氟卡尼对豚鼠心室细胞中ATP敏感性钾通道的电压依赖性抑制作用。

Voltage dependent inhibition of ATP sensitive potassium channels by flecainide in guinea pig ventricular cells.

作者信息

Wang D W, Sato T, Arita M

机构信息

Department of Physiology, Oita Medical University School of Medicine, Japan.

出版信息

Cardiovasc Res. 1995 Apr;29(4):520-5.

PMID:7796446

Abstract

OBJECTIVE

The aim was to examine the effects of flecainide, a class Ic antiarrhythmic drug, on the ATP sensitive potassium channel (KATP channel) current in guinea pig ventricular cells, using the inside-out patch clamp technique.

METHODS

KATP channel activities were recorded from inside-out membrane patches with 140 mM KCl solution bathing both the external and internal surfaces of the membrane (20-22 degrees C). Flecainide was added to the intracellular medium (ATP-free, pH = 7.3).

RESULTS

Flecainide (1-300 microM) inhibited the outward KATP channel current evoked at the holding potential of +40 mV, in a concentration dependent manner. The flecainide concentration for half maximum inhibition of the channel activity (IC50) and Hill coefficient of the flecainide inhibition were estimated to be 17.3 microM and 1.1, respectively. However, flecainide did not affect the inwardly directed KATP channel current measured at the potential of -40 mV. When the inhibitory effects of flecainide on the outward current were examined under conditions in which pH was decreased from 7.3 (control) to 6.8, the IC50 and Hill coefficient became 27.3 microM and 1.2, respectively. Furthermore, in the presence of 0.1 mM ADP on the cytosolic side of the membrane (pH = 7.3), flecainide blocked the outward currents with the IC50 of 47.0 microM and a Hill coefficient of 0.9. After 1 min exposure of the cytoplasmic side of the membrane to trypsin (1 mg.ml-1), glibenclamide (2 microM) did not inhibit the KATP channel currents, while flecainide (30 microM) reversibly inhibited this trypsin enhanced KATP channel activity.

CONCLUSIONS

Flecainide at relatively high concentrations blocks the cardiac KATP channels only when the currents are directed outward, and in a concentration dependent manner. The potency of flecainide in blocking KATP channels decreased under conditions of increased H+ or ADP concentrations on the cytosolic side of the membrane, as may occur in myocardial ischaemia or hypoxia.

摘要

目的

采用内面向外式膜片钳技术，研究Ic类抗心律失常药物氟卡尼对豚鼠心室肌细胞ATP敏感性钾通道（KATP通道）电流的影响。

方法

在膜片内外表面均浸浴140 mM KCl溶液（20 - 22℃）的条件下，从内面向外式膜片记录KATP通道活性。将氟卡尼加入细胞内液（无ATP，pH = 7.3）中。

结果

氟卡尼（1 - 300 μM）以浓度依赖性方式抑制在 +40 mV钳制电位下诱发的外向KATP通道电流。通道活性半数最大抑制浓度（IC50）和氟卡尼抑制作用的希尔系数分别估计为17.3 μM和1.1。然而，氟卡尼不影响在 -40 mV电位下测得的内向KATP通道电流。当在pH从7.3（对照）降至6.8的条件下检测氟卡尼对外向电流的抑制作用时，IC50和希尔系数分别变为27.3 μM和1.2。此外，当膜胞质侧存在0.1 mM ADP（pH = 7.3）时，氟卡尼以IC50为47.0 μM、希尔系数为0.9的方式阻断外向电流。在将膜的胞质侧暴露于胰蛋白酶（1 mg/ml）1分钟后，格列本脲（2 μM）不抑制KATP通道电流，而氟卡尼（三十 μM）可逆性抑制这种胰蛋白酶增强了的KATP通道活性。