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Antigen Processing and Presentation

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Title: Antigen Processing and Presentation

1
Antigen Processing and Presentation

2
Important Concepts

Antigen processing
Events leading to the degradation of antigen into
peptides that form the peptide-MHC complex
Antigen presentation
Degraded peptides associate with MHC
intracellularly
Peptide- MHC display on an APC
Peptide-MHC complex is transported to the
membrane for display
MHC molecules and binding of peptides
Class I and binding of peptides derived from
endogenous antigens
Class II and binding of peptides derived from
exogenous antigen

Rosenthal and Shevach
Demonstration of self-MHC restriction use of
inbred and congenic strains
T helper cells respond only to macrophages of the
same MHC haplotype (same Class II alleles)
Antigen recognition by CD4 T helper cells is
class II restricted

Zinkernagel and Doherty
Demonstration of self-MHC restriction in CD8 T
cells
Immunization of mice with lymphocytic
choriomeningitis (LCM) virus
Activated T cytotoxic cells (CTLs) attacked only
syngeneic virus-infected cells
Congenic mice studies Antigen recognition by
CD8 T cells is class I MHC restricted

Evidence for the Role of Antigen Presenting Cells
(APCs)
Early dogma antigen recognition by B and T cells
is the same (recognition of the entire native
antigen)
Contradicting dogma
experiments by Gell and Benacerraf demonstrating
T cell recognition of denatured protein
Additional data from Ziegler and Unanue
Shimonkevitz Townsend et al.

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Target cells
cells that display peptides associated with class
I MHC to CD8 T cells
Antigen Presenting Cells
Cells that display peptides associated with class
II MHC to CD4 T cells
Differ in antigen uptake, expression of class II
MHC and co-stimulatory activity
Dendritic cells
Macrophages
B Cells
Non professional APCs induced to express class
II MHC molecules or co-stimulatory proteins

Elimination of intracellular and extracellular
antigens
Cytosolic pathway processing pathway for
endogenous antigens
Endogenous antigen is degraded within the cytosol
by proteasomes and assembled with class I MHC in
RER
Endocytic pathway processing pathway for
exogenous antigens taken up by endocytosis
Exogenous antigen are internalized and degraded
within acidic endocytic compartments and are
bound by class II MHC

Cytostolic proteolytic system
pathway used in normal turnover of intracellular
proteins
Ubiquitin-protein complex is degraded by
proteasome
Large, cylindrical particle of 4 rings of protein
subunits
Subunits are encoded by 2 MHC gene clusters and
1 non-MHC gene that are induced by T cell
cytokine (INF-?)
Degradation reaction
Requires ATP
Occurs within the central channel of the
proteasome
Generates a variety of peptides

Peptides generated by proteasome plus LMP2, LMP7,
LMP10 are 8-10 aa long
TAP has high affinity for proteins 8-10 aa long
and hydrophobic or basic carboxyl-terminal aa
(preferred anchor residues)
In RER class I ? chain associates with peptide
with the help of molecular chaperones
Calnexin
Calreticulin
Tapasin

Molecular Chaperones and peptide-class I MHC
assembly
class I MHC ? chain associates with calnexin
until ?2 microglobulin binds
class I MHC ? chain/ ?2 microglobulin
heterodimer bind to calreticulin and the
TAP-associated protein tapasin
Chaperones help fold the class I MHC protein for
proper antigen binding and export from RER

TAP1 and TAP2 genes map within class II MHC
region adjacent to LMP2 and LMP7 genes
TAP1 and TAP2 genes are polymorphic
Differences in allelic forms of TAP may
contribute to variation in the response to
antigen between individuals
TAP deficiencies lead to diseases and
autoimmunity, ex. bare lymphocyte syndrome,
TAP-deficiency syndrome

Exogenous Pathway
Antigen is internalized by phagocytosis,
endocytosis or both
Internalized peptides are degraded into peptides
within endocytic compartments and presented on
class II MHC
Process takes 1-3 hours
Involves early (pH 6.0-6.5), late endosomes
(endolysosomes, pH 5.0-6.0) and lysosomes (pH
4.5-5.0)
Antigens are degraded by lytic enzymes into 13-18
amino acids
Involves 6 major steps

Invariant chain restricts class II
peptide-binding and guides transport of class II
MHC to endosomes
Class II bind invariant chain in RER
blocks binding to endogenous antigen or premature
binding to exogenous antigen
Sorting signals in its cytoplasmic tail direct
the transport of class II MHC from trans-golgi
network to endocytic compartments
Peptide assembly with class II MHC
Invariant chain is degraded while moving through
endocytic compartments, digestion leaves CLIP

Generation of antigenic peptides in endocytic
processing pathway
Internalized exogenous antigen moves through
early endosome, late endosome, and lysosomes by
mechanisms not clearly understood
Antigen is digested into peptides
Associates with class II MHC transported in
vesicles to late endosomes

CLIP (class II-associated invariant chain
peptide) remains in the binding groove of class
II MHC molecule
HLA-DM dissociates CLIP from class II MHC in
endosomal compartment to allow antigen binding
Non-classical HLA-DO may act as a negative
regulator of class II antigen by binding to
HLA-DM
Expressed only in B cells and in cells of the
thymus expression is not induced by IFN-?

Presentation of bacterial nonpeptide antigens
(lipids and glycolipids)
Presented by CD1 family proteins associated with
?2-microglobulin
5 genes encode human CD1 proteins
Genes are located on Chromosome 1 not within MHC
Expression of specific genes varies within cell
types
CD1D1 genes are expressed on nonprofessional
APCs and certain subsets of B cells
CD1A, B ,and C are expressed on professional
APCs and immature thymocytes