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Seminar on
Transplantation Immunology: Organ and
Tissue Transplantation
Immunosuppressive Agents,
Immunosuppressive Therapy.
By
Mr.Pratap J. Patle
Deptt. Of Zoology
R.T.M. Nagpur University, Nagpur
Contents
 Introduction
 Immunology of Transplant Rejection
 Tissue and Organ Transplantation
 Immunosuppressive Agents
 Immunosuppressive Therapy
 Conclusion
 References
Introduction
 Transplantation immunology - sequence of events that
occurs after an allograft or xenograft is removed from
donor and then transplanted into a recipient.
 A major limitation to the success of transplantation is
the immune response of the recipient to the donor
tissue.
Types of Transplant
Autograft is self-tissue transferred from one body site to
another in the same individual.
Isograft is tissue transferred between genetically identical
individuals.
Allograft is tissue transferred between genetically different
members of the same species.
Xenograft is tissue transferred between different species
Immunology of Transplant
Rejection
Components of the Immune system involved in graft Rejection :
1) Antigen presenting cells –
 Dendritic cells
 Macrophages
 Activated B Cells
2) B cells and antibodies –
 Preformed antibodies
 Natural antibodies
 Preformed antibodies from prior sensatization
 Induced antibodies
3) T cells
4) Other cells –
 Natural killer cells
 T cells that express NK cell – associated Markers
 Monocytes/Macrophages
The Immunology of Allogeneic
Transplantation
 Recognition of transplanted cells that are self or
foreign is determined by polymorphic genes
(MHC) that are inherited from both parents and
are expressed co-dominantly.
 Alloantigens elicit both cell-mediated and
humoral immune responses.
Recognition of Alloantigens
 Direct Presentation
 Recognition of an intact MHC molecule displayed by donor APC in the
graft
 Basically, self MHC molecule recognizes the structure of an intact
allogeneic MHC molecule
 Involves both CD8+ and CD4+ T cells.
 Indirect Presentation
 Donor MHC is processed and presented by recipient APC
 Basically, donor MHC molecule is handled like any other foreign
antigen
 Involve only CD4+ T cells.
 Antigen presentation by class II MHC molecules.
Activation of Alloreactive T cells and
Rejection of Allografts
 Donor APCs migrate to regional lymph nodes
and are recognized by the recipient’s TH cells.
 Alloreactive TH cells in the recipient induce
generation of TDTH cell and CTLs then migrate
into the graft and cause graft rejection.
Activation of Alloreactive T cells and
Rejection of Allografts
( )
SENSATIZATION
Passenger leukocyte
.
Class II MHC
antigen
2
IL 
H
T H
T
H
T
H
T
Donar kidney
CTL DTH
T
CTL
DTH
T
LYMPH NODE
EFFECTOR
Role of CD4+ and CD8+ T Cells
 CD4+ differentiate into cytokine producing
effector cells
 Damage graft by reactions similar to DTH
 CD8+ cells activated by direct pathway kill
nucleated cells in the graft
 CD8+ cells activated by the indirect pathway are
self MHC-restricted
Role of Cytokines in Graft
Rejection
 IL – 2, IFN – , and TNF -  are important mediators of graft
rejection.
 IL – α promotes T-cell proliferation and generation of T –
Lymphocytes.
 IFN -  is central to the development of DTH response.
 TNF -  has direct cytotoxic effect on the cells of graft.
 A number of cytokines promote graft rejection by inducing
expression of class – I or class – II MHC molecule on graft cell.
 The interferon (α,  and ), TNF – α and TNF -  all increases
class – I MHC expression, and IFN -  increases class – II MHC
expression as well.
Effector Mechanisms of Allograft
Rejection
 Hyperacute Rejection
 Acute Rejection
 Chronic Rejection
Hyperacute Rejection
 Characterized by thrombotic occlusion of the
graft
 Begins within minutes or hours after
anastamosis
 Pre-existing antibodies in the host circulation
bind to donor endothelial antigens
 Activates Complement Cascade
 Xenograft Response
Hyperacute Rejection
1. Preformed Ab, 2. complement activation,
3. neutrophil margination, 4. inflammation,
5. Thrombosis formation
Acute Rejection
 Vascular and parenchymal injury mediated by T
cells and antibodies that usually begin after the
first week of transplantation if there is no
immunosuppressant therapy
 Incidence is high (30%) for the first 90 days
Acute Rejection
1. T-cell, macrophage and Ab mediated,
2. myocyte and endothelial damage,
3. Inflammation
Chronic Rejection
 Occurs in most solid organ transplants
 Heart
 Kidney
 Lung
 Liver
 Characterized by fibrosis and vascular
abnormalities with loss of graft function over a
prolonged period.
