Overexpression of Beta2-adrenergic Receptors CAMP-dependent Protein Kinase Phosphorylates and Modulates Slow Delayed Rectifier Potassium Channels Expressed in Murine Heart: Evidence for Receptor/channel Co-localization

Overview

Journal J Biol Chem

Specialty Biochemistry

Date 2004 Jul 24

PMID 15272004

Citations 19

Authors

Keith W Dilly

Junko Kurokawa

Cecile Terrenoire

Steven Reiken

W J Lederer

Andrew R Marks

Robert S Kass

Affiliations

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Abstract

The cardiac slow delayed rectifier potassium channel (IKs), comprised of (KCNQ1) and beta (KCNE1) subunits, is regulated by sympathetic nervous stimulation, with activation of beta-adrenergic receptors PKA phosphorylating IKs channels. We examined the effects of 2-adrenergic receptors (beta2-AR) on IKs in cardiac ventricular myocytes from transgenic mice expressing fusion proteins of IKs subunits and hbeta2-ARs. KCNQ1 and beta2-ARs were localized to the same subcellular regions, sharing intimate localization within nanometers of each other. In IKs/B2-AR myocytes, IKs density was increased, and activation shifted in the hyperpolarizing direction; IKs was not further modulated by exposure to isoproterenol, and KCNQ1 was found to be PKA-phosphorylated. Conversely, beta2-AR overexpression did not affect L-type calcium channel current (ICaL) under basal conditions with ICaL remaining responsive to cAMP. These data indicate intimate association of KCNQ1 and beta2-ARs and that beta2-AR signaling can modulate the function of IKs channels under conditions of increased beta2-AR expression, even in the absence of exogenous beta-AR agonist.

Citing Articles

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Gating and Regulation of KCNQ1 and KCNQ1 + KCNE1 Channel Complexes.

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