
ey
and
musce
known
consequences.
and poypaga (excessve eang, due o ssue “sar vaon” n e mds
peny).
cyoknes
smoo
tssues,
poydpsa (requen drnkng, due o deydraon rom urnar y osses),
ypergycema
o
no
descrbed
kdney,
urne),
s
dabees
some
ave
poyura
e
In
I
o
I
ssue
o
s
and
ese,
no
bood
we-
dabe-
cear
suppy
s
or
an
CHAPTER
Vascular
hallmarks
of
diabetic
vascular
disease
are
accelerated
and
hyalinization
of
small
and
medium-sized
o
gomeruar
ar Pathogeness.
he
ypergycema-assocaed
abnormaes
o
proeraon
o
vascuar
endoea
and
and
eson
ces,
smoo
deposon
arera
o
exraceuar
basemen
membrane,
marx
a
proens
propensy
n
or
severe
e
sma
vesse
e
and
cronc
umens
o
nlammaon.
vesses
and
Coecvey,
acceerae
ese
processes
agng-assocaed
o
vascuar
compromse
and
aso
he
consequences
o
e
vascuar
esons
are
Myocarda nfarcton s e mos common cause o dea n dabecs.
Iscemc
necross
dabecs
of
an
te
egs
(gangrene)
s
100
mes
more
n
e
dsease
o
genera
e
(mcroangopaty)
capar y
basemen
caracerzed
membranes
by
eyes,
and
complications
leading
other
o
an
n
ckenng
necons
11)
nondabecs;
o
and
an
he
e
ave
do
gomeruar
u-bown
vascuar
a
vascu-
prevaen
s
and
caracerzed
wa
o
e
areroes.
by
Paens
a
ger
ncdence
normogycemc
o
pyeone-
ndvduas.
dsease
rena
neproc
presens
dsease
rom
syndrome.
w
proenura
a
Abou
combnaon
o
40%
o
a
paens
esons
causng
wdespread
scemc
gomeruar
scar-
damage.
Retinopathy
ner ves,
to
descrbed
diabetes
scarring
include
glomerular
(glomerulosclerosis),
disease
a
lesions
affecting
retinal
blood
vessels,
and
vision.
renopay
e
ages
o
25
s
e
and
75.
prncpa
here
cause
may
be
a
o
vsua
genec
mparmen
predsposon,
some
as
well
paens
wereas
w
oers
unconroed
w
ypergycema
reasonabe
bood
never
gucose
deveop
conro
do.
as
Pathogeness.
vas-
he
paogeness
o
dabec
renopay
s
compex
and
ncompeey undersood. he ce rsk acor s susaned ypergycema,
may
ead
of
(see
smuae
e
producon
o
cyoknes
s
o
e
ncreased
syness
o
marx
beeved
o
damage
vesses
due
o
aeraons
n
bood
low,
or-
and maon
acors
result
nex.
lesions.
AGEs
the
compromise
esons
renopay
of
is
seriously
wc Pathogeness.
grow
more
dfuse
underes
Nephropathy
and
bo
popuaon.
because
cular
o
end-sage
and
beween kdney,
Chapter 11),
yane
Features.
progress
Dabec ckenng
Renal
areroosceross,
s
common
can
Sma-vesse
Diabetic
dabecs
Caper
Retinopathy
e
n
prone
(see
Diabetic
o
Hyane
yperenson,
evden
•
•
bross.
w
ssues.
•
n
by
ubuar
scema.
rng numerous
caused
w
narrow
deveop
n
areroes
aerosceross,
may
Clncal Features.
o
neprosceross,
o
Clncal eadng
n
wa
romb
prs orm,
narrowng
resu
mus-
are and
nersa
assocaed
amorpous, ce
esons,
may
descrbed more
ead
dsease
arteries. aropy
above
275
atheromcrovascuar
sclerosis
System
Lesions addon
The
Endocrine
16
o
AGEs,
and
possby
oer
mecansms.
hese
vascuar
canges
proens nay ead o mnue emorrages, scema, sma narcs (coon woo
n
e
gomeruar
mesangum.