Chronic Rejection
1. Macrophage – T cell mediated
2. Concentric medial hyperplasia
3. Chronic DTH reaction
Tissue and Organ
Transplantation
 Today it is possible to transplant many different organs
and tissues including.
 Most common transplantation is blood transfusion.
 Bone Marrow transplantation
 Organs : Heart, kidneys, pancrease, lungs, liver and
intestines.
 Tissues : include bones, corneas, skin, heart values,
veins, cartilage and other connective tissues.
Most Common Transplantation
-Blood Transfusion-
Transfuse Not transfused
Bone Marrow Transplantation
 Used for Leukemia, Anemia and immunodeficiency, especially
severe combined immunodeficiency (SCID).
 About 109 cells per kilogram of host body weight, is injected
intravenously into the recipients.
 Recipient of a bone marrow transplant is immunologically
suppressed before grafting.
 Eg. Leukemia patients are often treated with cyclo-phosphamide
and total body irradiation to kill all cancerous cells.
 Because the donor bone marrow contains immunocompetent
cells, the graft may reject the host, causing graft versus host
disease (GVHD).
Graft vs. Host Disease
 Caused by the reaction of grafted mature T-cells
in the marrow inoculum with alloantigens of the
host
 Acute GVHD
 Characterized by epithelial cell death in the skin, GI
tract, and liver
 Chronic GVHD
 Characterized by atrophy and fibrosis of one or
more of these same target organs as well as the lungs
Heart Transplantation :
 First heart transplant in South Africa by Dr. Christian Barnard in 1964.
 One year survival rate is >80%.
 HLA matching is desirable but not often possible, because of the limited
supply of heart and the urgency of the procedure.
Lung Transplantation :
 First attempt in 1963 by Hardy and Co - workers.
 First successful transplantation by Toronto group in 1983.
 In conjunction with heart transplantation, to treat diseases such as cystic
fibrosis and emphysema or acute damage to lungs.
 First year survival rate is about 60%.
Kidney Transplantation :
 Diseases like diabetes and various type of nephritis can be
elleviated by kidney transplantation.
 Survival rate after one year transplantation is >90%.
 25,000 candidates are waiting for kidney transplantation.
Liver transplantation :
 It treat congenital defects and damage from viral (hepatitis)
or chemical agents. (Chronic alcoholism).
 Liver one year survival exceeds 75% and five year is 70%.
Pancrease Transplantation :
 Offers a cure for diabetes mellitus.
 Graft survival is 72% at one year.
 Further improved if a kidney is transplanted simultaneously.
 Overall goal - to prevent the typical diabetic secondary
complications.
Skin grafting :
 It is used to treat burn victims.
 In severe burn, grafts of foreign skin may be used and rejection
must be prevented by the use of immunosuppressive therapy.
Xenogeneic Transplantation
 A major barrier to xenogeneic transplantation is
the presence of natural antibodies that cause
hyperacute rejection.
Immunosuppressive Agents
Immunosuppression can be brought about by 3
different ways :-
 Surgical ablation
 Total Lymphoid Irradiation
 Immunosuppressive drugs
Immunosuppressive Drugs
Three main immunosuppressant drugs
 Cyclosporins act by inhibiting T-cell activation, thus
preventing T-cells from attacking the transplanted organ.
 Azathioprines disrupt the synthesis of DNA and RNA and
cell division.
 Corticosteroids such as prednisolone suppress the
inflammation associated with transplant rejection.
Immunosuppressants can also be classified depending on the
specific transplant:
 Basiliximab in combination with cyclosporin and
corticosteroids, in kidney transplants.
 Daclizumab in combination with cyclosporin and
corticosteroids, in kidney transplants.
 muromonab CD3 (Orthoclone OKT3) along with
cyclosporin, in kidney, liver and heart transplants.
 Tacrolimus is used in liver transplants and is under study for
kidney, bone marrow, heart, pancreas, pancreatic island cell,
and small bowel transplantation.
