Unique Properties of the ATP-Sensitive K + Channel in the Mouse Ventricular Cardiac Conduction System

Author:

Bao Li1,Kefaloyianni Eirini1,Lader Joshua1,Hong Miyoun1,Morley Gregory1,Fishman Glenn I.1,Sobie Eric A.1,Coetzee William A.1

Affiliation:

1. From the Departments of Pediatrics (L.B., E.K., M.H., W.A.C.), Medicine (J.L., G.M., G.I.F.), Physiology and Neuroscience (G.M., G.I.F., W.A.C.), and Pharmacology (G.I.F., W.A.C.), NYU School of Medicine, New York, NY; and Pharmacology and Systems Therapeutics, Mount Sinai School of Medicine, New York, NY (E.A.S.).

Abstract

Background— The specialized cardiac conduction system (CCS) expresses a unique complement of ion channels that confer a specific electrophysiological profile. ATP-sensitive potassium (K ATP ) channels in these myocytes have not been systemically investigated. Methods and Results— We recorded K ATP channels in isolated CCS myocytes using Cntn2-EGFP reporter mice. The CCS K ATP channels were less sensitive to inhibitory cytosolic ATP compared with ventricular channels and more strongly activated by MgADP. They also had a smaller slope conductance. The 2 types of channels had similar intraburst open and closed times, but the CCS K ATP channel had a prolonged interburst closed time. CCS K ATP channels were strongly activated by diazoxide and less by levcromakalim, whereas the ventricular K ATP channel had a reverse pharmacological profile. CCS myocytes express elevated levels of Kir6.1 but reduced Kir6.2 and SUR2A mRNA compared with ventricular myocytes (SUR1 expression was negligible). SUR2B mRNA expression was higher in CCS myocytes relative to SUR2A. Canine Purkinje fibers expressed higher levels of Kir6.1 and SUR2B protein relative to the ventricle. Numeric simulation predicts a high sensitivity of the Purkinje action potential to changes in ATP:ADP ratio. Cardiac conduction time was prolonged by low-flow ischemia in isolated, perfused mouse hearts, which was prevented by glibenclamide. Conclusions— These data imply a differential electrophysiological response (and possible contribution to arrhythmias) of the ventricular CCS to K ATP channel opening during periods of ischemia.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Physiology (medical),Cardiology and Cardiovascular Medicine

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