Abstract

This Program Project grant is entitled """"""""Pathophysiology and Immunotherapy of NOD Disease"""""""". There are five interrelated projects that concern 1) understanding pathophysiologic events which lead to insulitis and diabetes in NOD mice; 2) attempt to develop immunotherapeutic regimens to block ultimate beta cell destruction, or 3) to replace islet tissue via transplantation. Project I will attempt to understand the mechanisms involved in a form of transplantation tolerance induction: the use of monoclonal antibodies reactive with the T cell subset bearing the CD4 differentiation antigen. Recent data from Dr. Fathman's laboratory have supported the concept that T cell clonal anergy results from this form of immunotherapy. In collaboration with Dr. Gerald Crabtree, they will explore potential mechanisms of anergy as they relate to transplantation tolerance (Project I) or to potential forms of immunotherapy (Project V). Project II brings Dr. Mark Davis' expertise in T Cell receptor characterization to the area of diabetes research. Dr. Davis plans to collaborate with Dr. Fathman in isolation and characterization of T lymphocytes which are involved in early inductive events leading to insulitis and/or later events leading to beta cell destruction and overt hyperglycemia. In Project III, Dr. Irving Weissman brings his expertise in identification and isolation of hematopoietic stem cells to the area of diabetes experimentation. This project interrelates with Project I to develop new methodologies to allow transplantation tolerance induction for islet allografts. Additionally, Dr. Weissman intends to ask whether stem cell reconstitution will result in blockade of disease induction or perpetuation in NOD mice as has been previously demonstrated by allogeneic bone marrow transplantation. Project IV deals with the development of transgenic NOD mice in which putative autoantigens, previously identified as potentially involved in pathophysiologic events in NOD disease, will be used to develop transgenic models. The hypothesis to be tested is that anergy to such transgenes will develop and demonstrate whether the transgene product is involved in the development of NOD disease. Finally, Project V is an attempt to directly identify those T cells involved in early inductive events of inflammatory insulitis, as well as later sequelae leading to beta cell destruction. All five of these projects interrelate within the context of this Program Project Grant and are dedicated to understanding pathophysiologic events leading to insulitis and/or diabetes in NOD mice and to asking whether novel forms of potential immunotherapy might either allow transplantation of islets into diabetic mice or prevent beta cell destruction in NOD mice prior to overt hyperglycemia.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Program Projects (P01)
Project #
1P01DK044837-01
Application #
3095696
Study Section
Diabetes, Endocrinology and Metabolic Diseases B Subcommittee (DDK)
Project Start
1992-05-01
Project End
1997-04-30
Budget Start
1992-05-01
Budget End
1993-04-30
Support Year
1
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
Stanford University
Department
Type
Schools of Medicine
DUNS #
800771545
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Li, Jinzhu; Ridgway, William; Fathman, C Garrison et al. (2007) High cell surface expression of CD4 allows distinction of CD4(+)CD25(+) antigen-specific effector T cells from CD4(+)CD25(+) regulatory T cells in murine experimental autoimmune encephalomyelitis. J Neuroimmunol 192:57-67
Krieger, N R; Fathman, C G; Shaw, M K et al. (2000) Identification and characterization of the antigen-specific subpopulation of alloreactive CD4+ T cells in vitro and in vivo. Transplantation 69:605-9
Gandy, K L; Weissman, I L (1998) Tolerance of allogeneic heart grafts in mice simultaneously reconstituted with purified allogeneic hematopoietic stem cells. Transplantation 65:295-304
Ridgway, W; Fasso, M; Fathman, C G (1998) Following antigen challenge, T cells up-regulate cell surface expression of CD4 in vitro and in vivo. J Immunol 161:714-20
Ito, H; Fathman, C G (1997) CD45RBhigh CD4+ T cells from IFN-gamma knockout mice do not induce wasting disease. J Autoimmun 10:455-9
Krieger, N R; Fathman, C G (1997) The use of CD4 and CD8 knockout mice to study the role of T-cell subsets in allotransplant rejection. J Heart Lung Transplant 16:263-7
Krieger, N R; Ito, H; Fathman, C G (1997) Rat pancreatic islet and skin xenograft survival in CD4 and CD8 knockout mice. J Autoimmun 10:309-15
Shimada, A; Rohane, P; Fathman, C G et al. (1996) Pathogenic and protective roles of CD45RB(low) CD4+ cells correlate with cytokine profiles in the spontaneously autoimmune diabetic mouse. Diabetes 45:71-8
Yang, Y; Charlton, B; Shimada, A et al. (1996) Monoclonal T cells identified in early NOD islet infiltrates. Immunity 4:189-94
Ridgway, W M; Fasso, M; Lanctot, A et al. (1996) Breaking self-tolerance in nonobese diabetic mice. J Exp Med 183:1657-62

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