Fundamentals of Pathology PDF

Summary

This document details fundamental concepts in pathology, specifically focusing on chronic inflammatory responses, including chronic granulomatous disease, and the crucial role of macrophages in resolving inflammation. It explores the underlying mechanisms and steps involved, providing a clear overview of this important medical topic.

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14 FUNDAMENTALS OF PATHOLOGY
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3. Chronic granulomatous disease (CGD) is characterized by poor O2-dependent
killing.
i. Due to NADPH oxidase defect (X-linked or autosomal recessive)
ii. Leads to recurrent infection and granuloma formation with catalase-positive
organisms, particularly Staphylococcus aureus, Pseudomonas cepacia,
Serratia marcescens, Nocardia, and Aspergillus
iii. Nitroblue tetrazolium test is used to screen for CGD. Leukocytes are
incubated with NBT dye, which turns blue if NADPH oxidase can convert
O2 to O2ꜙ, but remains colorless if NADPH oxidase is defective.
4. MPO deficiency results in defective conversion of H2O2 to HOCl.
i. Increased risk for Candida infections; however, most patients are
asymptomatic.
ii. NBT is normal; respiratory burst (O2 to H2O2) is intact.
5. O2-independent killing is less effective than O2 -dependent killing and occurs via
enzymes present in leukocyte secondary granules (e.g., lysozyme in macrophages
and major basic protein in eosinophils).
G. Step 7 - Resolution
1. Neutrophils undergo apoptosis and disappear within 24 hours after resolution of
the inflammatory stimulus.

V. MACROPHAGES
A. Macrophages predominate after neutrophils and peak 2-3 days after inflammation
begins.
1. Derived from monocytes in blood
B. Arrive in tissue via the margination, rolling, adhesion, and transmigration sequence
C. Ingest organisms via phagocytosis (augmented by opsonins) and destroy
phagocytosed material using enzymes (e.g., lysozyme) in secondary granules (O 2-
independent killing)
D. Manage the next step of the inflammatory process. Outcomes include
1. Resolution and healing - Anti-inflammatory cytokines (e.g., IL-10 and TGF-
β) are produced by macrophages.
2. Continued acute inflammation - marked by persistent pus formation; IL-8
from macrophages recruits additional neutrophils.
3. Abscess - acute inflammation surrounded by fibrosis; macrophages mediate
fibrosis via fibrogenic growth factors and cytokines.
4. Chronic inflammation - Macrophages present antigen to activate CD4+
helper T cells, which secrete cytokines that promote chronic inflammation.

CHRONIC INFLAMMATION
I. BASIC PRINCIPLES
A. Characterized by the presence of lymphocytes and plasma cells in tissue (Fig. 2.lB)
B. Delayed response, but more specific (adaptive immunity) than acute inflammation
C. Stimuli include (1) persistent infection (most common cause); (2) infection with
viruses, mycobacteria, parasites, and fungi; (3) autoimmune disease; (4) foreign
material; and (5) some cancers.

II. T LYMPHOCYTES
A. Produced in bone marrow as progenitor T cells
B. Further develop in the thymus where the T-cell receptor (TCR) undergoes
rearrangement and progenitor cells become CD4 + helper T cells or CD8 + cytotoxic T
cells
1. T cells use TCR complex (TCR and CD3) for antigen surveillance.
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Inflammation, Inflammatory Disorders, and Wound Healing 15

2. TCR complex recognizes antigen presented on MHC molecules.
i. CD4+ T cells - MHC class II
ii. CD8+ T cells - MHC class I
3. Activation of T cells requires (1) binding of antigen/MHC complex and (2)
an additional 2nd signal.
C. CD4 + helper T-cell activation
1. Extracellular antigen (e.g., foreign protein) is phagocytosed, processed, and
presented on MHC class II, which is expressed by antigen presenting cells
(APCs).
2. B7 on APC binds CD28 on CD4 + helper T cells providing 2nd activation signal.
3. Activated CD4 + helper T cells secrete cytokines that "help" inflammation and are
divided into two subsets.
i. TH1 subset secretes IFN-γ (activates macrophage, promotes B-cell class
switching from IgM to IgG, promotes TH1phenotype and inhibits TH2
phenotype).
ii. T H 2 subset secretes IL-4 (facilitates B-cell class switching to IgE), IL-5
(eosinophil chemotaxis and activation, and class switching to IgA), and IL-13
(function similar to IL-4).
D. CD8 + cytotoxic T-cell activation
1. Intracellular antigen (derived from proteins in the cytoplasm) is processed and
presented on MHC class I, which is expressed by all nucleated cells and platelets.
2. IL-2 from CD4 + TH1 cell provides 2nd activation signal.
3. Cytotoxic T cells are activated for killing.
4. Killing occurs via
i. Secretion of perforin and granzyme; perforin creates pores that allow
granzyme to enter the target cell, activating apoptosis.
ii. Expression of FasL, which binds Fas on target cells, activating apoptosis

III. B LYMPHOCYTES
A. Immature B cells are produced in the bone marrow and undergo immunoglobulin
rearrangements to become naïve B cells that express surface IgM and IgD.
B. B-cell activation occurs via
1. Antigen binding by surface IgM or IgD; results in maturation to IgM- or IgD-
secreting plasma cells
2. B-cell antigen presentation to CD4+ helper T cells via MHC class IL
i. CD40 receptor on B cell binds CD40L on helper T cell, providing 2nd
activation signal.
ii. Helper T cell then secretes IL-4 and IL-5 (mediate B-cell isotype switching,
hypermutation, and maturation to plasma cells).

IV. GRANULOMATOUS INFLAMMATION
A. Subtype of chronic inflammation
B. Characterized by granuloma, which is a collection of epithelioid histiocytes
(macrophages with abundant pink cytoplasm), usually surrounded by giant cells and
a rim of lymphocytes
C. Divided into noncaseating and caseating subtypes
1. Noncaseating granulomas lack central necrosis (Fig. 2.2A). Common etiologies
include reaction to foreign material, sarcoidosis, beryllium exposure, Crohn
disease, and cat scratch disease.
2. Caseating granulomas exhibit central necrosis and are characteristic of
tuberculosis and fungal infections (Fig. 2.2B).
D. Steps involved in granuloma formation