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ACQUIRED IMMUNITY

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Human defense system. Acquired immunity PROF. MOHAMED OSMAN GAD ELRAB. , KKUH .. – PowerPoint PPT presentation

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Title: ACQUIRED IMMUNITY

1
Human defense system.
Acquired immunity
PROF. MOHAMED OSMAN GAD ELRAB. , KKUH ..
2
Mediated by

1. T- lymphocyte
Programmed in the Thymus gland.
2. B- lymphocyte
Programmed in the bone marrow .

Central lymphoid tissues .
3
Features

1. RECOGNITION Microbial antigens are
recognized by specific T-cell or
B- cell
receptor .
2. SPECIFICITY Specific response
to
each microbe ( Humoral or
Cellular ).
3. MEMORY Immunological memory is the
most important consequence of
adaptive
immunity .

4
Events in central lymphoid tissues .
Diverse specificity of the
antigen receptor is aquired.

T- cell
receptor TCR. B - cell
receptor BCR .

( LYMPHOCYTE
REPERTOIRE).
5
Antigen specificity is determined by

1. Differentiation in the central
lymphoid tissues .
2. Gene rearrangement .
THIS ENSURES
1. Diversity of the lymphocyte
repertoire.(range of receptors )
2. Unique antigen receptors of
individual lymphocytes .
( each lymphocyte have I
different receptor .)

6
T-cell receptor diversity.
7
Recognition of self non-self .

A. Antigen receptors that react
weakly with self (MHC)
survive by positive selection
( 2 percent .)
B. Antigen receptors that react
strongly with self (MHC)
deleted by negative
selection.
(98 percent .)

8
This establish a mechanism that prevent
autoimmune disease .

Central immunological tolerance.
( no immune reactions against self.)

9
Activation of acquired immunity require

1. Breakdown of microbes into
peptides.
( ANTIGENS ).
2. Delivery of microbial
antigens ( in the form of
peptides )
to the surface of specialized
cells in
association with self MHC
molecules .
Antigen presenting cells.

10
MHC.
MHC.

Major histocompatibility
complex .
(Tissue antigens present in
chromosome 6 )
ENCODE THE HLA SYSTEM .
(human leukocyte
antigens. )
A POLYGENIC HIGHLY POLYMORPHIC
SYSTEM OF GENES.

11
MHC, short arm of chromosome 6.
MHC REGION . include HLA.
12
Antigen .
13
HLA system (human leukocyte antigens ).

Consist of 4 loci
HLA-A HLA-B HLA-C
HLA-D .
Each individual has 2 antigens
in
each locus
One haplotype from maternal origin
.
One haplotype from paternal
origin .

14
MHC haplotypes .
15
MHC CLASSES .

MHC CLASS 1
ENCODE HLA-A HLA-B HLA-C .
( Present in all nucleated
cells ).
MHC CLASS 11
ENCODE HLA-DP HLA-DQ HLA-DR .
(Present in antigen presenting
cells only ).

16
Distribution of MHC 1 MHC 11 in body cells.
17
MHC immune responses

MHC CLASS1
Important for
Target (infected - cell )
recognition .
MHC CLASS 11
Important for
Antigen recognition
presentation.

18
ANTIGEN PRESEANTING CELLS (APC).

1. Dendritic cells .
2. Macrophages .
3. B-lymphocytes .

19
ANTIGEN PRESENTING CELLS.

ACTIVATED BY
1. Receptors that signal
presence of microbes .
.
2. Cytokines.

20
DISTRIBUTION OF APC.

. 1. DENDRITIC CELLS
Take up particulate soluble
microbial
antigen form site of infection.
( handles
a wide variety of
pathogens. )

21
2. Macrophages

Phagocytic cells in the tissues but also
process
ingested pathogens actively ingest
microbes and particulate
antigens
entering lymph nodes through
afferent
lymphatic vessels .

22
3. B-lymphocytes

Process soluble antigens (microbial
toxins).
recirculate through the lymphoid tissues
and concentrate in the lymph.
follicles
in lymph nodes.

23
Functions of APC

1. On activation, express
co-stimulatory
molecules .
2. Degrade microbes into antigenic
peptides .
3. Load antigenic peptides in clefts
in
self-MHC molecules .
4. Transport peptide-MHC complex on
the surface of the
cell.

24
Antigen processing by APC

TWO PATHWAYS
1. ENDOGENOUS PATHWAY PROCESS
INTRACELLULAR MICROBES
- DEGRADATION IN CYTOSOLS.
- BIND PEPTIDE TO MHC 1.
- RECOGNIZED BY CYTOTOXIC CD8
T-CELLS.

