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Major Histocompatibility Complex and Transplantation

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Title: Major Histocompatibility Complex and Transplantation


1
Major Histocompatibility Complex and
Transplantation
  • Major histocompatibility complex (MHC) proteins
    were discovered for the first time with the
    advent of tissue transplantation
  • The success of tissue and organ transplantation
    depends upon the donors and recipients human
    leukocyte antigens (HLA) encoded by HLA genes
  • These proteins are allo-antigens

2
Major Histocompatibility Complex and
Transplantation
  • Genes for HLA proteins are clustered in the MHC
    complex located on the short arm of chromosome 6
  • Three genes HLA-A, HLA-B and HLA-C code for Class
    I MHC proteins
  • HLA-D loci encode for Class II MHC proteins ie,
    DP, DQ and DR

3
Major Histocompatibility Complex and
Transplantation
  • Each individual has two haplotypes ie, two sets
    of these genes one paternal and one maternal
  • These genes are very diverse polymorphic
  • 47 HLA-A
  • 88 HLA-B
  • 29 HLA-C
  • More than 300 HLA-D

4
Major Histocompatibility Complex and
Transplantation
  • Minor HLA genes unknown
  • They mount a weak immune response
  • Play role in chronic rejection of a graft
  • There are no laboratory tests to detect minor
    antigens
  • Class III MHC locus between MHC I II
  • Encode for TNF, lymphotoxin, C2 and C4

5
MHC Class I, II III Genes
6
MHC Class I Proteins
  • These are glycoproteins found on surface of
    virtually all the nucleated cells
  • There are 20 different proteins for A locus 40 at
    B locus and 8 at C locus
  • Complete class I protein is composed of a heavy
    chain bound to a ?2-microglobulin molecule
  • The heavy chain is highly polymorphic and has a
    hypervariable region at N-terminal
  • Polymorphism self and non-self recognition
  • Constant regions react with CD8 protein of Tc

7
MHC Class I Protein
8
Class II MHC Proteins
  • These glycoproteins are normally found on the
    surface of antigen presenting cells such as
    marophages, B cells, dendritic cells of spleen
    and Langerhans cells of skin
  • They are highly polymorphic
  • Composed of two polypeptide chains bound
    non-covalently
  • They have hypervariable regions
  • Polymorphism

9
MHC Class II Protein
10
Major Histocompatibility Complex and
Transplantation
  • Both chains of Class II MHC proteins are encoded
    by the MHC locus
  • Constant regions of both the peptides interact
    with CD4 proteins of helper T cells

11
Biologic Importance of MHC
  • Tc kills virus infected cells in association with
    class I MHC proteins
  • Helper T cell recognize antigen in association
    with class II MHC proteins
  • This is called MHC restriction
  • Success of organ transplant is determined by
    compatibility of the MHC genes

12
Transplantation antigens
13
Transplantation
  • Types of transplants
  • Autografts, Autologous grafts
  • Donor and recipient are same individual
  • Common in skin grafting bone marrow
  • Syngeneic grafts or (isograft)
  • Donor and recipient are genetically identical
  • Animal models identical twins

14
Transplantation
  • Types of transplants
  • Allogeneic grafts
  • Donor and recipient are same species, but
    genetically unrelated
  • Common heart, lung, kidney, liver graft
  • Xenogeneic grafts
  • Donor and recipient are different species
  • Artificial grafts

15
Transplantation
  • Major Barrier to transplantation is the immune
    response
  • T cells play primary role
  • B cells can/do play a role
  • Classic adaptive/acquired immune response
  • Memory
  • Specificity

16
1st set versus 2nd set reactions
17
1st set versus 2nd set reactions
Role of cell mediated responses
Unprimed syngeneic recipient
18
Role of CD4 versus CD8 T cells
Injecting recip. mice with mab to deplete one or
both types of T cell
19
Transplantation
  • T cells play primary role in 1st and 2nd set
    rejection reactions
  • Nude mice accept allografts
  • B cell deficient mice reject allografts

Nude mouse has a transplant of rabbit skin
20
Mechanisms involved in Graft Rejection
Sensitization stage Effector stage
21
Rejection Response
22
Clinical manifestations of graft rejection
  1. Hyperacute rejection very quick
  2. Acute rejection about 10 days (cell mediated)
  3. Chronic rejection months-years (both)

23
Chronic Rejection
  • This occurs months to years after engraftment
  • Main pathologic finding in chronic rejection is
    atherosclerosis of the vascular endothelium
  • Main cause of chronic rejection is not known
  • Minor histocompatibility antigen miss match
  • Side effects of immunosuppressive drugs

24
Graft-versus-Host (GVH) Reaction
  • Occurs in about two thirds of bone marrow
    transplants
  • Occurs because grafted immunocompetent T cells
    proliferate in the irradiated immunocompromised
    host and reject cells with foreign proteins
    resulting in sever organ dysfunction
  • Donors Tc cells play a major role in destroying
    the recipients cells
  • Symptoms are maculopapular rash, jaundice,
    hepatosplenomegaly and diarrhea
  • GVH reactions usually end in infections and death

25
HLA Typing in the Laboratory
  • Prior to transplantation laboratory test commonly
    called as HLA typing or tissue typing to
    determine the closest MHC match between the donor
    and recipient is performed
  • Methods
  • DNA sequencing by Polymerase Chain Reaction (PCR)
  • Serologic Assays
  • Mixed Lymphocyte Reaction (MLR)
  • Crossmatching (D) lys (R) serum complement

26
Tissue Matching
Effect of HLA class I II matching on survival
of kidney grafts
27
Tissue Matching
Serological Method
28
Tissue Matching
Mixed Leukocyte Reaction (MLR)
29
Tissue Matching
30
General Immunosuppression Therapy
  1. Mitotic inhibitor azathioprine (pre post)
  2. Corticosteroids ( 1)
  3. Cyclosporin A, FK506 IL-2 and IL-2R
  4. Total lymphoid irradiation

31
Immunosuppresive Therapy
32
Immunosuppresive Therapy
Cyclosporin FK506
33
Immunosuppresive Therapy
34
Specific Immunosuppression Therapy
  1. Mabs to T cell components or cytokines
  2. Agents that blocking co-stimulatory signal

35
Immunosuppresive Therapy
  • Downsides
  • Must be maintained for life
  • Toxicity
  • Susceptibility to infections
  • Susceptibility to tumors
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