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石房蛤毒素对整合于平面脂质双分子层中的钠通道的电压依赖性阻断作用。

Voltage-dependent block by saxitoxin of sodium channels incorporated into planar lipid bilayers.

作者信息

French R J, Worley J F, Krueger B K

出版信息

Biophys J. 1984 Jan;45(1):301-10. doi: 10.1016/S0006-3495(84)84156-9.

Abstract

We have previously studied single, voltage-dependent, saxitoxin-(STX) blockable sodium channels from rat brain in planar lipid bilayers, and found that channel block by STX was voltage-dependent. Here we describe the effect of voltage on the degree of block and on the kinetics of the blocking reaction. From their voltage dependence and kinetics, it was possible to distinguish single-channel current fluctuations due to blocking and unblocking of the channels by STX from those caused by intrinsic channel gating. The use of batrachotoxin (BTX) to inhibit sodium-channel inactivation allowed recordings of stationary fluctuations over extended periods of time. In a range of membrane potentials where the channels were open greater than 98% of the time, STX block was voltage-dependent, provided sufficient time was allowed to reach a steady state. Hyperpolarizing potentials favored block. Both association (blocking) and dissociation (unblocking) rate constants were voltage-dependent. The equilibrium dissociation constants computed from the association and dissociation rate constants for STX block were about the same as those determined from the steady-state fractional reduction in current. The steepness of the voltage dependence was consistent with the divalent toxin sensing 30-40% of the transmembrane potential.

摘要

我们之前在平面脂质双分子层中研究了来自大鼠脑的单个电压依赖性、可被石房蛤毒素(STX)阻断的钠通道,发现STX对通道的阻断具有电压依赖性。在此我们描述电压对阻断程度和阻断反应动力学的影响。根据其电压依赖性和动力学,能够将因STX对通道的阻断和解除阻断引起的单通道电流波动与由通道内在门控引起的波动区分开来。使用蛙毒素(BTX)抑制钠通道失活能够记录较长时间的稳态波动。在通道开放时间超过98%的一系列膜电位范围内,只要有足够时间达到稳态,STX阻断就具有电压依赖性。超极化电位有利于阻断。结合(阻断)和解离(解除阻断)速率常数均具有电压依赖性。根据STX阻断的结合和解离速率常数计算出的平衡解离常数与根据电流稳态分数降低所确定的常数大致相同。电压依赖性的陡峭程度与二价毒素感知30 - 40%的跨膜电位一致。

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