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Transcript
Immunologic Response

Three functions:

Defense

Homeostasis

Surveillance
Components of the Immune
System

Four components to be discussed:

Cells and tissues of the immune system

Monocyte-Macrophage Cell System

T Lymphocytes (T cells)

B lymphocytes (B cells)
Cells and tissues of the immune system

Pluripotential hematopoietic stem cells

Located within the bone marrow, fetal liver and
yolk sac of the fetus

Stem cells differentiate into 2 types of
“committed” stem cells

produce platelets, erythrocytes (red blood cells),
monocytes or granulocytes.

produces cells of the lymphoid line only
Hematopoietic Stem Cells
Cells and Tissues of the Immune
System

Cells of the immune system are found within the
blood, body tissues, thymus, spleen, liver, lymph
nodes and body areas exposed to the external
environment.

These organs comprise the reticuloendothelial
system (RES).
Reticuloendothelial System
Monocyte-Macrophage Cell System





Derived from stem cell in the bone
marrow.
Monocytes circulate to sites of
inflammation or migrate to various tissues.
Macrophages have cell surface
receptors, one of them being a receptor
for the Fc portion of the immunoglobulin
molecule.
Tissue macrophages possess a receptor
for the complement component C3b.
The presence of antibody and/or
complement enhances phagocytosis.
Monocyte-Macrophage Cell System

Macrophages participate in phagocytosis, inflammation, and
cellular immunity.

Macrophages are mainly involved in nonspecific immunity
and include the phagocytic cells: mononuclear phagocytes,
polymorphonuclear phagocytes (neutrophils), eosinophils and
mediator cells: basophils, mast cells and platelets.
T Lymphocytes (T cells)

Derived from stem cells in the bone marrow.

Leave bone marrow and travel to the thymus to
mature

Approximately 75 to 80% of lymphocytes are T
cells.

Important in recognizing foreign material that is
fixed in the tissues of cells.
T Lymphocytes (T cells)


Play an important role in regulating the
production of antibodies by B cells

Helper T cell

Suppressor T cell

Killer or Killer T cells
T cells have surface proteins known as
cluster determinants (CDs)

Helper T cells are CD4 positive cells enhance
and promote the action of other immune cells.

Suppressor T cells are CD8 positive and have
suppressive or cytotoxic effects
T Lymphocytes (T cells)

Two T-cells, one which recognizes a target
Activated T Cell
B lymphocytes (B cells)

Derived from stem cells in the bone marrow.

Transform into plasma cells and produce a family
of proteins known as antibodies or
immunoglobulins.

Activated B cells begin antibody production and
undergo a process called clonal expansion.
Overview of Antibody
Production

Antigen presented to
T cell and processed.

Presented to B cell

B cell produces
specific antibody

Antibody attaches to
specific antigen
Final Phase Memory Cells
Immune Response

Innate or nonspecific immune response.

Adaptive or specific immune response.
Innate immunity

Involves the body’s first line of defense.

Physical barriers which include intact skin and
mucous membranes.

Physiological factors.

Inflammation
Inflammation

Inflammation is the body's reaction to injury and is
known as the body's second line of defense
which results in:

Increased blood supply to the area.

Increased capillary permeability.

Migration of leukocytes into the surrounding tissue.

These three events manifest symptoms which
include pain, heat, redness and swelling.
Adaptive (specific)
Immunity

Involves ability to recognize self and non-self.

Encounters with non-self or foreign materials results
in production of antibodies (humoral immunity) or
actions of T-cells (cell mediated immunity).

Immunohematology primarily concerned with the
causes and effects of humoral immunity.
Antigens

Any substance which is recognized as foreign by
the body and is capable, under appropriate
conditions, of provoking a specific immune
response.

It is capable of:

Stimulating the formation of antibody and the
development of cell-mediated immunity.

Reacting specifically with the antibodies or T
lymphocytes produced.
Physical Nature of
Antigens

Foreign nature

Molecular size

Molecular complexity and rigidity

Genetic factors

Route of administration and dose – although not
a “physical nature” important for response
Antigenic Determinants or
epitopes

Structures on antigens that are recognized as
foreign by the immune system.

An immune response is directed against specific
determinants and resultant antibodies will
specifically bind to them.

Multivalent antigens may elicit antibodies of
different specificities.

Antibodies produced in response to one antigen
may cross react with other antigens having a
common determinant.
Blood group antigens

Chemical structures embedded in or protruding
from RBCs, WBCs, and platelets and have three
common forms:

Glycoproteins - HLA system.

Glycolipids - ABH, Lewis, Ii, and P blood group
systems.

Proteins - Rh, M, N blood group systems.
Haptens

Substances, usually of low molecular weight, that
can combine with antibody but cannot initiate an
immune response unless it is coupled to a larger
carrier molecule.

Most important in drug-induced hemolysis
covered later in this course.
Cellular Immunity

Important defense mechanism against viral
infections, some fungal infections, parasitic
disease and against some bacteria, particularly
those inside cells.

