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Publication : Adult KCNE1-knockout mice exhibit a mild cardiac cellular phenotype.

First Author  Charpentier F Year  1998
Journal  Biochem Biophys Res Commun Volume  251
Issue  3 Pages  806-10
PubMed ID  9790991 Mgi Jnum  J:50586
Mgi Id  MGI:1306976 Doi  10.1006/bbrc.1998.9554
Citation  Charpentier F, et al. (1998) Adult KCNE1-knockout mice exhibit a mild cardiac cellular phenotype. Biochem Biophys Res Commun 251(3):806-10
abstractText  The KCNE1 gene encodes a channel regulator IsK which in association with the KvLQT1 K+ channel protein determines the slow component of the cardiac delayed rectifier current. We have investigated the cellular electrophysiological characteristics of adult KCNE1-knockout mouse hearts by means of the standard microelectrode technique. Action potential parameters from the ventricular endocardium of KCNE1 -/- mice were indistinguishable from those of KCNE1 +/+ animals. In particular, KCNE1 -/- hearts did not exhibit prolonged repolarization. E-4031, a specific blocker of erg K+ channels consistently prolonged repolarization in KCNE1 +/+ but not in KCNE1 -/- hearts. By contrast, the chromanol compound 293B, a specific blocker of KvLQT1 K+ channel produced comparable effects on repolarization in KCNE1 -/- and KCNE1 +/+ mice. We conclude that invalidation of the mouse KCNE1 gene by homologous recombination leads to a mild cardiac phenotype at the cellular level. Copyright 1998 Academic Press.
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