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26
2 .EXOGENOUS PATHWAY

- DEGRADE MICROBES IN THE
VESICULAR SYSTEM .
(ENDOSOMES).
A. INTRAVESICULAR PATHOGENS.
- BIND PEPTIDE TO
MHC-11.
- RECOGNIZED BY CD4
T-CELLS.
B. EXTRACELLULAR PATHOGENS.
-BIND PEPTIDE TO
MHC-11.
-RECOGNIZED BY CD4
T-CELLS.

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Activated CD4 T- cells

2 Functional classes influenced by nature
of microbial antigen
A. TH 1 CELLS
Mediate cellular
immunity,
Destroy intracellular
pathogens .
B. TH 2 CELLS
Mediate humoral
immunity,
Destroy extra- cellular
pathogens.

29
EFFECTOR MECHANISMSOF ADAPTIVE
IMMUNITY.

Activation of T-cells ( TH1)
Cellular immunity ,
( Cell mediated )
Activation of B- cells (TH2TH1,helper,)
Humoral immunity
( Antibody - mediated ).
) microbes may induce both , but one is
predominant for control )

30
Primary and secondary immune responses

FIRST ENCOUNTER WITH A MICROBIAL
ANTIGEN GENERATES
A PRIMARY IMMUNE RESONSE
.
4 PHASES
1. LAG. 3-4 DAYS.
2. LOG. 4-7 DAYS.
3. PLATEU. 7-10
DAYS.
4. DECLINE.
(Primary I.R. may take few days to
several weeks ,)

31
Features of primary immuneresponses

1. Takes longer ( 4 phases)
2. IgM predominate .
3. Memory cells generated .

32
Features of secondary immune responses

1. Fast response ( memory cells )
2. IgG predominate .
3. High concentration of antibody or
cells.

33
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34
Factors influencing immune responses

1. Nature of microbial antigen (Epitope)
T- dependant (TD).
T- independent (TI).
protein , CHO., Iipopolysaccarhide,
lipid.
2. Dose of antigen.
- high , optimum , low .
Immunological paralysis.

35
FACTORS cont.

3.Route of entry
A. Blood-borne antigens spleen .
B. Skin tissues draining lymph
nodes.
C. Mucosal surfaces - MALT.
D. Intranasal inhaled - palatine
tonsils
adenoids.
E. Ingested micro fold (M-cells),
Peyers
patches.

36
LYMPHOCYTE TRAFFIC.

Naïve T-cells enter the lymphoid
tissues through the
HIGH ENDOTHELIAL VENULES.
( HEV.)
Contact thousands of ( APC.), then
pass out into the blood
recirculate
into other lymphoid organs .

37
ANTIGEN RECOGNITION.

One naïve T- cell ( in thousands ) is
likely to be ( specific for a
particular antigen ) and will be
trapped in the
the L.node .
LYMPHOCYTE TRAPPING.

38
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39
SURVIVAL SIGNAL .

T- cells that do not encounter
antigen
Receive survival signal from
self - MHC .
Pass through efferent lymphatic into
the blood to continue recirculating
through other lymphoid organs
.

40
Cell-mediated immunity

1. Naive T-cells encounter specific
antigen.
( on dendritic cell (APC) in peripheral
lymphoid tissue. ).
2. APC express co- stimulatory signal.
Necessary for synthesis and
secretion of IL-2 by
T-cells.

41
T-cell proliferation .

T- cells divide 2 - 3 times /
day.
one cell give rise to a
clone
of thousands of progeny
that all bear the same
receptor
for antigen .

42
T-cell differentiation.

IL-2 promote proliferation
differentiation of T-cells into
EFFECTOR CELLS.
(mediate cellular responses)
( cell - mediated immunity )
Some T-cells remain as
MEMORY CELLS.

43
THERAPEUTIC NOTE.

The immunosuppressive drugs
Cyclosporine A
FK 506 (Tacrolimus )
Rapamycin .
Inhibit IL-2 production.
(Prevent clonal expansion of T-cells )
Inhibit immune responses.

44
EFFECTOR T-CELLS EXERTDIFFERENT
FUNCTIONS

Adhesion molecules (P- selectin

E- selectin) recruit
T-cells into sites of
infection .
1. Some differentiate into cytotoxic
T-cells .
( CTL )
2. Some produce cytokines that act
on
A - CD8 cytotoxic
T-cells .
B - Macrophages .
C - NK-cells .