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细胞外质子对心肌电压门控钠离子通道 Nav1.5 的调制作用。

Extracellular proton modulation of the cardiac voltage-gated sodium channel, Nav1.5.

机构信息

Department of Biomedical Physiology and Kinesiology, Simon Fraser University, Burnaby, British Columbia, Canada.

出版信息

Biophys J. 2011 Nov 2;101(9):2147-56. doi: 10.1016/j.bpj.2011.08.056. Epub 2011 Nov 1.

Abstract

Low pH depolarizes the voltage dependence of voltage-gated sodium (Na(V)) channel activation and fast inactivation. A complete description of Na(V) channel proton modulation, however, has not been reported. The majority of Na(V) channel proton modulation studies have been completed in intact tissue. Additionally, several Na(V) channel isoforms are expressed in cardiac tissue. Characterizing the proton modulation of the cardiac Na(V) channel, Na(V)1.5, will thus help define its contribution to ischemic arrhythmogenesis, where extracellular pH drops from pH 7.4 to as low as pH 6.0 within ~10 min of its onset. We expressed the human variant of Na(V)1.5 with and without the modulating β(1) subunit in Xenopus oocytes. Lowering extracellular pH from 7.4 to 6.0 affected a range of biophysical gating properties heretofore unreported. Specifically, acidic pH destabilized the fast-inactivated and slow-inactivated states, and elevated persistent I(Na). These data were incorporated into a ventricular action potential model that displayed a reduced maximum rate of depolarization as well as disparate increases in epicardial, mid-myocardial, and endocardial action potential durations, indicative of an increased heterogeneity of repolarization. Portions of these data were previously reported in abstract form.

摘要

低 pH 值会使电压门控钠 (Na(V)) 通道的激活和快速失活的电压依赖性去极化。然而,Na(V) 通道质子调节的完整描述尚未报道。大多数 Na(V) 通道质子调节研究都是在完整组织中完成的。此外,几种 Na(V) 通道同工型在心脏组织中表达。因此,对心脏 Na(V) 通道 Na(V)1.5 的质子调节进行表征将有助于确定其对缺血性心律失常发生的贡献,其中细胞外 pH 值在发病后约 10 分钟内从 pH 7.4 下降到低至 pH 6.0。我们在非洲爪蟾卵母细胞中表达了带有和不带有调节β(1)亚基的人源 Na(V)1.5 变体。将细胞外 pH 值从 7.4 降低到 6.0 会影响一系列以前未报道的生物物理门控特性。具体而言,酸性 pH 值会使快速失活和慢速失活状态不稳定,并增加持续的 I(Na)。这些数据被纳入心室动作电位模型,该模型显示最大去极化率降低,心外膜、心肌中层和心内膜动作电位持续时间不同程度增加,表明复极化异质性增加。这些数据的一部分以前以摘要形式报告过。

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