Mcrovascuar
dsease
eads
o
reduced spos), and macuar edema, a o wc mpar vson. I scema s severe,
bood
low
and
acvaon
o
e
renn–angoensn
sysem,
wc
comoca producon o VEGF nduces neoangogeness (proerave renop-
pensaes by ncreasng low roug e gomeru. he resung gomeray), uar
yperraon
and
ncrease
n
vascuar
pressure
n
e
wc
s
emorrages. may
ave
deeerous
efecs
on
e
gomeruar
oten
assocaed
w
more
exensve
rena
and
vreous
pacng
racon
gomeru
permeaby
hese
may
organze
and
undergo
bross,
barrer. on
e
rena
a
eads
o
rena
deacmen,
mpared
vson,
and
even
Many oer abnormaes n sgnang paways n gomeruar epea bndness. ces
bu
(podocyes)
er
and
proens
conrbuon
o
e
o
e
esons
s
dapragm
remans
ave
been
repored,
uncear. Morphology.
ave. Morphology.
e
soogc
amarks
o
dabec
gomeruar
are
deposs
o
marx
maera
n
e
mesangum
and
dsease
may
be
renopay
s
nonproerave
caracerzed
or
by
proer-
ckenng
dso
ease
Rena
Nonproerave
capares,
aneur ysms,
emorrages,
edema,
and
exudaes
o
capeaked pasma proens and pds. Proerave renopay s a pro-
ar y
wa,
dfuse
gomeruar
basemen
membrane
ckenng,
and cess
progressve
deposed
scarrng
n
e
(Fg.
16.10).
gomeruus
Somemes,
appears
e
noduar,
marx
gvng
o
rse
o
noduar
gomeruosceross
(Kmmese-Wson
vesse
ormaon
and
bross.
e Clncal
erm
new
maera
esons).
Features.
Vsua
mparmen,
somemes
even
can
A
resu
rom
proerave
renopay,
especay
B
Fig.
men
16.10
from
thickened,
Diabetic
a
patient
tortuous
tesy
Dr.
Lisa
Y erian,
lam,
Department
of
nephropathy.
with
(A)
Nodular
long-standing
afferent
arteriole.
Department
Pathology,
of
glomerulosclerosis
diabetes.
The
University
(B)
Severe
amorphous
Pathology,
of
oa
bndness,
In
nature
University
T exas
of
Health
(Kimmelstiel-Wilson
renal
of
hyaline
the
thickened
Chicago,
Science
lesions)
arteriolosclerosis.
Chicago.
Center,
vascular
B,
San
wall
Courtesy
Antonio,
in
Note
is
Dr.
a
renal
the
evident.
M.A.
T exas.)
speci-
markedly
(A,
Cour-
Venkatacha-
e
macua
s
276
CHAPTER
afeced.
Organzaon
and
Endocrine
16
bross
o
vreous
System
emorrages
rom
e (Fg.
newy
ormed
vesses
can
cause
rena
deacmen.
In
addon
o
16.11B).
composed rena
dsease,
paens
are
prone
o
deveopng
caaracs
and
sow
s
conras,
uncona
norma-appearng
adenomas
ces
are
surrounded
soary
by
a
esons
capsue
D).
more
Carcnomas
aypa
and
are
ave
uncommon;
a
endency
n
o
ese
(Fg.
nvade
magnances,
vens
and
ces
ympa-
Neuropathy cs.
s
o
gaucoma. 16.11C,
Diabetic
By
e
ypcay
a
symmerc
perpera
neuropay
o
e
egs
a
W
unconng
adrena
umors,
bo
bengn
and
magnan,
afecs e adjacen adrena corex and a o e conraaera adrena gand
many
sensory
nerves
bu
may
aso
mpar
moor
uncon.
Auonomc are
aropc
as
a
resu
o
suppresson
o
endogenous
ACTH
produc-
neuropay aso occurs, resung n bowe and urnary dsurbances. hese on canges
are
probaby
e
resu
o
mcroangopay
afecng
vesses
by
g
corso
eves.
