Abstract

A critical factor in early pancreas and islet graft failure in individuals suffering from insulin-dependent diabetes mellitus (IDDM) is recurrent autoimmune- mediated destruction of the insulin producing beta cells. One approach to establish host tolerance to the grafts is to promote beta cell antigen- specific immune deviation. In this way, antigen-specific regulatory Th2 cells are induced to suppress the activity of autoreactive Th1 cells. The investigators and others have shown that this approach is indeed effective in preventing diabetes in the NOD mouse, a murine model for spontaneous IDDM. Furthermore, the applicants have recent evidence demonstrating that an ongoing diabetogenic response can be suppressed in NOD mice treated with the beta cell autoantigen glutamic acid decarboxylase (GAD65). The current challenge, however, is to establish strategies of immune deviation which induce effective, long-term protection in a safe manner. With this in mind, the applicants have developed four specific aims. First, the applicants will determine the phenotype and peptide specificity of GAD65- specific regulatory T cells capable of suppressing ongoing IDDM in NOD mice. Furthermore, the investigators will examine the relative contribution of CD4+ Th2 cells in disease suppression, and the precise mechanism by which this protection is mediated. Second, the applicants will determine whether GAD65- and insulin chain-specific peptide immunotherapy can effectively induce regulatory T cells and suppress ongoing IDDM in NOD mice. Third, the investigators will assess the feasibility of genetic vaccines as a delivery system to induce beta cell antigen-specific regulatory T cells and in turn, prevent and suppress the diabetogenic response. Fourth, the investigators will determine whether beta cell autoantigen-specific induced immune deviation can lead to permanent protection for syngeneic islets grafted in overtly diabetic NOD mice. In addition, the applicants will assess the applicability of antigen-specific immune deviation to suppress an islet allograft response.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI041580-02
Application #
6100166
Study Section
Project Start
1998-08-01
Project End
1999-07-31
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
2
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
University of North Carolina Chapel Hill
Department
Type
DUNS #
078861598
City
Chapel Hill
State
NC
Country
United States
Zip Code
27599

  Publications

van Deventer, Hendrik W; Serody, Jonathon S; McKinnon, Karen P et al. (2002) Transfection of macrophage inflammatory protein 1 alpha into B16 F10 melanoma cells inhibits growth of pulmonary metastases but not subcutaneous tumors. J Immunol 169:1634-9
June Brickey, W; Felix, Nathan J; Griffiths, Robert et al. (2002) Prolonged survival of class II transactivator-deficient cardiac allografts. Transplantation 74:1341-8
Felix, Nathan J; de Serres, Suzan; Meyer, Anthony A et al. (2002) Comparison of Abeta(b-/-), H2-DM(-), and CIITA(-/-) in second-set skin allograft rejection. J Surg Res 102:185-92
Tisch, R; Wang, B; Weaver, D J et al. (2001) Antigen-specific mediated suppression of beta cell autoimmunity by plasmid DNA vaccination. J Immunol 166:2122-32
Taxman, D J; Ting, J P (2001) Identification of novel Mycoplasma hyorhinis gene fragments by differential display analysis of co-cultures. J Microbiol Methods 44:217-23
Weaver Jr, D J; Liu, B; Tisch, R (2001) Plasmid DNAs encoding insulin and glutamic acid decarboxylase 65 have distinct effects on the progression of autoimmune diabetes in nonobese diabetic mice. J Immunol 167:586-92
Maile, R; Wang, B; Schooler, W et al. (2001) Antigen-specific modulation of an immune response by in vivo administration of soluble MHC class I tetramers. J Immunol 167:3708-14
Felix, N J; Brickey, W J; Griffiths, R et al. (2000) H2-DMalpha(-/-) mice show the importance of major histocompatibility complex-bound peptide in cardiac allograft rejection. J Exp Med 192:31-40
Piskurich, J F; Lin, K I; Lin, Y et al. (2000) BLIMP-I mediates extinction of major histocompatibility class II transactivator expression in plasma cells. Nat Immunol 1:526-32
Taxman, D J; Cressman, D E; Ting, J P (2000) Identification of class II transcriptional activator-induced genes by representational difference analysis: discoordinate regulation of the DN alpha/DO beta heterodimer. J Immunol 165:1410-6

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