Heparin reduces glomerular infiltration and TGF-beta protein expression by macrophages in puromycin glomerulosclerosis.

@article{citeulike:2663192, abstract = {BACKGROUND: In a number of experimental models of nephropathy, heparin is renoprotective because it inhibits mesangial matrix synthesis and cell proliferation; in most of these models, glomerular macrophage infiltration has a pathogenic role. We investigated the hypothesis that heparin might also be renoprotective by modulating the macrophages in various ways in the chronic puromycin glomerulosclerosis model. METHODS: We studied the effect of a 3 month course, two different dosages of a non-anticoagulant heparin by immunohistochemical evaluation of the number of macrophages (ED-1 positive cells) in glomeruli, as well as the expression and deposition of TGF-beta and latent TGF-beta binding protein in foam cells and mesangial matrix. RESULTS: The renoprotective effect of heparin in this model was confirmed by our observation of lower urine protein and albumin excretion, and a reduced glomerular sclerosis score. These effects were associated with the prevention of macrophage glomerular infiltration, and the inhibition of the TGF-beta axes in foam cells as shown by the reduction in cytoplasm immunostaining for TGF-beta and LTBP-1; heparin also reduced peri-macrophagic collagen IV deposition. CONCLUSIONS: The inhibition of TGF-beta in macrophages seems to be part of heparin general activities. The inhibitory effect of heparin on macrophage infiltration and TGF-beta synthesis in this renal disease model supports the notion that heparin and derived molecules constitute potentially useful therapeutic agents in nephropathies.}, address = {Department of Medical and Surgical Sciences, Division of Nephrology, Policlinico Universitario, University of Padua, Via Giustiniani 2, 35128 Padua, Italy.}, author = {Ceol, M. and Vianello, D. and Schleicher, E. and Anglani, F. and Barbanti, M. and Bonfante, L. and Bertaglia, G. and Graziotto, R. and D'Angelo, A. and Del Prete, D. and Gambaro, G. }, citeulike-article-id = {2663192}, issn = {1121-8428}, journal = {Journal of nephrology}, number = {2}, pages = {210--218}, posted-at = {2008-04-13 10:12:40}, priority = {2}, title = {Heparin reduces glomerular infiltration and TGF-beta protein expression by macrophages in puromycin glomerulosclerosis.}, url = {http://view.ncbi.nlm.nih.gov/pubmed/12768067}, volume = {16}, year = {2003} }

TY - JOUR ID - citeulike:2663192 L3 - citeulike-article-id:2663192 TI - Heparin reduces glomerular infiltration and TGF-beta protein expression by macrophages in puromycin glomerulosclerosis. JF - Journal of nephrology VL - 16 IS - 2 SP - 210 EP - 218 AD - Department of Medical and Surgical Sciences, Division of Nephrology, Policlinico Universitario, University of Padua, Via Giustiniani 2, 35128 Padua, Italy. SN - 1121-8428 N2 - BACKGROUND: In a number of experimental models of nephropathy, heparin is renoprotective because it inhibits mesangial matrix synthesis and cell proliferation; in most of these models, glomerular macrophage infiltration has a pathogenic role. We investigated the hypothesis that heparin might also be renoprotective by modulating the macrophages in various ways in the chronic puromycin glomerulosclerosis model. METHODS: We studied the effect of a 3 month course, two different dosages of a non-anticoagulant heparin by immunohistochemical evaluation of the number of macrophages (ED-1 positive cells) in glomeruli, as well as the expression and deposition of TGF-beta and latent TGF-beta binding protein in foam cells and mesangial matrix. RESULTS: The renoprotective effect of heparin in this model was confirmed by our observation of lower urine protein and albumin excretion, and a reduced glomerular sclerosis score. These effects were associated with the prevention of macrophage glomerular infiltration, and the inhibition of the TGF-beta axes in foam cells as shown by the reduction in cytoplasm immunostaining for TGF-beta and LTBP-1; heparin also reduced peri-macrophagic collagen IV deposition. CONCLUSIONS: The inhibition of TGF-beta in macrophages seems to be part of heparin general activities. The inhibitory effect of heparin on macrophage infiltration and TGF-beta synthesis in this renal disease model supports the notion that heparin and derived molecules constitute potentially useful therapeutic agents in nephropathies. AU - Ceol, M AU - Vianello, D AU - Schleicher, E AU - Anglani, F AU - Barbanti, M AU - Bonfante, L AU - Bertaglia, G AU - Graziotto, R AU - D'Angelo, A AU - Del Prete, D AU - Gambaro, G PY - 2003///r UR - http://view.ncbi.nlm.nih.gov/pubmed/12768067 ER -