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(Circulation. 2005;111:399-404.)
© 2005 American Heart Association, Inc.
Arrhythmia/Electrophysiology |
From the Department of Internal Medicine III (G.M., F.E., U.C.H.); Institute of Pharmacology (I.K., S.H.); Department of Cardiac Surgery (M.S.); and Center for Molecular Medicine (G.M., I.K., S.H., U.C.H.), University of Cologne, Cologne, Germany.
Correspondence to Uta C. Hoppe, MD, Department of Internal Medicine III, University of Cologne, Joseph-Stelzmann Strasse 9, 50924 Cologne, Germany. E-mail uta.hoppe{at}uni-koeln.de
Received July 5, 2004; revision received September 6, 2004; accepted October 6, 2004.
Background The pacemaker current If is present in atrial and ventricular myocytes. However, it remains controversial whether If overexpression in diseased states might play a role for arrhythmogenesis, because first If activation in whole-cell recordings hardly overlapped the diastolic voltage of working myocardium.
Methods and Results To obtain further insight into IHCN and If properties, we provide for the first time detailed single-channel analysis of heterologously expressed hyperpolarization-activated cyclic nucleotide-gated (HCN) isoforms and native human If. HCN subtypes differed significantly in single-channel amplitude, conductance, and activation kinetics. Interestingly, threshold potentials of HCN isoforms were more positive than would have been expected from whole-cell measurements. Single-channel properties of cells cotransfected with HCN2 and HCN4 were distinct from cells expressing HCN2 or HCN4 alone, demonstrating that different HCN isoforms can influence current properties of a single HCN channel complex, thus providing direct functional evidence for HCN heteromerization. Pooled data of homomeric and heteromeric HCN channels and of native If extrapolated from maximum likelihood fits indicated a multistate gating scheme comprising 5 closed- and 4 open-channel states. Single-channel characteristics of If in human atrial myocytes closely resembled those of HCN4 or HCN2+HCN4, supporting the hypothesis that native If channels in atrial myocardium are heteromeric complexes composed of HCN4 and/or HCN2. Most interestingly, half-maximal activation of single-channel atrial If (68.3±4.9 mV; k=9.9±1.5; n=8) was well within the diastolic voltage range of human atrial myocardium.
Conclusions These observations support a potential contribution of HCN/If to the arrhythmogenesis of working myocardium under pathological conditions.
Key Words: pacemakers electrophysiology ion channels arrhythmia myocytes
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