Carcnomas
o
oer
organs
measac
o
supe
adrenas
bu
usuay
are
muc
more
common
an
prmary
adrena
cancers,
pyng e nerves, bu may aso ave a componen o drec axona damage. cause
ypoadrenasm,
no
Cusng
syndrome.
Acute Diabetic Ketoacidosis and Nonketotic Hyperosmolar Coma
Aoug
n
cronc
dabecs,
moray
paen
uary
on,
n
e
and
gucose
o
markedy
Insun
eves
as
worsens
aernave
or
and
consue
s
(and
e
occasonay
o
as
rggers
source
o
Excessve
deveopng
500
o
osmoc
1
700
o
(parcuary
a
edema,
e
meaboc
wc
can
o
s
parc-
de,
nec-
dabees
n
may
bood
ypergycema
severe
deydraon.
keones,
bran)
acdoss
be
and
n
dabees,
ncreases
acdc
or
presens
aered
eve
n
probems
morbdy
known
hs
resung
2
or
on
generang
o
ype
sudden
mg/dL.
cnca
o
dsease
dabees
eadng
eads
cerebra
e
compcaes
duress,
energy
keoss
ow
ype
poyss,
major
cause
supermposed
mbaance,
g
e
sress
e
eadng
oten
Unrecognzed
ypes
decency
rsk
dabees
meaboc
sarvaon.
e
1
obese.
oer
e
o
ype
keoacdoss
popuaon)
n
worsen
an
compcaons
acue
aa
wc
durng
and
are
saes
ncreases
s
no
rec-
ognzed and reaed mmedaey. Deydraon and eecroye mbaances
mus
may
be
careuy
deveop
correced
yperosmoar
e
paen
nonkeoc
s
o
coma.
survve.
s
Type
syndrome
2
dabecs
resus
rom
severe deydraon due o susaned osmoc duress n ndvduas wose
waer nake s nadequae. Afeced paens are ypcay oder adus wo
Clncal
Features.
enson
and
runca
obesy,
ror
neck
aropy
musce
and
o
“moon
back
mass
and
secondar y
brused,
e
resorpon
cods
a
o
o
mensrua
ncudng
rena
on
o
area
bone
suppress
varey
o
e
e
usuay
s
mb
e
skn
and
assocaed
becomes
and
a
caused
meanoc ye-smuang
o
a
and
by
paens
rage
a
o
o
skn
e
seecve
decreased
and
s
easy
n
e
gucocor-
ncreased
ncude
rsk
or
rsusm,
sympoms,
psycoss.
Exraad-
ACTH
pgmenaon
ACTH
nduce
resung
ncreases
ecopc
as
pose-
parcuary
psycarc
or
yper-
e
ces,
B ecause
are
rank
puar y
ncreased
by
C orso
oseopoross.
and
n
causes
(srae),
manesaons
acvy
a
Gucocorcods
16.7).
number
w
manesed
resuan
gucose
n
eFg.
response,
w
o
emorrages
depresson,
syndrome
w
weakness.
upake
Addona
presen
ssue,
Hypercorsosm
consequen
swngs,
adpose
accumuaon
(Suppemena
mmune
o
myobers,
cuaneous
abnormaes,
Cusng
and
II)
nb
necons.
mood
ypercorsosm
ump).
(ype
dabees.
abdomna
aces, ”
proxma
and
eadng
w
redsrbuon
(bufao
as-wc
guconeogeness
n
Paens
cenrpea
secre-
secondar y
precursor
moecue.
ave been dsabed by sroke or some oer debang ness.
Hyperaldosteronism
ADRENAL
GLANDS
Excessive,
chronic
overproduction
of
aldosterone
causes
hypertension. Eac
adrena
gand
consss
o
wo
dsnc
regons,
e
corex
and
•
Prmary
yperadosteronsm
s
caused
mos
oten
by
baera
nod-
medua. he corex produces ree ypes o serod ormones: gucocoruar cods
(many
corso),
mneraocorcods
(adoserone),
and
sex
yperpasa
(esrogens
and
androgens).
he
medua
produces
epneprne.