Some immunosuppressants are also used to treat a variety of
autoimmune diseases:
 Azathioprine in treatment of rheumatoid arthritis , chronic ulcerative
colitis but limited value.
 Cyclosporin is used in heart, liver, kidney, pancreas, bone marrow and
heart/lung transplantation. Also used to treat psoriasis and rheumatoid
arthritis, multiple sclerosis, diabetes and myesthenia gravis.
 Glatiramer acetate is used in treatment of relapsing-remitting multiple
sclerosis.
 Mycophenolate is used along with cyclosporin in kidney, liver and heart
transplants. Also used to prevent the kidney problems associated with
lupus erythematosus.
 Sirolimus in combination with cyclosporin and corticosteroids, in kidney
transplants. The drug is also used for the treatment of psoriasis.
Immunosuppressive Therapy
Monoclonal antibodies
 To suppress the activity of subpopulation of T-cells.
 To block co-stimulatory signals.
 Ab to the CD3 molecule of TCR (T cell receptor) complex results in a rapid
depletion of mature T-cells from the circulation.
 Ab specific for the high-affinity IL-2 receptor is expressed only on activated
T-cell, blocks proliferation of T-cells activated in response to the alloantigens
of the graft.
 To treat donor’s bone marrow before it is transplanted.
 Molecules present on particular T-cells subpopulation may also be targeted
for immunosuppressive therapy.
 Antibody to CD4 shown to prolong graft survival.
 Ab specific for implicated cytokine can prolong the survival of graft.
Conclusion
 More than 50,000 people, waiting for compatible donor. For
ethical an practical reasons, species closely related to human such
as Chimpanzee have not been widely used.
 Xenogeneic transplantation may be major issue of research
xenograft technology including genetically modified animal may
become a new source of organ supply.
 Side effects of immunosuppressive agent use for graft need a
change of specificity in action and avoiding general immune
suppression.
 Techniques such as transgenic animal production and wide range
of research in this field hope to result in opening a new window
for the process of transplantation immunology.
References
•Immunology by – Janis Kuby
•Immunology by – Abdul Abbas
•Immunology by – Roitt
•Fundamental Immunology by – William E. Paul
Information from –
•www.organtransplants.org
•www.transweb.org
•www.organdonor.web
Thank you !
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Seminar on Transplantation Immunology and Immunosuppressive Therapy

  • 1. Seminar on Transplantation Immunology: Organ and Tissue Transplantation Immunosuppressive Agents, Immunosuppressive Therapy. By Mr.Pratap J. Patle Deptt. Of Zoology R.T.M. Nagpur University, Nagpur
  • 2. Contents  Introduction  Immunology of Transplant Rejection  Tissue and Organ Transplantation  Immunosuppressive Agents  Immunosuppressive Therapy  Conclusion  References
  • 3. Introduction  Transplantation immunology - sequence of events that occurs after an allograft or xenograft is removed from donor and then transplanted into a recipient.  A major limitation to the success of transplantation is the immune response of the recipient to the donor tissue.
  • 4. Types of Transplant Autograft is self-tissue transferred from one body site to another in the same individual. Isograft is tissue transferred between genetically identical individuals. Allograft is tissue transferred between genetically different members of the same species. Xenograft is tissue transferred between different species
  • 5. Immunology of Transplant Rejection Components of the Immune system involved in graft Rejection : 1) Antigen presenting cells –  Dendritic cells  Macrophages  Activated B Cells 2) B cells and antibodies –  Preformed antibodies  Natural antibodies  Preformed antibodies from prior sensatization  Induced antibodies 3) T cells 4) Other cells –  Natural killer cells  T cells that express NK cell – associated Markers  Monocytes/Macrophages
  • 6. The Immunology of Allogeneic Transplantation  Recognition of transplanted cells that are self or foreign is determined by polymorphic genes (MHC) that are inherited from both parents and are expressed co-dominantly.  Alloantigens elicit both cell-mediated and humoral immune responses.
  • 7. Recognition of Alloantigens  Direct Presentation  Recognition of an intact MHC molecule displayed by donor APC in the graft  Basically, self MHC molecule recognizes the structure of an intact allogeneic MHC molecule  Involves both CD8+ and CD4+ T cells.
  • 8.  Indirect Presentation  Donor MHC is processed and presented by recipient APC  Basically, donor MHC molecule is handled like any other foreign antigen  Involve only CD4+ T cells.  Antigen presentation by class II MHC molecules.
