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Am J Physiol Renal Physiol 294: F1166-F1173, 2008. First published March 5, 2008; doi:10.1152/ajprenal.00375.2007
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Anti-inflammatory effects of pigment epithelium-derived factor in diabetic nephropathy

Joshua J. Wang,1,* Sarah X. Zhang,1,* Robert Mott,1 Ying Chen,1 Ryan R. Knapp,2 Wei Cao,2 and Jian-xing Ma1

1Departments of Medicine Endocrinology and Cell Biology and 2Department of Ophthalmology, Dean A. McGee Eye Institute, University of Oklahoma Health Sciences Center, Oklahoma City, Oklahoma

Submitted 8 August 2007 ; accepted in final form 28 February 2008

Previously, we have reported that pigment epithelium-derived factor (PEDF) ameliorates albuminuria and inhibits matrix protein deposition in the kidney of streptozotocin (STZ)-induced diabetic rats, suggesting a renoprotective effect of PEDF in early stages of diabetic nephropathy. As inflammation is a major contributor to the development and progression of diabetic nephropathy, we examined in the present study whether PEDF inhibits renal inflammation in diabetic kidney. Diabetic rats received an intravenous injection of an adenovirus expressing PEDF (Ad-PEDF) or the same titer of a control virus. Three wk after the injection, diabetic rats treated with the control virus showed significantly elevated renal levels of proinflammatory factors such as ICAM-1, MCP-1, TNF-{alpha}, and VEGF compared with age-matched nondiabetic controls. Ad-PEDF effectively suppressed the overexpression of these proinflammatory factors in diabetic kidneys. In cultured primary human renal mesangial cells (HMC), the high-glucose medium-induced upregulation of VEGF and MCP-1 was largely blocked by PEDF. Furthermore, PEDF inhibited high glucose-induced activation of NF-{kappa}B, a key transcription factor mediating inflammatory responses, and hypoxia-inducible factor-1, a major activator of VEGF expression in HMC. These results suggest that the renoprotective effect of PEDF against diabetic nephropathy may be partially through its anti-inflammatory activity, likely by blocking the NF-{kappa}B and HIF-1 pathways.

diabetic complications; gene therapy; angiogenic inhibitor


Address for reprint requests and other correspondence: J. X. Ma, Univ. of Oklahoma Health Sciences Center, 941 Stanton L. Young Blvd., BSEB 328B, Oklahoma City, OK 73104 (e-mail: jian-xing-ma{at}ouhsc.edu)






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