Abstract

It is not yet known whether an antigen-specific event or a more global defect in immune regulation allows the initiation of insulitis in insulin- dependent diabetes mellitus (IDDM). This grant intends to explore two competing hypothesis concerning the """"""""initiation"""""""" of auto-immune insulitis. The first, more traditional paradigm: initiation of type I diabetes in NOD mice (and in man) is associated with the major histocompatibility complex (MHC) class II gene products due to presentation of """"""""diabetogenic"""""""" islet beta cell antigens to T cells. The contrasting novel hypothesis suggests that autoimmunity in the NOD mouse is, in part, due to """"""""inefficient"""""""" I- A/g7 thymic editing (positive and negative selection) leading to a repertoire of CD4 T cells in NOD mice which have high affinity T cell receptor (TCR) regulation of self-peptides. These two hypothesis will be tested by analyzing the earliest islet-infiltrating NOD T cells. T cells will be examined directly from the early insulitic lesions, as well as after adoptive transfer of """"""""early"""""""" NOD islet-infiltrating T cells into NOD Rag-2 knockout mice. Hybridomas and T cell clones derived from islet infiltrating T cells will be used to screen a beta cell-enriched expression library. An additional set of experiments will study thymic editing (positive and negative selection) in NOD mice which may lead to the escape of high affinity self-reactive T cells and resultant widespread autoimmunity. The final set of experiments, using cell surface CD4 expression (which increases dramatically on activated T cells), FACS sorting, limiting dilution analyses and T cell cloning, should allow characterization of islet antigen-specific T cells. This grant proposes to study (1) antigens recognized by islet-infiltrating T cells, (2) potential defects in thymic education involved in the pathophysiology of NOD disease and (3) the pathophysiology of inflammatory insulitis in NOD mice. It is proposed that such studies may provide an understanding of components of the pathophysiology of human IDDM.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK039959-13
Application #
6164521
Study Section
Immunological Sciences Study Section (IMS)
Program Officer
Akolkar, Beena
Project Start
1988-03-01
Project End
2002-02-28
Budget Start
2000-03-01
Budget End
2001-02-28
Support Year
13
Fiscal Year
2000
Total Cost
$335,685
Indirect Cost

  Institution

Name
Stanford University
Department
Internal Medicine/Medicine
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
Szanya, Veronika; Ermann, Joerg; Taylor, Cariel et al. (2002) The subpopulation of CD4+CD25+ splenocytes that delays adoptive transfer of diabetes expresses L-selectin and high levels of CCR7. J Immunol 169:2461-5
Urbanek-Ruiz, I; Ruiz, P J; Paragas, V et al. (2001) Immunization with DNA encoding an immunodominant peptide of insulin prevents diabetes in NOD mice. Clin Immunol 100:164-71
Fasso, M; Anandasabapathy, N; Crawford, F et al. (2000) T cell receptor (TCR)-mediated repertoire selection and loss of TCR vbeta diversity during the initiation of a CD4(+) T cell response in vivo. J Exp Med 192:1719-30
Lejon, K; Fathman, C G (1999) Isolation of self antigen-reactive cells from inflamed islets of nonobese diabetic mice using CD4high expression as a marker. J Immunol 163:5708-14
Seroogy, C M; Fathman, C G (1998) A gene therapy approach to treatment of autoimmune disease. Immunol Res 18:15-26
Ridgway, W M; Ito, H; Fasso, M et al. (1998) Analysis of the role of variation of major histocompatibility complex class II expression on nonobese diabetic (NOD) peripheral T cell response. J Exp Med 188:2267-75
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
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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