  • 9. Activation of Alloreactive T cells and Rejection of Allografts  Donor APCs migrate to regional lymph nodes and are recognized by the recipient’s TH cells.  Alloreactive TH cells in the recipient induce generation of TDTH cell and CTLs then migrate into the graft and cause graft rejection.
  • 10. Activation of Alloreactive T cells and Rejection of Allografts ( ) SENSATIZATION Passenger leukocyte . Class II MHC antigen 2 IL  H T H T H T H T Donar kidney CTL DTH T CTL DTH T LYMPH NODE EFFECTOR
  • 11. Role of CD4+ and CD8+ T Cells  CD4+ differentiate into cytokine producing effector cells  Damage graft by reactions similar to DTH  CD8+ cells activated by direct pathway kill nucleated cells in the graft  CD8+ cells activated by the indirect pathway are self MHC-restricted
  • 12. Role of Cytokines in Graft Rejection  IL – 2, IFN – , and TNF -  are important mediators of graft rejection.  IL – α promotes T-cell proliferation and generation of T – Lymphocytes.  IFN -  is central to the development of DTH response.  TNF -  has direct cytotoxic effect on the cells of graft.  A number of cytokines promote graft rejection by inducing expression of class – I or class – II MHC molecule on graft cell.  The interferon (α,  and ), TNF – α and TNF -  all increases class – I MHC expression, and IFN -  increases class – II MHC expression as well.
  • 13. Effector Mechanisms of Allograft Rejection  Hyperacute Rejection  Acute Rejection  Chronic Rejection
  • 14. Hyperacute Rejection  Characterized by thrombotic occlusion of the graft  Begins within minutes or hours after anastamosis  Pre-existing antibodies in the host circulation bind to donor endothelial antigens  Activates Complement Cascade  Xenograft Response
  • 15. Hyperacute Rejection 1. Preformed Ab, 2. complement activation, 3. neutrophil margination, 4. inflammation, 5. Thrombosis formation
  • 16. Acute Rejection  Vascular and parenchymal injury mediated by T cells and antibodies that usually begin after the first week of transplantation if there is no immunosuppressant therapy  Incidence is high (30%) for the first 90 days
  • 17. Acute Rejection 1. T-cell, macrophage and Ab mediated, 2. myocyte and endothelial damage, 3. Inflammation
  • 18. Chronic Rejection  Occurs in most solid organ transplants  Heart  Kidney  Lung  Liver  Characterized by fibrosis and vascular abnormalities with loss of graft function over a prolonged period.
  • 19. Chronic Rejection 1. Macrophage – T cell mediated 2. Concentric medial hyperplasia 3. Chronic DTH reaction
  • 20. Tissue and Organ Transplantation  Today it is possible to transplant many different organs and tissues including.  Most common transplantation is blood transfusion.  Bone Marrow transplantation  Organs : Heart, kidneys, pancrease, lungs, liver and intestines.  Tissues : include bones, corneas, skin, heart values, veins, cartilage and other connective tissues.
  • 21. Most Common Transplantation -Blood Transfusion- Transfuse Not transfused
  • 22. Bone Marrow Transplantation  Used for Leukemia, Anemia and immunodeficiency, especially severe combined immunodeficiency (SCID).  About 109 cells per kilogram of host body weight, is injected intravenously into the recipients.  Recipient of a bone marrow transplant is immunologically suppressed before grafting.  Eg. Leukemia patients are often treated with cyclo-phosphamide and total body irradiation to kill all cancerous cells.  Because the donor bone marrow contains immunocompetent cells, the graft may reject the host, causing graft versus host disease (GVHD).
  • 23. Graft vs. Host Disease  Caused by the reaction of grafted mature T-cells in the marrow inoculum with alloantigens of the host  Acute GVHD  Characterized by epithelial cell death in the skin, GI tract, and liver  Chronic GVHD  Characterized by atrophy and fibrosis of one or more of these same target organs as well as the lungs
  • 24. Heart Transplantation :  First heart transplant in South Africa by Dr. Christian Barnard in 1964.  One year survival rate is >80%.  HLA matching is desirable but not often possible, because of the limited supply of heart and the urgency of the procedure. Lung Transplantation :  First attempt in 1963 by Hardy and Co - workers.  First successful transplantation by Toronto group in 1983.  In conjunction with heart transplantation, to treat diseases such as cystic fibrosis and emphysema or acute damage to lungs.  First year survival rate is about 60%.
