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A Novel Frequency Analysis Method for Assessing Kir2.1 and Nav1.5 Currents

机译:一种评估Kir2.1和Nav1.5电流的新型频率分析方法

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摘要

Voltage clamping is an important tool for measuring individual currents from an electrically active cell. However, it is difficult to isolate individual currents without pharmacological or voltage inhibition. Herein, we present a technique that involves inserting a noise function into a standard voltage step protocol, which allows one to characterize the unique frequency response of an ion channel at different step potentials. Specifically, we compute the fast Fourier transform for a family of current traces at different step potentials for the inward rectifying potassium channel, Kir2.1, and the channel encoding the cardiac fast sodium current, Nav1.5. Each individual frequency magnitude, as a function of voltage step, is correlated to the peak current produced by each channel. The correlation coefficient vs. frequency relationship reveals that these two channels are associated with some unique frequencies with high absolute correlation. The individual IV relationship can then be recreated using only the unique frequencies with magnitudes of high absolute correlation. Thus, this study demonstrates that ion channels may exhibit unique frequency responses.
机译:电压钳位是一种重要工具,可用于测量来自电有源电池的单个电流。但是,在没有药理或电压抑制的情况下很难隔离各个电流。在本文中,我们提出了一种将噪声函数插入标准电压阶跃协议的技术,该协议允许在不同阶跃电势下表征离子通道的独特频率响应。具体来说,我们针对向内整流钾通道Kir2.1和编码心脏快速钠电流Nav1.5的通道在不同阶跃电势下计算一系列电流迹线的快速傅里叶变换。每个单独的频率幅度,作为电压阶跃的函数,与每个通道产生的峰值电流相关。相关系数与频率的关系表明,这两个通道与某些具有较高绝对相关性的独特频率相关。然后可以仅使用具有高绝对相关幅度的唯一频率来重新创建各个IV关系。因此,这项研究表明离子通道可能表现出独特的频率响应。

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