Responsible for delayed hypersensitivity,
transplant rejection and possibly tumor
surveillance.

Review your Immunlogy notes from Fall for more
information.
The Humoral Immune
Response

Production of antibodies induced when the host's
immune system comes into contact with foreign
antigenic substance and reacts to this antigenic
stimulation.

Two types of responses:

Primary

Secondary
Humoral Immune
Response

Antibody production occurs in four phases
following antigen challenge:

Lag phase when no antibody is detectable.

Log phase in which antibody titer rises
logarithmically.

Plateau phase during which the antibody titer
remains steady.

Decline phase during which antibody levels
gradually decline.
Humoral Immune
Response

You must be able to differentiate a
primary vs secondary immune response
based on the following:






Time
Antibody Titer
Antibody Class
Antibody affinity and avidity
These are critical to understanding
reactions obtained in Blood Banking
The following chart nicely illustrates the
concepts.
Memorize!
Immunoglobulins

Humans produce specific proteins or
immunoglobulins which can be differentiated on
the basis of:

Size

Biologic function

biochemical properties

serological activity
Basic Structure of
Immunoglobulins

An antibody digested by papain yields two fragments
Fab contains antigen binding site.
 Fc is the region that determine biological properties of the Ig.

Immunoglobulin Structures
IgM Class
IgM






Largest of all the antibody molecules and the
structure consists of five of the basic units (pentamer)
joined together by a structure known as J-chain.
Accounts for about 5-10% of the immunoglobulin
pool.
restricted almost entirely to the intravascular space
due to its large size.
fixes complement and is much more efficient than
IgG in the activation of complement and
agglutination.
first antibody to be produced and is of greatest
importance in the first few days of a primary immune
response to an infecting organism. does not cross
the placenta.
Many blood group antibodies that are capable of
agglutinating antigen positive RBCs suspended in
saline in tests performed at 22 C are IgM causing
visible agglutination, ie, ABO antibodies.
IgG

Most abundant of the immunoglobulins in the plasma Consists of
one basic structural unit, i.e. Y-shaped molecule having 2 light
chains and 2 Gamma heavy chains.

Produced in response to a wide variety of antigens, including
bacteria, viruses and RBC and WBC allo-antigens.

Coats organisms to enhance phagocytosis by neutrophils and
macrophages.

Through its ability to cross the placenta, maternal IgG provides the
major line of defense against infection for the first few weeks of a
baby's life.

It is the predominant antibody produced in the secondary
response.

The serologic behavior and characteristics of IgG antibodies make
them one of the most clinically significant in blood banking.

Most blood group antigens capable of eliciting an immune
response result in the production of IgG antibodies.

These antibodies are detected by serologic test procedures based on
their behavior characteristics, such as reactivity at 37 C, complement
activation, indirect agglutination and hemolysis.

Much of routine blood banking involves serologic test procedures
designed to detect and identify IgG antibodies.
IgA

Found in saliva, tears, colostrum breast milk and in nasal, bronchial
and intestinal secretions. IgA is present in large quantities in
colostrum and breast milk and can be transferred across the gut
mucosa in the neonate and plays an important role in protecting
the neonate from infection.

Produced in high concentrations by lymphoid tissues lining the
gastrointestinal, respiratory and genitourinary tracts.

Plays an important role in protection against respiratory, urinary
tract and bowel infections and preventing absorption of potential
antigens in the food we eat.

Represents 10 to 15% of the total circulatory immunoglobulin pool.

In plasma IgA may exist as a single basic structural unit or as two or
three basic units joined together.

The IgA present in secretions exists as two basic units (a dimer)
attached to another molecule know as secretory component.

1) This substance is produced by the cells lining the mucous membranes.

2) It is thought to protect the IgA in secretions from destruction by
digestive enzymes.
IgA Structure

The dimeric IgA molecule.

1 H-chain,

2 L-chain,

3 J-chain,

4 secretory component
IgE






Trace plasma protein (only about 0.004%) in the
plasma of non-parasitized individuals.
Major importance because it mediates some types
of allergic reactions and is generally responsible for
an individual's immunity to invading parasites.
Fc region binds strongly to a receptor on mast cells
and basophils and, when antigen is bound it causes
the basophil (or mast cell) to release histamines and
heparin from these cells, resulting in allergic
symptoms.
Clinical effects of IgE mediated reactions include
increased vascular permeability, skin rashes,
respiratory tract constriction (wheezing), and
increased secretions from epithelium (watery eyes,
runny nose).
Not much else is known about its biologic role.
IgE does not fix complement and does not cross the
placenta.
IgE
IgD

Accounts for less than 1% of the total
immunoglobulin pool.

This is primarily a cell membrane
immunoglobulin found on the surface
of B lymphocytes.

IgD does not fix complement and
does not cross the placenta.

Little is known about the function of
this class of antibody.

