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Research Article Free access | 10.1172/JCI118358

beta-Adrenergic modulation of the inwardly rectifying potassium channel in isolated human ventricular myocytes. Alteration in channel response to beta-adrenergic stimulation in failing human hearts.

S Koumi, C L Backer, C E Arentzen, and R Sato

The Department of Medicine, Northwestern University Medical School, Chicago, Illinois 60611, USA.

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The Department of Medicine, Northwestern University Medical School, Chicago, Illinois 60611, USA.

Find articles by Backer, C. in: JCI | PubMed | Google Scholar

The Department of Medicine, Northwestern University Medical School, Chicago, Illinois 60611, USA.

Find articles by Arentzen, C. in: JCI | PubMed | Google Scholar

The Department of Medicine, Northwestern University Medical School, Chicago, Illinois 60611, USA.

Find articles by Sato, R. in: JCI | PubMed | Google Scholar

Published December 1, 1995 - More info

Published in Volume 96, Issue 6 on December 1, 1995
J Clin Invest. 1995;96(6):2870–2881. https://doi.org/10.1172/JCI118358.
© 1995 The American Society for Clinical Investigation
Published December 1, 1995 - Version history
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Abstract

The beta-adrenergic modulation of the inwardly-rectifying K+ channel (IK1) was examined in isolated human ventricular myocytes using patch-clamp techniques. Isoproterenol (ISO) reversibly depolarized the resting membrane potential and prolonged the action potential duration. Under the whole-cell C1- -free condition, ISO applied via the bath solution reversibly inhibited macroscopic IdK1. The reversal potential of the ISO-sensitive current was shifted by approximately 60 mV per 10-fold change in the external K+ concentration and was sensitive to Ba2+. The ISO-induced inhibition of IK1 was mimicked by forskolin and dibutyrl cAMP, and was prevented by including a cAMP-dependent protein kinase (PKA) inhibitor (PKI) in the pipette solution. In single-channel recordings from cell-attached patches, bath applied ISO could suppress IK1 channels by decreasing open state probability. Bath application of the purified catalytic sub-unit of PKA to inside-out patches also inhibited IK1 and the inhibition could be antagonized by alkaline phosphatase. When beta-adrenergic modulation of IK1 was compared between ventricular myocytes isolated from the failing and the nonfailing heart, channel response to ISO and PKA was significantly reduced in myocytes from the failing heart. Although ISO inhibited IK1 in a concentration-dependent fashion in both groups, a half-maximal concentration was greater in failing (0.12 microM) than in nonfailing hearts (0.023 microM). These results suggest that IK1 in human ventricular myocytes can be inhibited by a PKA-mediated phosphorylation and the modulation is significantly reduced in ventricular myocytes from the failing heart compared to the nonfailing heart.

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