Mos
o
e
known
dseases
o
e
adrena
reaed
o
excessve
or
deecve
uncon
o
e
gands
or
an
adrena
umor,
mos
a
soar y
adrena
n
e
adenoma.
kdney,
Adoserone
eadng
o
lud
ncreases
reenon
and
sodum
ncreased
gands bood
are
adrena
caecoamnes, reabsorpon
many
e
secommony
rods
o
pressure.
Because
rena
bood
low
ncreases,
e
producon
corex. o renn n e kdney s reduced. Paens presen w yperenson,
and up o a rd ave reduced serum poassum (because o reduced
Cushing
Syndrome:
Hypercortisolism
reabsorpon This
syndrome
is
caused
by
increased
levels
of
ncreased resulting
in
metabolic
and
other
S econdary
n In
cnca
pracce,
s
e
admnsraon
kdneys).
adoserone
Dagnosc
and
e
mos
common
cause
o
yperadosteronsm
response
reduced
aboraory
renn
ndngs
are
acvy.
o
serods
o
rea
o
acvaon
o
s
e
caused
by
adoserone
renn–angoensn
producon
sysem,
seen
n
Cusng condons
syndrome
e
serum
abnormalities.
•
Pathogeness.
n
glucocorticoids,
nlammaory
o
reduced
rena
peruson,
as
n
vascuar
dseases
o
e
dskdney
and
congesve
ear
aure.
I
aso
s
a
bass
or
yperen-
eases. Endogenous Cusng syndrome may be caused by ncreased ACTH son. producon
by
a
puary
adenoma
(aso
caed
Cusng
dsease,
∼70%
o
cases), a umor or yperpasa o e adrena corex (15% o 20%), or eco-
Adrenogenital pc
ACTH
producon
by
some
oer
umor,
suc
as
sma
ce
ung
Excessive cer
(∼10%).
In
a
orms,
urnary
ree
corso
concenraon
s
puary
Cusng
dsease
and
Cusng
syndrome
caused
production
secreon,
serum
ACTH
eves
are
eevaed
due
o
by
oss
eedback
conro
by
corso.
Wen
Cusng
syndrome
s
umor
or
prmary
yperpasa
o
e
adrena
corex,
causes
changes
in
ACTH
are
produced
n
e
gonads
and
adrena
corex.
e
nega-
caused
eves
corex
produces
precursors
a
are
convered
o
esoserone
by
n a
hormones
ecopc
o
adrena ve
androgenic
organs.
Androgens ACTH
of
ncreased.
genital In
Syndromes
can-
perpera
ssues.
Unke
gonada
androgens,
adrena
androgens
are
are
reguaed
by
ACTH.
under
nluence
Excessve
adrena
androgens
may
be
produced
beow norma because eedback nbon s nac.
e
genec
an Morphology.
Paens
w
ACTH-dependen
Cusng
dsease
auosoma
dfuse
yperpasa
o
e
adrena
corex
(Fg.
ACTH,
by
congenta
recessve
dsease
adrena
adrena
n
wc
umors,
or
n
yper pasa
enzymes
an
uncommon
(CAH).
nvoved
n
CAH
s
corso
syndrome bosyness,
sow
o
caed
16.11A).
mos
oten
21-ydroxyase,
are
deecve.
Because
cor-
Prso
producon
s
reduced,
ere
s
a
compensaor y
ncrease
n
ACTH
mary corca yperpasa s ypcay assocaed w noduar esons, reease
rom
e
puar y
a
secondary
ncreases
e
producon
o
somemes
o
wc are oten dark n appearance due o accumuaon o pouscn adrena
androgens.
he
adrena
gands
are
yperpasc,
CHAPTER
Supplemental
teristic
striae.
WF
features
eFig.
(Reproduced
(editors):
ington,
DC,
16.7
include
Atlas
with
of
American
A
patient
central
permission
Nontumor
Registry
with
obesity,
Cushing
“moon
from
Lloyd
Pathology:
of
syndrome.
facies,”
RV,
Douglas
Endocrine
Pathology,
2002.)
and
Charac-
abdominal
BR,
Diseases.
