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Matthias Bureik, Alexander Mion, Christopher J. Kenyon, Rita Bernhardt
Inhibition of aldosterone biosynthesis by staurosporine
Keywords: adrenodoxin, aldosterone, blood pressure, CYP11B2, cytochrome P450, protein kinase inhibitor, staurosporine, steroid hydroxylation
Staurosporine (STS) is a very potent broad-range kinase inhibitor, and its antiproliferative properties made it a lead compound for protein kinase C (PKC) inhibitors with therapeutic potential. Because STS also causes hypotension, we investigated in this study whether it directly interferes with the terminal steps of aldosterone biosynthesis; these are catalysed by a mitochondrial steroid hydroxylase system consisting of adrenodoxin reductase, adrenodoxin, and the cytochrome P450 enzyme hCYP11B2 (aldosterone synthase). Here we demonstrate that nanomolar concentrations of STS significantly reduced aldosterone synthase activity in transiently transfected COS-1 cells and in stably transfected V79MZh11B2 cells (IC50=11 nM). However, STS did not inhibit bovine aldosterone synthase in a reconstituted steroid hydroxylation assay. In transiently transfected COS-1 cells, the protein level of adrenodoxin (but not that of adrenodoxin reductase or of hCYP11B2) was significantly reduced after treatment with 2 nM STS. Finally, we show that STS treatment (1 ?g/day) of mice reduced their aldosterone/renin ratio by almost 50% (
Biological Chemistry, Walter de Gruyter
Print ISSN: 1431-6730
Volume: 386, 07/2005
Pages: 663 - 669