Effects of high glucose concentrations on human mesangial cell proliferation


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Effects of high glucose concentrations on human mesangial cell proliferation

FG Cosio
Department of Internal Medicine, Nephrology, Ohio State University, Columbus 43210-1228, USA.

High concentrations of glucose in vitro inhibit cell proliferation and stimulate matrix protein synthesis. These studies sought to characterize the relationship between the effects of glucose on cell proliferation and matrix synthesis and to assess the mechanism(s) responsible for these cellular effects of glucose. The initial experiments showed that high glucose levels stimulate fibronectin (FN) synthesis by human mesangial cells (HMC) but only in those cultures in which cell proliferation was inhibited by glucose. To assess whether this relationship was due to an effect of glucose on the capacity of HMC to respond to cytokines, the responses of HMC to serum or cytokines were measured in the presence of different glucose concentrations. High concentrations of glucose inhibited (3H)thymidine incorporation in response to serum and platelet-derived growth factor. Under the conditions of these experiments, transforming growth factor-beta (TGF- beta) also stimulated thymidine incorporation by HMC, and high glucose concentrations inhibited thymidine incorporation in response to TGF- beta. In contrast, high concentrations of glucose did not inhibit the stimulation of FN synthesis caused by platelet-derived growth factor, serum, or TGF-beta. The antiproliferative effects of high glucose levels were first observed after 48 h of incubation and were reversible after the withdrawal of high glucose from the media. The following evidence suggest that the effects of glucose may be mediated via protein kinase C (PKC): (1) incubation with high glucose concentrations caused an increase in HMC PKC levels; (2) PKC activation with phorbol esters inhibited HMC proliferation; and (3) depletion or inhibition of PKC stimulated HMC proliferation and prevented the antiproliferative effects of glucose. In contrast to these findings, inhibitors of protein glycosylation and myo-inositol supplementation of culture media did not prevent the antiproliferative effects of glucose. In conclusion, high glucose concentrations acutely and reversibly inhibit HMC proliferation, perhaps by a PKC-dependent mechanism. Because PKC can also stimulate FN synthesis, glucose-induced changes in PKC may explain the relationship between the effects of high glucose concentrations on cell proliferation and FN synthesis.

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				S. Lin, A. Sahai, S. S. Chugh, X. Pan, E. I. Wallner, F. R. Danesh, J. W. Lomasney, and Y. S. Kanwar High Glucose Stimulates Synthesis of Fibronectin via a Novel Protein Kinase C, Rap1b, and B-Raf Signaling Pathway J. Biol. Chem., October 25, 2002; 277(44): 41725 - 41735. [Abstract] [Full Text] [PDF]

				C. I. Whiteside and J. A. Dlugosz Mesangial cell protein kinase C isozyme activation in the diabetic milieu Am J Physiol Renal Physiol, June 1, 2002; 282(6): F975 - F980. [Abstract] [Full Text] [PDF]

				L. A. Silveira, C. E. Bacchi, G. A. Pinto, and J. B. L. de Faria The Genetics of Hypertension Modifies the Renal Cell Replication Response Induced by Experimental Diabetes Diabetes, May 1, 2002; 51(5): 1529 - 1534. [Abstract] [Full Text] [PDF]

				S. J. Shankland and G. Wolf Cell cycle regulatory proteins in renal disease: role in hypertrophy, proliferation, and apoptosis Am J Physiol Renal Physiol, April 1, 2000; 278(4): F515 - F529. [Abstract] [Full Text] [PDF]

				M. B. Ganz, K. Hawkins, and R. F. Reilly High glucose induces the activity and expression of Na+/H+ exchange in glomerular mesangial cells Am J Physiol Renal Physiol, January 1, 2000; 278(1): F91 - F96. [Abstract] [Full Text] [PDF]

				J. KAPOR-DREZGIC, X. ZHOU, T. BABAZONO, J. A. DLUGOSZ, T. HOHMAN, and C. WHITESIDE Effect of High Glucose on Mesangial Cell Protein Kinase C-{delta} and - is Polyol Pathway-Dependent J. Am. Soc. Nephrol., June 1, 1999; 10(6): 1193 - 1203. [Abstract] [Full Text]

				P. Nelson, K Moissoglu, J Vargas, P. Klotman, and I. Gelman Involvement of the protein kinase C substrate, SSeCKS, in the actin-based stellate morphology of mesangial cells J. Cell Sci., January 2, 1999; 112(3): 361 - 370. [Abstract] [PDF]