Abstract

With mounting evidence of autoimmune mechanisms in the pathogenesis of Type I insulin-dependent diabetes mellitus (IDDM), and the availability of the BB/w rat model of IDDM, it has become possible to formulate and test strategies in using specific immunological techniques in clarifying and modulating this disease. With out continued interest in islet transpolantation as a potential cure for IDDM, we have been investigating the potential autoimmune destruction of native and transplanted islets. Our in vivo preliminary results show that MHC matched and mismatched islets transplanted into acutely diabetic BB/w rats are equally destroyed; evidence that the autoimmune mechanism leading to initial expression of IDDM is active and not restricted by the MHC. We have expanded this work to show that cytotoxic T lymphocytes (CTL) against islet cells can be derived from the acutely diabetic BB/w rat at the non-clonal and clonal levels. They appear in vitro to be specific for islet cells and not to be restricted by the MHC. Our ability to generate these cytotoxic cell lines specific for islet cells (beta cells?) makes it possible to formulate and execute the following series of experiments to attempt specific immunological modulation of IDDM in the BB/w rat model, not only as a means of modulating the native disease, but as a method of protection against autoimmune destruction of transplanted islets. We, therefore, propose 1) to generate islet beta-cell reactive cytolytic and non-cytolytic T cell clones from the acutely diabetic BB/w rat and to define their specificity toward endocrine (beta-cell, non beta-cell) and non-endocrine cells; 2) to use these beta-cell specific T effector cell lines in the induction of IDDM in diabetic prone and non-diabetic prone BB/w rats and to investigate the possible role that such cytolytic and non-cytolytic beta-cell specific T cells may play in the manifestation of diabetes mellitus; 3) to test the possibility of using the T effector cells in an attenuated form (Gamma irradiated) to vaccinate diabetic prone BB/w rats against the development of IDDM; and 4) to generate monoclonal antibodies (MAb) recognizing the t cell receptors of the anti-beta-cell specific CTL's and possibly use these MAb's in the modulation of the onset and progression of IDDM in the BB/w rat.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK035228-03
Application #
3233513
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Project Start
1985-12-01
Project End
1988-11-30
Budget Start
1987-12-01
Budget End
1988-11-30
Support Year
3
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
Columbia University (N.Y.)
Department
Type
Schools of Medicine
DUNS #
064931884
City
New York
State
NY
Country
United States
Zip Code
10027

  Publications

Hardy, M A; Suciu-Foca, N; Reed, E et al. (1991) Immunomodulation of kidney and heart transplants by anti-idiotypic antibodies. Ann Surg 214:522-8;discussion 528-30
Wasfie, T; Reed, E; Marboe, C et al. (1991) The effect of antiidiotypic antibodies in the rat: II. Correlation of in vitro blocking activity and immunopathology of cardiac allograft survival. Transplant Proc 23:378-9
Binah, O; Zhang, H L; Oluwole, S F et al. (1991) Mechanical and electrophysiologic changes in rat cardiac allografts during immunologic rejection. Transplantation 52:508-12
Oluwole, S F; Engelstad, K; Hardy, M A (1990) Prevention of GVHD by modulation of rat bone marrow with UV-B irradiation: II. Kinetics of migration of UV-B-irradiated bone marrow cells in naive and lethally irradiated rats. Cell Immunol 128:289-300
Stegall, M D; Tezuka, K; Oluwole, S F et al. (1990) Interstitial class II-positive cell depletion by donor pretreatment with gamma irradiation. Evidence of differential immunogenicity between vascularized cardiac allografts and islets. Transplantation 49:246-51
Chabot, J A; Pepino, P; Wasfie, T et al. (1990) UVB pretreatment of rat bone marrow allografts. Prevention of GVHD and induction of allochimerism and donor-specific unresponsiveness. Transplantation 49:886-9
Marin, M L; Gordon, R E; Hardy, M A et al. (1990) Immunomodulation of vascular endothelium. 1. Ultrastructural changes following ultraviolet B irradiation of peripheral veins. J Surg Res 48:134-43
Wasfie, T; Reed, E; Suciu-Foca, N et al. (1990) Production of antiidiotypic antibodies in the rat: in vitro characterization of specificity and correlation with in vivo specific suppression of cardiac allograft immune reaction across major histocompatibility complex. Surgery 108:431-40;discussion 440-1
Marin, M L; Hardy, M A; Gordon, R E et al. (1990) Immunomodulation of vascular endothelium: effects of ultraviolet B irradiation on vein allograft rejection. J Vasc Surg 11:103-11
Patel, A; Hardy, M A; Chowdhury, N R et al. (1989) Long-term correction of genetic defect of liver function in rat by transplantation of liver cells after ultraviolet irradiation. Mol Biol Med 6:187-96

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