Abstract

Complement activation plays an important role in many human glomerular diseases and in the animal models that mimic these conditions.Although the deleterious effects of glomerular complement activation have been characterized in detail, the role of complement regulation in glomerular disorders is not well understood. During the tenure of the current R29 award, the Principal Investigator has isolated three complement regulatory substances produced by cultured rat glomerular epithelial cells (GEC). These are: 1) a chondroitin sulfate B proteoglycan termed glomerular complement regulatory factor (GCRF); 2) complement receptor type 1 (CR1); and, 3) Crry. These substances are present in vivo, and, therefore, are likely to have complement regulatory actions in that rat glomerulus. Previous studies in humans, and in models of human disease, suggest a role for abnormal complement regulation in several glomerulophathies. By defining the roles of glomerular CR1, Crry, and GCRF under normal and pathological conditions, the proposed research will test the hypothesis that impaired glomerular complement regulation results in disease.
Specific aims 1 and 2 are planned in cultured GEC. The capacity of CR1, Crry, and GCRF to limit complement activation on GEC under disease conditions will be evaluated. The likelihood that the pathogenic antibody of experimental rat membranous nephropathy binds and inhibits CR1 and Crry to account for its nephritogenicity will be assessed. The role for CR1 in processing immune complexes formed with both extrinsic and intrinsic antigens will also be evaluated. Expression of CR1, Crry, and GCRF will be determined in cultured GEC by measuring immunoreactive protein and mRNA quantities. GEC will be studied to discover which inflammatory stimuli account for absent CR1 protein but elevated mRNA expression in human lupus nephritis. The possibility that Crry and GCRF are affected similarly to CR1 under disease conditions will also be determined.
Specific aims 3 and 4 will be accomplished in rats. Alterations of Cr1, Crry, and GCRF proteins in different experimental glomerular diseases will be evaluated by immunoassay and histochemistry, while in situ and northern hybridizations will be performed to assess the localization and quantities of their mRNA. Rat models of immune complex glomerulonephritis, anti-glomerular basement membrane (GBM) nephritis, and membranous nephropathy will be studied. In human pathology specimens, CR1 has been shown to be reduced in each of these disorders. The functions of CR1, Crry, and GCRF under basal conditions in rats will be evaluated by the passive administration of F(ab')2 antibodies that neutralize the activity of the complement regulators. In addition, the role for inhibition of complement regulation by nephritogenic antibodies in rat models of anti-GBM nephritis and membranous nephropathy will be assessed. The part GEC CR1 plays in clearing immune complexes will be evaluated in a model of chronic serum sickness, in which circulating immune complexes traverse the glomerulus. The results of these studies in cultured cells and in animals will help define the role for complement regulation in human glomerular diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK041873-10
Application #
2444032
Study Section
Pathology B Study Section (PTHB)
Project Start
1989-08-15
Project End
1998-06-30
Budget Start
1997-08-01
Budget End
1998-06-30
Support Year
10
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
University of Chicago
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
225410919
City
Chicago
State
IL
Country
United States
Zip Code
60637

  Publications

Alexander, Jessy J; Chaves, Lee D; Chang, Anthony et al. (2016) Abrogation of immune complex glomerulonephritis by native carboxypeptidase and pharmacological antagonism of the C5a receptor. Cell Mol Immunol 13:651-7
Alexander, Jessy J; Chaves, Lee D; Chang, Anthony et al. (2015) CD11b is protective in complement-mediated immune complex glomerulonephritis. Kidney Int 87:930-9
Chaves, Lee Daniel; Bao, Lihua; Wang, Ying et al. (2014) Loss of CD11b exacerbates murine complement-mediated tubulointerstitial nephritis. PLoS One 9:e92051
Chaves, Lee D; Mathew, Liby; Shakaib, Mohammed et al. (2013) Contrasting effects of systemic monocyte/macrophage and CD4+ T cell depletion in a reversible ureteral obstruction mouse model of chronic kidney disease. Clin Dev Immunol 2013:836989
Naik, Abhijit; Sharma, Shweta; Quigg, Richard J (2013) Complement regulation in renal disease models. Semin Nephrol 33:575-85
Jacob, Alexander; Chaves, Lee; Eadon, Michael T et al. (2013) Curcumin alleviates immune-complex-mediated glomerulonephritis in factor-H-deficient mice. Immunology 139:328-37
Cravedi, Paolo; van der Touw, William; Heeger, Peter S (2013) Complement regulation of T-cell alloimmunity. Semin Nephrol 33:565-74
Alexander, Jessy J; Chaves, Lee; Chang, Anthony et al. (2012) The C5a receptor has a key role in immune complex glomerulonephritis in complement factor H-deficient mice. Kidney Int 82:961-8
Bao, Lihua; Wang, Ying; Haas, Mark et al. (2011) Distinct roles for C3a and C5a in complement-induced tubulointerstitial injury. Kidney Int 80:524-34
Bao, Lihua; Haas, Mark; Quigg, Richard J (2011) Complement factor H deficiency accelerates development of lupus nephritis. J Am Soc Nephrol 22:285-95

Showing the most recent 10 out of 46 publications