Immune Response Overview (BIOM 611G, PCOM Georgia)

Summary

This document provides an overview of the immune response, covering both innate and adaptive immunity. It includes information on the various components of the immune system, including physical barriers, cell-mediated responses, and effector molecules. The summary also touches on immune system communication through cytokines and chemokines.

Full Transcript

BIOM 611G, Medical Microbiology
PCOM Georgia

OVERVIEW
OF THE
IMMUNE
RESPONSE
Valerie E. Cadet, PhD
Assistant Dean of Health Equity Integration
Professor of Microbiology and Immunology BMS1 & BMS2
Department of Biomedical Sciences November 21,
EEK…OUR BODY IS UNDER
ATTACK!

Or

The inside out
From the outside in 2
 3 LINES OF IMMUNE
DEFENSE
(NON-SPECIFIC) INNATE
Physical, Biochemical and Microbial Barriers
 External Defenses:
 Skin, mucus membranes and associated hairs (ex: cilia)
 Fluids: sweat, tears, urine
 Commensal bacteria

 Internal Defenses:
 pH: Stomach acid, digestive enzymes in mouth
 Chemicals released from cells and damaged tissues
 Defensins, interferons (IFN), lysozyme, histamine

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 3 LINES OF IMMUNE
DEFENSE, CON’T
(NON-SPECIFIC) INNATE
2. Cellular and Protein Defenses
a. Cells via non-specific recognition of microbial patterns (PAMPs) via cell receptors (PRRs)
 Phagocytes: white blood cells that “eat” foreign matter
 Natural killer cells: surveillance and killing

b. Complement System: lysis of pathogen

c. Inflammation: attracts white blood cells to the area and prevents spread of infection

d. Fever: speeds up the activity of white blood cells and slows down viral replication

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 3 LINES OF IMMUNE
DEFENSE,
(Specific) CON’T
Adaptive Immunity
3. Cell-mediated responses
 B lymphocytes (humoral response mediated by antibodies)
 T lymphocytes (helper and killer cells)
 Memory cells created

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INNATE AND ADAPTIVE
IMMUNE RESPONSES
 The mechanisms of innate
immunity provide the initial
 Adaptive immune responses
develop later and require the
defense against infections: activation of lymphocytes:
 1st and 2nd line  3rd line

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INNATE VS ADAPTIVE
RESPONSES SUMMARIZED
INNATE (native): Non-specific Adaptive (Acquired): Specific
Acquired over a lifetime as an adaptation
Everyone is born with this response
to infection
Response is antigen-independent Response is antigen-dependent
There is immediate maximal Lag time between exposure and maximal
response response
Exposure results in no immunologic
Exposure results in immunologic memory
memory

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 HOW OUR IMMUNE SYSTEM
1.
PROVIDES
Surveillance/Detection
DEFENSE
 Watches the body for signs of damage or disease
 Pattern recognition receptors (innate), antigen receptors (adaptive)

2. Communication
 Cell-to-cell contact
 Chemical messages (cytokines, chemokines)

3. Elicit an effector response
 Attack on antigen
 Sometimes also on self (auto-immunity)
 Potential for Tissue Damage

4. Resolution of problem detected
 Memory (only in adaptive responses)

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https://www.arcr.niaaa.nih.gov/arcr372/article02.htm
 WHAT/ WHO ARE THE
9
MAJOR PLAYERS IN
THE IMMUNE
SYSTEM?
Terminology to Know
COMPONENTS OF THE
IMMUNE SYSTEM
 Cells
 White blood cells

 Tissues/Organs
 Skin
 Bone Marrow
 Thymus
 Lymph nodes
 Spleen
 MALT/GALT

 Effector Molecules
 Complement system proteins
 Cytokines
 Antibodies
 Others
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 OUR IMMUNE SYSTEM
RECOGNIZES
Neoplastic or normal host cells
ANTIGENS
Microbial proteins and carbohydrates

Streptococcus pneumoniae Viral proteins
with polysaccharide
antigens and carrier protein
Environmental factors

Antigen (Ag)
Pollen Animal dander
Substance that reacts with the products of a specific immune response
Molecule recognized by specific receptors on T or B cells  ANTIbody GENerating Agent
May be microbial or otherwise foreign to the body, neoplastic or normal host cell in origin 11
HOW OUR IMMUNE SYSTEM
COMMUNICATES: CYTOKINES
 One of a large group of low-molecular-weight proteins secreted by various cell
types
 Involved in cell-to-cell communication
 Coordinating antibody and T cell immune interactions
 Amplifying immune reactivity

 Cytokines include colony-stimulating factors (CSF), interferons (IFN), interleukins
(IL), and lymphokines, which are secreted by lymphocytes

 Stimulate variety of immunologic functions
 Most have more than one function
 Many have overlapping functions

Mosby's Medical Dictionary, 8th edition 12
HOW OUR IMMUNE SYSTEM
COMMUNICATES:
CHEMOKINES

Any of a group of low-molecular-weight cytokines, ex: IL-8,
identified on the basis of their ability to induce chemotaxis or
chemokinesis in leukocytes (or in particular populations of
leukocytes) in inflammation
 The group is divided into four subgroups on the basis of
genetic, structural, and functional criteria

 They function as regulators of the immune system

Mosby's Medical Dictionary, 8th edition 13
 HOW TO IDENTIFY
A CELL: CD
MOLECULE
Cluster of Differentiation What cell is this?
How can you know?
 Cell surface molecules
 Cells can be identified in vitro and in vivo based on
the types of CD molecules expressed on their
membranes

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 Bacteria

THE COMPLEMENT SYSTEM,
AKA COMPLEMENT
 Series of ~ 30 serum proteins
 Activated sequentially following infection
 Leads to:
 Formation of opsonins
 Proteins which facilitate phagocytosis
 Acute inflammation
 Process whereby neutrophils leave blood stream
and enter tissues in response to tissue damage (ie,
infection)
 Cell lysis
 i.e., kill extracellular bacteria and other
extracellular microbes
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 IMMUNE ACTIVATION CAN
RESULT IN TISSUE DAMAGE
Tissue damage due to:
 Microbe itself
 Cell lysis or tissue damage due to
microbe replication
 Microbial toxins

 Host inflammatory responses

Microbe-induced Host-induced
Tissue damage Tissue damage

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