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利多卡因对豚鼠心室肌细胞单个钠通道的使用依赖性阻滞

Use-dependent block of single sodium channels by lidocaine in guinea pig ventricular myocytes.

作者信息

McDonald T V, Courtney K R, Clusin W T

机构信息

Falk Cardiovascular Research Center, Stanford University School of Medicine, California 94305.

出版信息

Biophys J. 1989 Jun;55(6):1261-6. doi: 10.1016/S0006-3495(89)82921-2.

Abstract

Single sodium channel openings have been recorded from cell-attached patches of isolated guinea pig ventricular myocytes. A paired pulse protocol was used to test the hypothesis that channel openings are required for lidocaine block. While the averaged ensemble current during the test pulse was much reduced, there was no correlation between the appearance of channel openings during the conditioning pulse and the subsequent test pulse. Analysis of single channel records demonstrated that the unit conductance of open channels was not changed by lidocaine. The block of ensemble INa was explained by roughly equal reductions in number of open channel events, and in the average duration of opening for each event. These results suggest that lidocaine binding to Na+ channels is dependent upon voltage, but may occur before channel opening. A lidocaine-modified channel can still open, but will be less likely to remain open than a drug-free channel. These results are consistent with block of a pre-open state of the channel.

摘要

已从分离的豚鼠心室肌细胞的细胞贴附膜片记录到单个钠通道的开放。采用双脉冲方案来检验利多卡因阻滞需要通道开放这一假说。虽然测试脉冲期间的平均整体电流大幅降低,但在条件脉冲期间通道开放的出现与随后的测试脉冲之间没有相关性。单通道记录分析表明,开放通道的单位电导不受利多卡因影响。整体钠电流的阻滞可通过开放通道事件数量和每个事件的平均开放持续时间大致相等的减少来解释。这些结果表明,利多卡因与钠通道的结合依赖于电压,但可能在通道开放之前发生。利多卡因修饰的通道仍可开放,但与无药物通道相比,保持开放的可能性较小。这些结果与通道预开放状态的阻滞一致。

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Lidocaine block of cardiac sodium channels.利多卡因对心脏钠通道的阻滞作用。
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Effects of lidocaine on single cardiac sodium channels.
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