Abstract

Diabetes mellitus is a major cause of renal morbidity and mortality. Approximately 25-40% of all patients with insulin dependent diabetes mellitus will develop clinical nephropathy. The constellation of the lesions of diabetic glomerulosclerosis associated with the clinical expression of this disorder is unique. The striking morphological feature is the expansion of the mesangial matrix which accounts for the increase in the mesangial volume fraction. This lesion is correlated with decreased capillary filtration surface and with albuminuria, hypertension and declining GFR. The mechanisms involved in the expansion of mesangial matrix are not known. In diabetic nephropathy, the deposition of fibronectin, laminin and type IV collagen is increased in the mesangium. Possible explanations for this increase include: Increased synthesis of matrix by mesangial cells; increased rate of incorporation of proteins into the matrix due to altered binding of matrix proteins to mesangial cells, decreased rates of degradation of matrix by mesangial cells or some combination of these three possibilities. We have found by immunocytochemistry, gel electrophoresis and solid phase ELISA that cultures of mesangial cells grown continuously for 4 weeks under conditions that mimic the diabetic environment (i.e., high glucose, 30 mM) display increased deposition of fibronectin, laminin, and type IV collagen similar to that reported in diabetic nephropathy in vivo. The objective of this proposal is to determine the mechanism(s) of this increased matrix deposition by mesangial cells grown in high glucose-containing medium.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK029787-13
Application #
2138228
Study Section
Pathology A Study Section (PTHA)
Project Start
1981-08-01
Project End
1996-12-31
Budget Start
1994-04-01
Budget End
1996-12-31
Support Year
13
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
University of Texas Health Science Center San Antonio
Department
Pathology
Type
Schools of Medicine
DUNS #
800772162
City
San Antonio
State
TX
Country
United States
Zip Code
78229

  Publications

Kreisberg, J I; Ghosh-Choudhury, N; Radnik, R A et al. (1997) Role of Rho and myosin phosphorylation in actin stress fiber assembly in mesangial cells. Am J Physiol 273:F283-8
Kreisberg, J I; Radnik, R A; Kreisberg, S H (1996) Phosphorylation of cAMP responsive element binding protein after treatment of mesangial cells with high glucose plus TGF beta or PMA. Kidney Int 50:805-10
Kreisberg, J I; Kreisberg, S H (1995) High glucose activates protein kinase C and stimulates fibronectin gene expression by enhancing a cAMP response element. Kidney Int Suppl 51:S3-11
Kreisberg, J I; Radnik, R A; Ayo, S H et al. (1994) High glucose elevates c-fos and c-jun transcripts and proteins in mesangial cell cultures. Kidney Int 46:105-12
Feng, L; Xia, Y; Kreisberg, J I et al. (1994) Interleukin-1 alpha stimulates KC synthesis in rat mesangial cells: glucocorticoids inhibit KC induction by IL-1. Am J Physiol 266:F713-22
Kreisberg, J I; Garoni, J A; Radnik, R et al. (1994) High glucose and TGF beta 1 stimulate fibronectin gene expression through a cAMP response element. Kidney Int 46:1019-24
Glass 2nd, W F; Troyer, D A; Kreisberg, J I (1994) Regulation of mesangial cell function by thrombin. Semin Thromb Hemost 20:333-8
Kreisberg, J I; Ayo, S H (1993) The glomerular mesangium in diabetes mellitus. Kidney Int 43:109-13
Glass 2nd, W F; Kreisberg, J I; Troyer, D A (1993) Two-chain urokinase, receptor, and type 1 inhibitor in cultured human mesangial cells. Am J Physiol 264:F532-9
Glass 2nd, W F; Kreisberg, J I (1993) Regulation of integrin-mediated adhesion at focal contacts by cyclic AMP. J Cell Physiol 157:296-306

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