Y oung
Wash-
16
Endocrine
System
276.e1
CHAPTER
A
Endocrine
16
System
277
B
C
D
Fig.
16.11
adrenal
gland
evident.
adrenal
ing
Cushing
The
glands
from
cortical
There
mild
Department
sze.
ambguous
promnen.
I
e
genaa.
Maes
dsease
In
were
w
gland
(A)
Diffuse
section,
was
presen
in
Mayo
rom
precocous
the
by
neoplastic
its
cells
patient
grs
rsusm
pubery
(B)
solitary,
are
and
with
vacuolated
enarged
adrenal
yellow
gland
and
pigmented
(C)
and
(bottom)
thickened,
Cushing
nodular
Adrenocortical
nature.
because
necrosis
of
not
a
adrenocortical
The
Histologic
presence
seen.
(B,
a
normal
nodularity
in
whom
hyperplasia
adenoma
features
of
with
subtle
syndrome,
adenoma.
(D)
the
are
contrasted
and
of
show-
is
an
distin-
adrenal
intracytoplasmic
Courtesy
Dr.
Aidan
is
both
lipid.
Carney,
Minnesota.)
w
acne
is
circumscribed
activity
presen
the
ACTH-dependent
gland.
Rochester,
and
of
cortex
Primary
adrenal
Mitotic
Clinic,
br,
cdren,
a
adrenal
hyperplastic.
nodules
pleomorphism.
Medicine,
hyperplasia
the
from
hyperplasia
The
nuclear
of
s
cross
diffusely
nodular
pospubera
presen
a
pigmented
adenoma.
is
In
abnormal
prominent
guished
enormous
(top).
syndrome.
are
counres,
Addson
ubercuoss
and
unga
necons
are
mporan
causes
o
dsease.
gen-
as. Paens respond we o serod reamen, wc repaces e deMorphology.
cen
gucocorcods
and
suppresses
ACTH
srunken
due
ympocyc
Adrenal
Cortical
Adrenal
Addison
Insufficiency
(Addison
to
disease,
deciency
progressive
of
multiple
In
adrenocorca
adrenas,
e
corex,
e
necons,
wc
adrena
gands
conans
granuomaous
or
a
are
varabe
ger-ncome
nsuicenc y
reacons
o
e
paogen
may
be
oer
ypes
presen.
destruction
of
the
adrenal
Features.
Cnca
manesaons
become
apparen
ony
ater
cortex an
90%
o
e
gands
are
desroyed.
Paens
presen
w
weak-
hormones. ness,
Pathogenes s.
In
o
Disease)
more leads
aropy
nrae.
nlammaor y
Clncal In
auommune
o
Insufficiency o
Chronic
In
producon.
counres,
(aso
known
60%
as
o
70%
Addson
o
gasronesna
he
skn
rse
o
s
sympoms,
yperpgmened
eecroye
because
e
mbaances,
precursor
and
ypoenson.
poypepde
a
gves
cronc
dsease)
s
ACTH
aso
s
processed
o
reease
meanocye-smuang
or-
due mone, wc rses n response o e ow corso eves.
o
auommune
caed
e
adrenas,
auommune
mos
commony
poyganduar
as
syndrome.
par
One
o
a
dsorder
subype
o
s
Acute syndrome
resus
rom
oss
o
uncon
muaons
n
e
gene
In wc
conros
e
expresson
o
se
angens
n
e
ymus
con ras
e
emnaon
o
se-reacve
T
ces.
Oer
endocrne
adrena
are
subjec
o
auommune
aack
n
afeced
paens
yrod,
parayrod,
puar y,
and
pancreas.
