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HYPERSENSITIVITY Dr. Akshay Agarwal
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Hypersensitivity reaction pathology microbiology immunity

Jan 23, 2018

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Page 1: Hypersensitivity reaction  pathology microbiology immunity

HYPERSENSITIVITY Dr. Akshay Agarwal

Page 2: Hypersensitivity reaction  pathology microbiology immunity

Hypersensitivity

-Hypersensitivity (allergy) is an inappropriate immune response that may develop in the humoral or cell-

mediated responses

-Was first termed anaphylaxis

-can be systematic, which often leads to shock and can be fatal, or localized,

which is various atopic reactions

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Types of ReactionsThere are four

types of reactions:

Type I-IgE mediated

Type II-Antibody-Mediated

Type III-Immune Complex-Mediated

Type IV-Delayed-Type Hypersensitivity (DTH)

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Type I: IgE-Mediated Hypersensitivity

• Allergen: a non-parasitic antigen capable of stimulating a Type I hypersensitive response.

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Type I: IgE-Mediated Hypersensitivity

• In immediate hypersensitivity (type I hypersensitivity), the injury is caused by TH2 cells, IgE antibodies, and mast cells and other leukocytes.

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Two Phases

• Immediate Phase : vasodilation, vascular leakage, smooth muscle spasm and glandular secretions

• Late Phase : 2-24 hours later : Mucosal epithelial cell damage by infiltrated leukocytes

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A little background on these mast cells:

• Located in nearly all vascularized peripheral tissues

• Contain many packets of membrane-bound granule, ready for release upon activation by an allergen

• Can also release cytokines

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The chemically active effectors within the granules released via degranulation are called mediators. This group includes:

• Histamines• Leukotrienes• Prostaglandins• Cytokines

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1.Anaphylactic shock

2.Allergic rhinitis

3.Food allergies

4.Asthma

Consequences

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Type 2 Hypersensitivity

• In antibody-mediated disorders (type II hypersensitivity), secreted IgG and IgM antibodies injure cells by promoting their phagocytosis or lysis and injure tissues by inducing inflammation

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Type II-Antibody-Mediated Cytotoxic Hypersensitivity

• Involves the antibody mediated destruction of cells

• Can mediated cell destruction by activating the complement system to create pores in the membrane of the foreign cell

• Can also be mediated by Antibody-Dependent Cell-Mediated Cytotoxicity (ADCC) where the Fc receptors bind to Fc receptor of antibody on the target cell and promote killing

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3 Mechanisms

• Opsonization and phagocytosis

• Complement and Fc receptor mediated inflammation

• Antibody mediated cellular dysfunction

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Opsonization and phagocytosis

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Complement and Fc receptor mediated inflammation

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Antibody mediated cellular dysfunction

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Type III-Immune Complex-Mediated Hypersensitivity

• Immune complex–mediated disorders (type III

hypersensitivity), IgG and IgM antibodies bind antigens

usually in the circulation, and the antigen-antibody

complexes deposit in tissues and induce inflammation.

• The leukocytes that are recruited (neutrophils and

monocytes) produce tissue damage by release of

lysosomal enzymes and generation of toxic free radicals.

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Two Types

• Localised

• Generalised

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Localized Type III Reactions:1. Injection of an Antigen:

• Can lead to an acute Arthus reaction within 4-8 hours

• Localized tissue and vascular damage result from accumulation of fluid (edema) and RBC (erythema)

• Severity can vary from mild swelling to redness to tissue necrosis

1. Insect bite:• May first have a rapid type I

reaction• Some 4-8 hours later a

typical Arthus reaction develops

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Generalized Type III Reactions:• Large amounts of antigens enter

the blood stream and bind to antibody, circulation immune complexes can form

• These can’t be cleared by phagocytosis and can cause tissue damaging Type III reactions

• Serum Sickness-type III hypersensitivity reaction that develops when antigen is intravenously administered resulting in formation of large amounts antigen-antibody complexes and the deposition in tissue

• Other conditions caused by Type III-

1. Infectious Diseases• Meningitis• Hepatitis• Mononucleosis

1. Drug Reactions• Allergies to penicillin and

sulfonamides1. Autoimmune Diseases

• Systematic lupus erythematosus• Rheumatoid arthritis

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Type IV Hypersensitivity• In cell-mediated immune disorders (type IV

hypersensitivity), sensitized T lymphocytes (TH1 and TH17 cells and CTLs) are the cause of the tissue injury.

Generally occurs 2-3 days after T cells interact with antigen

• An important part of host defense against intracellular parasites and bacteria

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Two Phases

• Sensitization phase

• Effector phase

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Phases of the DTH Response

Sensitization phase: occurs 1-2 weeks after primary contact with Ag

What happens during this phase?• TH cells are activated and

clonally expanded by Ag presented together with class II MHC on an appropriate APC, such as macrophages or Langerhan cell (dendritic epidermal cell)

• Generally CD4+ cells of the TH1 subtype are activated during sensitization and designated as TDTH cells

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Phases of the DTH Response

Effector phase: occurs upon subsequent exposure to the Ag

What happens during this phase?• TDTH cells secrete a variety of

cytokines and chemokines, which recruit and activate macrophages

• Macrophage activation promotes phagocytic activity and increased concentration of lytic enzymes for more effective killing

• Activated macrophages are also more effective in presenting Ag and function as the primary effector cell

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What happens if the DTH response is prolonged?

A granuloma develops…• Continuous activation of

macrophages induces the macrophages to adhere closely to one another, assuming an epithelioid shape and sometimes fusing together to form giant, multinucleated cells.

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Protective Role of DTH Response

• A variety of intracellular pathogens and contact antigens can induce a DTH response.

• Cells harboring intracellular pathogens are rapidly destroyed by lytic enzymes released by activated macrophages

Intracellular bacteria Intracellular viruses Contact Antigens

Mycobacterium tuberculosis

Herpes simplex virus Hair dyes

Mycobacterium leprae Measles virus Poison ivy

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Detrimental Effects of DTH Response

• The initial response of the DTH is nonspecific and often results in significant damage to healthy tissue

• In some cases, a DTH response can cause such extensive tissue damage that the response itself is pathogenic

• Example: Mycobacterium tuberculosis – an accumulation of activated macrophages whose lysosomal enzymes destroy healthy lung tissue

• In this case, tissue damage far outweighs any beneficial effects.

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How Important is the DTH Response?

• The AIDS virus illustrates the vitally important role of the DTH response in protecting against various intracellular pathogens.

• The disease cause severe depletion of CD4+ T cells, which results in a loss of the DTH response.

• AIDS patients develop life-threatening infections from intracellular pathogens that normally would not occur in individuals with intact DTH responses.

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Thank You