Abstract

The hypothesis underlying this proposal is that cytokines derived from platelets, glomerular endothelial cells, and macrophages regulate glomerular mesangial and endothelial cell proliferation and matrix production. The overexpression of these cellular functions may lead to the development glomerular sclerosis. It is postulated that two likely mediators involved in the process of glomerular sclerosis are platelet derived growth factor and transforming growth factor beta, both platelet products which may also be synthesized by glomerular endothelial cells. Methods were developed in the past 12 months which allow routine culture of bovine glomerular endothelial cells. Therefore, the influence of cytokines on glomerular endothelial and mesangial cells in vitro can be determined, and the role of glomerular endothelial cell-derived mediators on glomerular mesangial cell function can be examined. The proposed studies will delineate glomerular endothelial cell and mesangial cell proliferation, matrix synthesis, and other functions in response to a number of known polypeptide cytokines. Studies will involve the determination of DNA synthesis, cell number as a function of time, and the quantification of collagen, matrix proteoglycan add fibronectin synthesis. The question whether platelet derived growth factor and transforming growth factor beta modulate glomerular cell growth and matrix synthesis will receive particular attention. Using gel filtration chromatography, enzyme susceptibility profiles, radioligand binding inhibition studies, neutralizing antibody studies and Western blotting techniques, the proposal furthermore seeks to define the identity of mitogenic and anti-proliferative mediators released by glomerular endothelial cells. Finally, in co-culture systems it will determined whether specific mediators released by glomerular endothelial cells in fact regulate mesangial cell proliferation and matrix synthesis. These studies will identify possible mediators that may alter glomerular mesangial cell and endothelial cell functions to produce glomerular sclerosis in vivo.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Program Projects (P01)
Project #
5P01DK040839-02
Application #
3876244
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
2
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
Brigham and Women's Hospital
Department
Type
DUNS #
071723621
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Kelley, V R; Strom, T B (1995) A paradigm 1994: the allograft response. Blood Purif 13:199-205
Ballermann, B J; Ott, M J (1995) Adhesion and differentiation of endothelial cells by exposure to chronic shear stress: a vascular graft model. Blood Purif 13:125-34
Yokoyama, H; Kreft, B; Kelley, V R (1995) Biphasic increase in circulating and renal TNF-alpha in MRL-lpr mice with differing regulatory mechanisms. Kidney Int 47:122-30
Yokoyama, H; Zheng, X; Strom, T B et al. (1994) B7(+)-transfectant tubular epithelial cells induce T cell anergy, ignorance or proliferation. Kidney Int 45:1105-12
Diamond, J R (1994) The adverse effects of cholesterol in progressive glomerular injury. Md Med J 43:451-5
Kim, E G; Choi, M E; Ballermann, B J (1994) Spatially restricted expression of set mRNA in developing rat kidney. Am J Physiol 266:F155-61
Rennke, H G (1994) How does glomerular epithelial cell injury contribute to progressive glomerular damage? Kidney Int Suppl 45:S58-63
Oliver 3rd, J D; Simons, J L; Troy, J L et al. (1994) Proteinuria and impaired glomerular permselectivity in uninephrectomized fawn-hooded rats. Am J Physiol 267:F917-25
Simons, J L; Provoost, A P; Anderson, S et al. (1994) Modulation of glomerular hypertension defines susceptibility to progressive glomerular injury. Kidney Int 46:396-404
Rubin Kelley, V; Bloom, R D; Yui, M A et al. (1994) Pivotal role of colony stimulating factor-1 in lupus nephritis. Kidney Int Suppl 45:S83-5

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