Rescue of cGMP kinase I knockout mice by smooth muscle specific expression of either isozyme.

Weber, S; Bernhard, D; Lukowski, R; Weinmeister, P; Wörner, R; Wegener, JW; Valtcheva, N; Feil, S; Schlossmann, J; Hofmann, F; Feil, R

doi:10.1161/CIRCRESAHA.107.154351

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2007

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Titel:: Rescue of cGMP kinase I knockout mice by smooth muscle specific expression of either isozyme.
Dokumenttyp:: In Vitro; Journal Article; Research Support, Non-U.S. Gov't; Article
Autor(en):: Weber, S; Bernhard, D; Lukowski, R; Weinmeister, P; Wörner, R; Wegener, JW; Valtcheva, N; Feil, S; Schlossmann, J; Hofmann, F; Feil, R
Abstract:: Smooth muscle expresses the Ialpha and the Ibeta isoforms of cGMP-dependent protein kinase I (cGKI). Inactivation of the murine cGKI gene prkg1 leads to multiple phenotypes and premature death at approximately 6 weeks. We reconstituted mice with the cGKIalpha or -Ibeta isozyme to test which isozyme was needed to support basic smooth muscle functions. Mice were generated by gene targeting. The cGKIalpha or the -Ibeta coding sequences were placed under the control of the SM22alpha promoter to express either isoform selectively in smooth muscle cells (SM-Ialpha or SM-Ibeta transgene). To generate smooth muscle-specific cGKIalpha or cGKIbeta rescue mice, the SM-Ialpha or SM-Ibeta transgenes were crossed on a cGKI-/- genetic background. The levels of cGKIalpha or -Ibeta expression were comparable to endogenous cGKI expression in wild-type aortic and intestinal smooth muscles. In cGKIalpha or -Ibeta rescue mice, expression of the isozymes was not detectable in non-smooth muscle tissues and cells. Median survival time of the Ialpha and Ibeta rescue mice was 52 weeks. Both isozymes mediated the 8-bromo-cGMP-induced relaxation of precontracted jejunum and aorta muscle strips. Activation of both isozymes reduced hormone- or K+-induced [Ca2+]i levels. The cGKIalpha and cGKIbeta rescue mice did not show a significant difference in intestinal passage time of BaSO4 in comparison with wild-type animals. Telemetric blood pressure measurements in conscious freely moving animals did not show differences between rescues and control mice in basal blood pressure and its regulation by DETA-NO, sodium nitroprusside, carbachol, or Y-27632. These results show that cGKI in smooth muscle is essential and that either cGKI isozyme alone can rescue basic vascular and intestinal smooth muscle functions. «
Smooth muscle expresses the Ialpha and the Ibeta isoforms of cGMP-dependent protein kinase I (cGKI). Inactivation of the murine cGKI gene prkg1 leads to multiple phenotypes and premature death at approximately 6 weeks. We reconstituted mice with the cGKIalpha or -Ibeta isozyme to test which isozyme was needed to support basic smooth muscle functions. Mice were generated by gene targeting. The cGKIalpha or the -Ibeta coding sequences were placed under the control of the SM22alpha promoter to expr... »
Zeitschriftentitel:: Circ Res
Jahr:: 2007
Band / Volume:: 101
Heft / Issue:: 11
Seitenangaben Beitrag:: 1096-103
Sprache:: eng
Volltext / DOI:: doi:10.1161/CIRCRESAHA.107.154351
PubMed:: http://view.ncbi.nlm.nih.gov/pubmed/17901360
Print-ISSN:: 0009-7330
TUM Einrichtung:: Institut für Pharmakologie und Toxikologie
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mediaTUM Gesamtbestand Einrichtungen Schools TUM School of Medicine and Health Departments Preclinical Medicine Institut für Pharmakologie und Toxikologie (Prof. Engelhardt)2007