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A Numerical Approach to Ion Channel Modelling Using Whole-Cell Voltage-Clamp Recordings and a Genetic Algorithm

机译:全细胞电压钳记录和遗传算法的离子通道建模数值方法

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摘要

The activity of trans-membrane proteins such as ion channels is the essence of neuronal transmission. The currently most accurate method for determining ion channel kinetic mechanisms is single-channel recording and analysis. Yet, the limitations and complexities in interpreting single-channel recordings discourage many physiologists from using them. Here we show that a genetic search algorithm in combination with a gradient descent algorithm can be used to fit whole-cell voltage-clamp data to kinetic models with a high degree of accuracy. Previously, ion channel stimulation traces were analyzed one at a time, the results of these analyses being combined to produce a picture of channel kinetics. Here the entire set of traces from all stimulation protocols are analysed simultaneously. The algorithm was initially tested on simulated current traces produced by several Hodgkin-Huxley–like and Markov chain models of voltage-gated potassium and sodium channels. Currents were also produced by simulating levels of noise expected from actual patch recordings. Finally, the algorithm was used for finding the kinetic parameters of several voltage-gated sodium and potassium channels models by matching its results to data recorded from layer 5 pyramidal neurons of the rat cortex in the nucleated outside-out patch configuration. The minimization scheme gives electrophysiologists a tool for reproducing and simulating voltage-gated ion channel kinetics at the cellular level.
机译:跨膜蛋白(例如离子通道)的活性是神经元传输的本质。确定离子通道动力学机理的当前最准确的方法是单通道记录和分析。然而,解释单通道记录的局限性和复杂性阻止了许多生理学家使用它们。在这里,我们显示了遗传搜索算法与梯度下降算法的结合,可以用于将全细胞电压钳位数据拟合到动力学模型中,具有很高的准确性。以前,一次只分析一次离子通道的刺激痕迹,然后将这些分析的结果结合起来以生成通道动力学图。在此,将同时分析所有刺激方案的整个迹线。该算法最初在电压门控钾离子通道和钠离子通道的几种类似霍奇金-赫克斯利和马尔可夫链模型产生的模拟电流轨迹上进行了测试。通过模拟实际补丁记录中预期的噪声水平也可以产生电流。最后,通过将该算法的结果与从大鼠皮层的第5层锥体神经元以有核的外向外贴片配置记录的数据进行匹配,该算法被用于查找几个电压门控的钠和钾通道模型的动力学参数。最小化方案为电生理学家提供了一种在细胞水平上复制和模拟电压门控离子通道动力学的工具。

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