In
d s e as e,
nsu c enc y
may
w c
be
a
s
c ron c
me d c a
and
prog ress ve,
emergenc y.
c aus e
s
ad rena
emor rage
du e
o
co agu a on
Te
mos
d s orders .
ncude
In e
Insuficiency
Adds on
gands
common a
o
and
ac ue ence
Adrenal
AIRE,
ower-ncome
e
s e ng
o
dss em nae d
s epss,
s
cond on
s
reer re d
o
as
278
e
CHAPTER
Waterou s e-Fr der c s e n
manes a on
e y
o
o
sysemc
s epss
sudden
and,
w
are
ad rena
sg ns
ereore,
wo
of
the
mos
adrena
re ae d
mos
o
and
e
( w c
pro du c on )
e- re aen ng
so ck,
bu
a
u nd ery ng
nsu cenc y
re a men
serod
System
a s o
or
s ress
n
ey
produce
a
Pathogeness.
up on
genes,
ACT H
(e
p a en s
Mos
ncudng
cause
o
and
ce
cnca
correcabe
conrbue
o
umors
RET,
von
NF1
ave
(e
sgncance
orm
o
es
n
e
ac
a
yperenson.
muaons
cause
Hppe-Lndau
umorgeness
was
o
n
one
o
severa
neurobromaoss),
syndrome).
dscussed
n
How
ese
Caper
onco-
and
VHL
genes
may
5
Medulla
prmar y
umors
o
e
adrena
medua
are Morphology.
peocromocyoma
her
surgcay
c aus e
o c c urs
suppress es
paragangomas).
var -
nsu cenc y.
Adrenal
common
Te
yp oens on
ad rena
serod
endogenous
undery ng
s
sy mpoms
Ac ue
o
sy ndrome.
cr ss
and
common .
w drawa
Tumors
he
o
Endocrine
16
e
umors
are
usuay
we-dened
masses
a
com-
neurobasoma. press
e
adrena.
ey
range
rom
sma,
crcumscrbed
esons
o
arge, emorragc, cysc masses (Fg. 16.12A). ey are composed o
Pheochromocytoma
ness Pheochromocytomas
are
tumors
of
chromafn
cells
that
n catecholamine
and
other
o
poygona
or
spnde-saped
ces,
conanng
caecoamnes
produce er
granues,
surrounded
by
a
vascuar
nework
(Fg.
16.12B).
hormones. Bengn esons may sow capsuar and vascuar nvason, so e den-
hese
rare
umors
arse
rom
caecoamne-producng
ces
n ng caracersc o magnancy s dsan measass.
e
adrena
medua
(90%)
and
sympaec
ganga
(10%,
aso
A
caed
B
C
D
Fig.
16.12
Tumors
attenuated
(lower
portion).
Granules
(such
toma.
tumor
cortex
as
of
and
(B)
containing
the
The
one
tumor
showing
in
the
adrenal
medulla.
demonstrates
areas
Photomicrograph
catecholamine
the
cells
center
form
extensive
of
(A,
of
Pheochromocytoma.
demonstrating
are
this
not
visible
image),
psuedorosettes
neuronal
B)
hemorrhage.
in
even
around
differentiation.
The
characteristic
this
in
a
nests
preparation.
The
It
is
of
core
arrow
of
points
fibrillary
to
a
tumor
is
residual
cells
not
pheochromocytomas
central
The
(A)
comma-shaped
with
are
material.
neuron.
to
find
benign.
(D)
within
gland
abundant
uncommon
that
enclosed
adrenal
is
cytoplasm.
bizarre
(C)
an
seen
cells
Neuroblas-
Ganglioneuroma,
a
CHAPTER
Clncal
Features.
cromocyoma:
magnan.
may
be
bood
he
he
10%
“rue
are
majory
epsodc,
pressure,
o
en”
s
oten
exraadrena,
o
paens
presenng
assocaed
as
an
w
used
10%
are
presen
abrup
o
w
and
acycarda,
caracerze
baera,
and
yperenson
precpous
eadace,
peo-
10%
are
wc
ncrease
sweang,
n
and
remors. hese paroxysms are arbuabe o e perodc reease o ca-
ecoamnes
e
rom
ormone
e
may
umor.
cause
In
ear
severe
aure,
cases,
e
sudden
myocarda
producon
narcon,
and
do
no
c aus e
prog noss
n