  • 25. Kidney Transplantation :  Diseases like diabetes and various type of nephritis can be elleviated by kidney transplantation.  Survival rate after one year transplantation is >90%.  25,000 candidates are waiting for kidney transplantation. Liver transplantation :  It treat congenital defects and damage from viral (hepatitis) or chemical agents. (Chronic alcoholism).  Liver one year survival exceeds 75% and five year is 70%.
  • 26. Pancrease Transplantation :  Offers a cure for diabetes mellitus.  Graft survival is 72% at one year.  Further improved if a kidney is transplanted simultaneously.  Overall goal - to prevent the typical diabetic secondary complications. Skin grafting :  It is used to treat burn victims.  In severe burn, grafts of foreign skin may be used and rejection must be prevented by the use of immunosuppressive therapy.
  • 27. Xenogeneic Transplantation  A major barrier to xenogeneic transplantation is the presence of natural antibodies that cause hyperacute rejection.
  • 28. Immunosuppressive Agents Immunosuppression can be brought about by 3 different ways :-  Surgical ablation  Total Lymphoid Irradiation  Immunosuppressive drugs
  • 29. Immunosuppressive Drugs Three main immunosuppressant drugs  Cyclosporins act by inhibiting T-cell activation, thus preventing T-cells from attacking the transplanted organ.  Azathioprines disrupt the synthesis of DNA and RNA and cell division.  Corticosteroids such as prednisolone suppress the inflammation associated with transplant rejection.
  • 30. Immunosuppressants can also be classified depending on the specific transplant:  Basiliximab in combination with cyclosporin and corticosteroids, in kidney transplants.  Daclizumab in combination with cyclosporin and corticosteroids, in kidney transplants.  muromonab CD3 (Orthoclone OKT3) along with cyclosporin, in kidney, liver and heart transplants.  Tacrolimus is used in liver transplants and is under study for kidney, bone marrow, heart, pancreas, pancreatic island cell, and small bowel transplantation.
  • 31. Some immunosuppressants are also used to treat a variety of autoimmune diseases:  Azathioprine in treatment of rheumatoid arthritis , chronic ulcerative colitis but limited value.  Cyclosporin is used in heart, liver, kidney, pancreas, bone marrow and heart/lung transplantation. Also used to treat psoriasis and rheumatoid arthritis, multiple sclerosis, diabetes and myesthenia gravis.  Glatiramer acetate is used in treatment of relapsing-remitting multiple sclerosis.  Mycophenolate is used along with cyclosporin in kidney, liver and heart transplants. Also used to prevent the kidney problems associated with lupus erythematosus.  Sirolimus in combination with cyclosporin and corticosteroids, in kidney transplants. The drug is also used for the treatment of psoriasis.
  • 32. Immunosuppressive Therapy Monoclonal antibodies  To suppress the activity of subpopulation of T-cells.  To block co-stimulatory signals.  Ab to the CD3 molecule of TCR (T cell receptor) complex results in a rapid depletion of mature T-cells from the circulation.  Ab specific for the high-affinity IL-2 receptor is expressed only on activated T-cell, blocks proliferation of T-cells activated in response to the alloantigens of the graft.  To treat donor’s bone marrow before it is transplanted.  Molecules present on particular T-cells subpopulation may also be targeted for immunosuppressive therapy.  Antibody to CD4 shown to prolong graft survival.  Ab specific for implicated cytokine can prolong the survival of graft.
  • 33. Conclusion  More than 50,000 people, waiting for compatible donor. For ethical an practical reasons, species closely related to human such as Chimpanzee have not been widely used.  Xenogeneic transplantation may be major issue of research xenograft technology including genetically modified animal may become a new source of organ supply.  Side effects of immunosuppressive agent use for graft need a change of specificity in action and avoiding general immune suppression.  Techniques such as transgenic animal production and wide range of research in this field hope to result in opening a new window for the process of transplantation immunology.
  • 34. References •Immunology by – Janis Kuby •Immunology by – Abdul Abbas •Immunology by – Roitt •Fundamental Immunology by – William E. Paul Information from – •www.organtransplants.org •www.transweb.org •www.organdonor.web
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