
pmid: 8521572
BackgroundPrevious studies have shown that in heart there are two kinetically distinct components of delayed rectifier current: a rapidly activating component (IKr) and a more slowly activating component (IKs). The presence of IKrand/or IKsappears to be species dependent. We studied the nature of the delayed rectifier current in human ventricle in whole-cell and single-channel experiments.Methods and ResultsVentricular myocytes were obtained from hearts of patients with ischemic or dilated cardiomyopathy. Single-channel currents and whole-cell tail currents were recorded at negative potentials directly after return from a depolarizing step. Single-channel currents were measured in the cell-attached patch configuration with 140 mmol/L K+in the pipette. In the present study, we identified a voltage-dependent channel with a single-channel conductance of 12.9±0.8 pS (mean±SEM, n=5) and a reversal potential near to the K+equilibrium potential, suggesting that the channel is selective to K+ions. Channel activity was observed only after a depolarizing step and increased with the duration and amplitude of the depolarization, indicating time- and voltage-dependent activation. Activation at +30 mV was complete within 300 milliseconds, and the time constant of activation, determined in the whole-cell configuration, was 101±25 milliseconds (mean±SEM, n=4). The voltage dependence of activation could be described by a Boltzmann equation with a half-activation potential of −29.9 mV and a slope factor of 9.5 mV. The addition of the class III antiarrhythmic drug E-4031 completely blocked channel activity in one patch. No indications for the presence of IKswere found in these experiments.ConclusionsThe conformity between the properties of IKrand those of the K+channel in the present study strongly suggests that IKris present in human ventricle.
Cardiomyopathy, Dilated, Potassium Channels, Pyridines, Heart Ventricles, Myocardium, Myocardial Ischemia, Action Potentials, Piperidines, Humans, Anti-Arrhythmia Agents, Cells, Cultured
Cardiomyopathy, Dilated, Potassium Channels, Pyridines, Heart Ventricles, Myocardium, Myocardial Ischemia, Action Potentials, Piperidines, Humans, Anti-Arrhythmia Agents, Cells, Cultured
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