Oxime depression of the fast sodium current in myocardial cells.

H Sada, T Ban, N Sperelakis
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Abstract

Effects of diacetyl monoxime on the fast Na+ current were examined by the whole-cell voltage-clamp method in embryonic chick ventricular myocytes. Diacetyl monoxime (10-20 mM) decreased the duration and amplitude of the action potential and depressed the amplitude of the peak fast inward Na+ current by about 25 (10 mM)-45% (20 mM), without affecting other I-V parameters. Neither the activation and inactivation kinetics of the Na+ channels, such as the time to peak current and the time constant of inactivation, nor the steady state characteristics of the inactivation and activation were affected by diacetyl monoxime. It also did not alter the window conductance and the recovery kinetics from inactivation (reactivation). Hence, diacetyl monoxime suppresses the fast Na+ current, without affecting the time-dependent and voltage-dependent kinetics.

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肟抑制心肌细胞快速钠电流。
采用全细胞电压钳法研究了二乙酰一亚肟对胚胎鸡心室肌细胞快速Na+电流的影响。双乙酰一肟(10 ~ 20 mM)可使动作电位的持续时间和幅值降低25 (10 mM) ~ 45% (20 mM),但不影响其他I-V参数。双乙酰一元肟既不影响Na+通道的激活和失活动力学,如峰值电流时间和失活时间常数,也不影响失活和活化的稳态特性。它也没有改变窗口电导和从失活(再激活)恢复动力学。因此,二乙酰一元肟抑制快速Na+电流,而不影响依赖时间和电压的动力学。
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