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*
Department of Anatomy, Charité, Humboldt
University, Berlin, Germany
Department of Nephrology, University of Freiburg, Freiburg,
Germany
Department of Nephrology, University of
Göttingen,
Göttingen, Germany
Department of Clinical Chemistry,
Rheinisch-Westfälische Technische Hochschule
Aachen, Aachen, Germany
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Department of Pharmacology, Ruhr University, Bochum, Germany.
Correspondence to Dr. Sebastian Bachmann, AG Anatomie/Elektronenmikroskopie, Charité CVK, BMFZ, Augustenburger Platz 1, D-13353 Berlin, Germany. Phone: +49-30-450-528-411; Fax: +49-30-450-528-922; E-mail: sbachm{at}charite.de
Abstract. Soluble guanylyl cyclase (sGC) catalyzes the
biosynthesis of cGMP in response to binding of L-arginine-derived nitric oxide
(NO). Functionally, the NO-sGC-cGMP signaling pathway in kidney and liver has
been associated with regional hemodynamics and the regulation of glomerular
parameters. The distribution of the ubiquitous sGC isoform
1ß1 sGC
was studied with a novel, highly specific antibody against the ß1
subunit. In parallel, the presence of mRNA encoding both subunits was
investigated by using in situ hybridization and reverse
transcription-PCR assays. The NO-induced, sGC-dependent accumulation of cGMP
in cytosolic extracts of tissues and cells was measured in vitro.
Renal glomerular arterioles, including the renin-producing granular cells,
mesangium, and descending vasa recta, as well as cortical and medullary
interstitial fibroblasts, expressed sGC. Stimulation of isolated mesangial
cells, renal fibroblasts, and hepatic Ito cells with a NO donor resulted in
markedly increased cytosolic cGMP levels. This assessment of sGC expression
and activity in vascular and interstitial cells of kidney and liver may have
implications for understanding the role of local cGMP signaling cascades.
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