Self antigen is the target of most nephritogenic immune responses, yet little is known abut the proximal events that generate, regulate, and induce expression of autoreactive lymphocytes. Effective therapy for severe autoimmune disease thus remains limited to nonspecific and toxic immunosuppression. The goal of the proposed studies is to gain a better understanding of the immunologic mechanisms that normally regulate nephritogenic humoral autoimmunity, as a basis for developing more specific interventions to eliminate or inactivate autoreactive cells and/or reestablish tolerance. These studies emphasize autoantibodies that target renal basement membrane (BM) antigens because BM proteins are the only confirmed renal targets in human autoimmune nephritis, BM is targeted in both systemic and organ-restricted autoimmunity, and regular of immune responses to these complex matrix antigens has been virtually ignored to date. The proposed studies will test the hypothesis that unmutated nephritogenic anti-laminin and anti-DNA B cells similar to those activated in systemic lupus are present but tolerant in the normal host; that their expression can be induced by inherited autoimmune susceptibility and/or environmental challenge; and that nephritogenic anti-alpha3(IV)NC1 collagen B cells persist as nontolerant (""""""""ignorant"""""""") lymphocytes in the periphery of nonautoimmune hosts until activated by specific immunization in a permissive genetic background. The Ig transgenic approach is used for this purpose because it permits enrichment for the autoreactive B cell population of interest while preserving complex immunologic microenvironments in vivo. Six established Ig-tg lines that encode lupus anti-laminin (LamH) or nephritogenic and anti-DNA (238H) Ig will be used to determine the presence, phenotype, functional state and pathogenecity of autoreactive B cells in the nonautoimmune B6 and autoimmune MRL genetic backgrounds. Laminin epitopes recognized by autoantibodies will be determined, using spontaneous Ig recovered from nontolerant mice and Ig rescued from tolerance mice by in vitro or in vivo bcl-2 expression. Finally, B6 mice will be rendered transgenic for an anti-alpha3(IV)NC1 Mab that recognizes Goodpasture's epitope, to determine the tolerance phenotype of B cells specific for a cryptic and organ-restricted BM antigen targeted in severe human nephritis. The autoantibody transgenic model thus provides a well defined experimental system in which to study immunologic mechanisms and etiologic influences and to test novel therapeutic interventions for autoimmune renal disease.

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK047424-06
Application #
6138016
Study Section
Pathology A Study Section (PTHA)
Program Officer
Flessner, Michael Francis
Project Start
1995-01-01
Project End
2000-06-30
Budget Start
2000-01-01
Budget End
2000-06-30
Support Year
6
Fiscal Year
2000
Total Cost
$50,926
Indirect Cost
Name
University of Pennsylvania
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104
Clark, Amy G; Buckley, Elizabeth S; Foster, Mary H (2018) Altered toll-like receptor responsiveness underlies a dominant heritable defect in B cell tolerance in autoimmune New Zealand Black mice. Eur J Immunol 48:492-497
Clark, Amy G; Fan, Qihua; Brady, Graham F et al. (2013) Regulation of basement membrane-reactive B cells in BXSB, (NZBxNZW)F1, NZB, and MRL/lpr lupus mice. Autoimmunity 46:188-204
Clark, Amy G; Weston, Melissa L; Foster, Mary H (2013) Lack of galectin-1 or galectin-3 alters B cell deletion and anergy in an autoantibody transgene model. Glycobiology 23:893-903
Clark, Amy G; Mackin, Katherine M; Foster, Mary H (2011) Genetic elimination of ?3(IV) collagen fails to rescue anti-collagen B cells. Immunol Lett 141:134-9
Zhang, Ying; Su, Susan C; Hecox, Douglas B et al. (2008) Central tolerance regulates B cells reactive with Goodpasture antigen alpha3(IV)NC1 collagen. J Immunol 181:6092-100
Clark, Amy G; Mackin, Katherine M; Foster, Mary H (2008) Tracking Differential Gene Expression in MRL/MpJ Versus C57BL/6 Anergic B Cells: Molecular Markers of Autoimmunity. Biomark Insights 3:335-350
Foster, Mary H (2007) T cells and B cells in lupus nephritis. Semin Nephrol 27:47-58
Clark, Amy G; Chen, Sihong; Zhang, Hao et al. (2007) Multifunctional regulators of cell growth are differentially expressed in anergic murine B cells. Mol Immunol 44:1274-85
Foster, Mary H; Zhang, Ying; Clark, Amy G (2006) Deconstructing B cell tolerance to basement membranes. Arch Immunol Ther Exp (Warsz) 54:227-37
Brady, Graham F; Congdon, Kendra L; Clark, Amy G et al. (2004) Kappa editing rescues autoreactive B cells destined for deletion in mice transgenic for a dual specific anti-laminin Ig. J Immunol 172:5313-21

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