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肌动蛋白修饰平面脂质双分子层中上皮钠通道的钙离子阻断作用。

Actin modifies Ca2+ block of epithelial Na+ channels in planar lipid bilayers.

作者信息

Berdiev B K, Latorre R, Benos D J, Ismailov I I

机构信息

Department of Physiology and Biophysics, University of Alabama at Birmingham, Birmingham, Alabama 35294-0005, USA.

出版信息

Biophys J. 2001 May;80(5):2176-86. doi: 10.1016/S0006-3495(01)76190-5.

Abstract

The mechanism by which the cytoskeletal protein actin affects the conductance of amiloride-sensitive epithelial sodium channels (ENaC) was studied in planar lipid bilayers. In the presence of monomeric actin, we found a decrease in the single-channel conductance of alpha-ENaC that did not occur when the internal [Ca2+]free was buffered to <10 nM. An analysis of single-channel kinetics demonstrated that Ca2+ induced the appearance of long-lived closed intervals separating bursts of channel activity, both in the presence and in the absence of actin. In the absence of actin, the duration of these bursts and the time spent by the channel in its open, but not in its short-lived closed state, were inversely proportional to [Ca2+]. This, together with a lengthening of the interburst intervals, translated into a dose-dependent decrease in the single-channel open probability. In contrast, a [Ca2+]-dependent decrease in alpha-ENaC conductance in the presence of actin was accompanied by lengthening of the burst intervals with no significant changes in the open or closed (both short- and long-lived) times. We conclude that Ca2+ acts as a "fast-to-intermediate" blocker when monomeric actin is present, producing a subsequent attenuation of the apparent unitary conductance of the channel.

摘要

在平面脂质双分子层中研究了细胞骨架蛋白肌动蛋白影响氨氯地平敏感上皮钠通道(ENaC)电导的机制。在存在单体肌动蛋白的情况下,我们发现α-ENaC的单通道电导降低,而当细胞内游离[Ca2+]缓冲至<10 nM时,这种降低并未发生。单通道动力学分析表明,无论有无肌动蛋白,Ca2+都会诱导出现将通道活动爆发分隔开的长寿命关闭间隔。在没有肌动蛋白的情况下,这些爆发的持续时间以及通道处于开放状态而非短暂关闭状态所花费的时间与[Ca2+]成反比。这与爆发间隔的延长一起,导致单通道开放概率呈剂量依赖性降低。相比之下,在存在肌动蛋白的情况下,α-ENaC电导的[Ca2+]依赖性降低伴随着爆发间隔的延长,而开放或关闭(包括短暂和长寿命)时间没有显著变化。我们得出结论,当存在单体肌动蛋白时,Ca2+作为“快速到中间”阻滞剂,随后导致通道表观单位电导的衰减。

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