No blood group antibodies have
Clinical Significance of Blood
Group Antibodies

Clinical significance of blood group antibodies is
evaluated by their ability to

produce hemolytic transfusion reactions
(destruction of transfused red cells) or

hemolytic disease of the newborn (HDN)
(destruction of fetal cells)
Transfusion Reaction

Term used to describe an unfavorable
response by a recipient to the infusion
of blood or blood products and
include the following:








In-vivo hemolysis,
Decreased survival of transfused cells,
anaphylaxis,
graft-versus-host disease,
post-transfusion purpura,
alloimmunization,
sepsis due to bacterial contaminated
components,
and disease transmission.
Severity

Depends on a number of factors,
including the characteristics of the
antibody class involved.
 Antibodies to the ABO system antigens
are usually IgM, cause complement
activation and intra vascular
hemolysis.
 Other RBC antigens induce formation
of IgG class antibodies which may
cause accelerated RBC destruction
extra vascularly.
 Symptoms may include fever, low
back pain, nausea and vomiting,
circulatory shock, anemia, jaundice,
and kidney failure which may
Antibody MediatedHemolysis

Hemolysis can be intravascular or extravascular.

Antibodies destroy the red cells IN THE CIRCULATION. Due
to antibody binding activating complement with
destruction of RBCs, VERY BAD, will see RED serum/plasma.

Extravascular hemolysis is due to RBCs being coated and
destroyed OUTSIDE the circulation in the RES system. If this
occurs slowly may not be detectable.
Complement

Spend quality time on your notes from Serology.
Complement

Three primary functions:

Lysis of antibody coated cells, such as bacteria and
RBCs.

Mediation of opsonization, preparation of foreign
cells for phagocytosis.

Generation of peptide fragments that regulate
features of the inflammatory and immune response.
Importance in Blood
Banking

Two major areas:

Some antigen-antibody complexes cause sufficient
quantities of complement to be bound to RBCs to
complete activation cycle, causing hemolysis.

Antigen-antibody complexes initiate complement
binding in such a way that allows demonstration of
the existence of such complexes by the use of
serologic techniques
The Classic Pathway

Eleven components involved, numbered C1 to
C9.

Complement cascade requires presence of
cations, both calcium and magnesium.

Activation of the classic pathway almost always
initiated by immunoglobulin.

Requires only 1 molecule of IgM.

Requires 2 molecules of IgG.
Two IgG, One IgM
The Classic Pathway

Recognition Phase - Recognition unit:
C1q,C1r,C1s.

Activation Phase -Activation Unit:
C4b,C2b,C3b,C5b

Attack Phase – Attack Unit:
C5b,C6,C7,C8 and C9

Classic pathway:
C1,C4,C2,C3,C5,C6,C7,C8,C9

Must go to completion for hemolysis to
occur. The next two slides are to assist
Classical Pathway
Alternative (Properdin)
Pathway

Proteins in the alternative pathway perform
activities similar to those in the classic pathway
but are usually non-antibody triggered.

Any one of a variety of substances can initiate
complement activation including:


bacterial polysaccharides and
lipopolysaccharides,

endotoxins,

cobra venom,

trypsin like enzymes,

and aggregates of IgA and IgG4 that do not
activate C1.
C1, C4 and C2 do not participate.
Alternative Pathway
Lectin Pathway

Activation begins when mannan-binding protein (MBP)
binds to the mannose groups of the microbial
carbohydrates.

Two more lectin pathway proteins called MASP1 and
MASP2 (equivalent to C1r and C1s of the classical
pathway) now bind to the MBP.

This forms an enzyme similar to C1 of the classical
complement pathway that is able to cleave C4 and C2 to
form C4bC2a, the C3 convertase capable of
enzymatically splitting hundreds of molecules of C3 into
C3a and C3b.

The beneficial results are the same as in the classical
complement pathway above:

trigger inflammation (C5a>C3a>c4a);

chemotactically attract phagocytes to the infection site
(C5a);

promote the attachment of antigens to phagocytes via
enhanced attachment or opsonization (C3b>C4b);

serves as a second signal for the activation of naive B-
Lectin Pathway - FYI

Overview of the lectin complement pathway. In humans, MBL
and ficolin that are lectins form complexes with MASPs (MASP1,MASP-2 and MASP-3) and sMAP. Note that MBL consists of
several sizes of oligomers and that the composition of MASPs
and sMAP of each MBL oligomer has not been fully
elucidated. Once the complexes bind to carbohydrates on
the surfaces of microbes, activated MASPs cleave C4, C2 and
C3.
Comparison of 3
Pathways
Regulation of
Complement
Activation of complement cascade results in complex
series of molecular event with potent biologic
consequences.
 Modulating mechanisms are necessary to regulate
complement activation and control production of
biologically active split products.
 First mechanism is spontaneous decay of activated
components.
 Second mechanism involves specific control proteins
that modulate the activity of certain complement
components at critical activation steps.



C1 inhibitor blocks activities of C1r and C1s.
Other factors inhibit activation of other complement
components.
A number of proteins act to control the membrane
attack unit.
 Bottom line, gotta turn it off!
