Abstract

Lupus nephritis is believed to result from glomerular deposition of immune complexes, triggering local kidney inflammation, followed by worsening glomerulosclerosis and end stage renal disease. The mechanisms responsible for this chronic kidney disease progression are poorly understood. Several reports and our preliminary data suggest a link between decreases in T cell production of transforming growth factor beta (TGFbeta) with autoantibody production, and increases in renal TGFbeta expression with the development of chronic kidney lesions. The central hypothesis of this proposal is that TGFbeta plays dual roles in the development and progression of lupus nephritis: while decreased TGFbeta levels promote early stage lupus nephritis by enhancing T and B cell activation and autoantibody production, increased TGFbeta levels accelerate late stage kidney disease by inducing increased extracellular matrix production. The proposed studies will evaluate changes in the expression levels of TGFb, its receptors and signaling proteins in the lymphoid and renal tissues during progression of kidney disease in murine models of lupus. These studies will build on preliminary data indicating that urine TGFbeta levels rise in response to increases in TGFbeta activity in lupus kidney cells, thus serving as a diagnostic marker for chronic kidney damage. The proposed studies will also investigate the potential mechanisms of renal TGFb overexpression in lupus, and more importantly, determine the contribution of the TGFbeta system to autoantibody production and kidney damage. TGFbeta blockade in vivo using monoclonal antibodies will be investigated as a potential therapeutic approach that could inhibit or reverse the development of chronic kidney lupus disease, without worsening autoimmunity. Our broad goals in this proposal are to understand the mechanisms of kidney damage in lupus. Relevant to the current RFA, this proposal will: a) identify a diagnostic marker (e.g., urine TGFbeta levels) that will allow prediction of the progression of disease in target organs, b) make use of novel conditional, tissue-specific TGFb signaling knockout mice to investigate the mechanisms that cause matrix deposition and tissue damage, and c) explore alternative treatment strategies for preventing organ damage in lupus.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR050797-04
Application #
6891949
Study Section
Special Emphasis Panel (ZAR1-TAS-D (O2))
Program Officer
Gretz, Elizabeth
Project Start
2003-09-30
Project End
2007-05-31
Budget Start
2005-06-01
Budget End
2006-05-31
Support Year
4
Fiscal Year
2005
Total Cost
$374,460
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
092530369
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Yang, Jun-Qi; Kim, Peter J; Singh, Ram Raj (2012) Brief treatment with iNKT cell ligand ýý-galactosylceramide confers a long-term protection against lupus. J Clin Immunol 32:106-13
Yang, Jun-Qi; Wen, Xiangshu; Kim, Peter J et al. (2011) Invariant NKT cells inhibit autoreactive B cells in a contact- and CD1d-dependent manner. J Immunol 186:1512-20
Azhar, Mohamad; Yin, Moying; Bommireddy, Ramireddy et al. (2009) Generation of mice with a conditional allele for transforming growth factor beta 1 gene. Genesis 47:423-31
Eriksson, Anna U; Singh, Ram Raj (2008) Cutting edge: migration of langerhans dendritic cells is impaired in autoimmune dermatitis. J Immunol 181:7468-72
Saxena, Vijay; Lienesch, Douglas W; Zhou, Min et al. (2008) Dual roles of immunoregulatory cytokine TGF-beta in the pathogenesis of autoimmunity-mediated organ damage. J Immunol 180:1903-12
Khurma, Vandana; Meyer, Cris; Park, Grace S et al. (2008) A pilot study of subclinical coronary atherosclerosis in systemic sclerosis: coronary artery calcification in cases and controls. Arthritis Rheum 59:591-7
Wong, Maida; Ziring, David; Korin, Yael et al. (2008) TNFalpha blockade in human diseases: mechanisms and future directions. Clin Immunol 126:121-36
Smith-Bouvier, Deborah L; Divekar, Anagha A; Sasidhar, Manda et al. (2008) A role for sex chromosome complement in the female bias in autoimmune disease. J Exp Med 205:1099-108
Lin, Jan; Ziring, David; Desai, Sheetal et al. (2008) TNFalpha blockade in human diseases: an overview of efficacy and safety. Clin Immunol 126:13-30
Bommireddy, Ramireddy; Babcock, George F; Singh, Ram R et al. (2008) TGFbeta1 deficiency does not affect the generation and maintenance of CD4+CD25+FOXP3+ putative Treg cells, but causes their numerical inadequacy and loss of regulatory function. Clin Immunol 127:206-13

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