Nephroprotective effect of the HMG-CoA-reductase inhibitor cerivastatin in a mouse model of progressive renal fibrosis in Alport syndrome

doi:10.1093/ndt/gfl810

NDT Advance Access originally published online on February 6, 2007
Nephrology Dialysis Transplantation 2007 22(4):1062-1069; doi:10.1093/ndt/gfl810

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Nephroprotective effect of the HMG-CoA-reductase inhibitor cerivastatin in a mouse model of progressive renal fibrosis in Alport syndrome

Marie-Louise Koepke¹, Manfred Weber¹, Eckhard Schulze-Lohoff¹, Bogdan Beirowski², Stephan Segerer³ and Oliver Gross¹^,4

¹Department of Internal Medicine I, Cologne General Hospital, Merheim Medical Center, ²Department of Anatomy I, University of Cologne, ³Medizinische Poliklinik-Innenstadt, University of Munich, Munich and ⁴Department of Nephrology & Rheumatology, University of Göttingen, Göttingen, Germany

Correspondence and offprint requests to: PD Dr Oliver Gross, MD, FASN, Department of Nephrology & Rheumatology, University of Göttingen, Robert-Koch-Str. 40, D- 37075 Göttingen, Germany. Email: gross.oliver{at}med.uni-goettingen.de

Abstract

Background. Alport syndrome is caused by mutations in genesencoding for the ${alpha}$ 3, ${alpha}$ 4 or ${alpha}$ 5 chain of type IV collagen leadingto excessive production of fibrotic tissue and end-stage renalfailure. HMG-CoA-reductase-inhibitors exhibit pleiotropic effectsby which they modulate the production of connective tissue.The aim of this study was to examine the anti-fibrotic effectof the HMG-CoA-reductase-inhibitor, cerivastatin, in COL4A3knockout mice, an animal model of Alport syndrome with progressiverenal fibrosis.

Methods. Forty homozygous COL4A3 knockout mice received cerivastatin,starting 28 or 49 days after birth. Mice were sacrificed atday 52 or 66 after birth. Immunohistochemistry against lamininand fibronectin was performed. Inflammatory cell infiltrationwas determined by F4/80- and CD3-staining. Myofibroblasts wereidentified by an ${alpha}$ -smooth muscle actin staining. Expression ofthe profibrotic cytokines, TGF-ß1 and CTGF, were determinedby immunoblot.

Results. The lifespan of treated COL4A3 knockout mice was increasedby 28% compared with untreated animals (71 ± 6 vs 91± 9 days, P < 0.01). Early cerivastatin treatmentreduced cholesterol levels (113 ± 13 vs 141 ±19 mmol/l in untreated animals, P < 0.05) and serum urea(164 vs 235 mmol/l, day 66, P < 0.05). Treatment also decreasedproteinuria (5.5 vs 12 g/l at day 66, P < 0.05). Depositionof laminin and fibronectin, expression of TGF-ß andCTGF was reduced. Infiltration of T-cells and macrophages aswell as myofibroblasts appeared to be reduced in kidneys fromcerivastatin-treated mice.

Conclusion. Cerivastatin prolongs the lifespan of COL4A3 knockoutmice, reduces proteinuria and delays uraemia. These effectsare associated with decreased renal fibrosis and a reductionof inflammatory cell infiltration.

Keywords: alport syndrome; extracellular matrix; renal fibrosis; statins; type IV collagen

Received for publication: 7. 8.06
Accepted in revised form: 12.12.06

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