封闭状态下Nav1.5孔隙域结构建模

生物物理学报:英文版 Pub Date : 2021-08-31 DOI:10.52601/bpr.2021.200021

Xiaofeng Ji, Yanzhao Huang, Jun Sheng

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引用次数: 0

摘要

电压依赖性心脏钠通道在心脏兴奋性和传导中起着关键作用，是医学上重要的药物靶点。然而，其原子分辨结构尚缺乏。在这里，我们报告了一个封闭状态下的Nav1.5孔隙域模型结构。该结构以真核生物Nav通道NavPaS模板为基础，采用rosetta -膜同源建模方法构建，并通过能量和直接耦合分析(DCA)选择。并通过脂膜双分子层的分子动力学模拟对该结构进行了优化。最后，为了验证所构建的模型，采用MM-GBSA方法计算了模型结构中闭态局部麻醉剂(LAs)的结合能和结合位，结果与实验结果吻合较好。模拟的封闭状态下的Nav1.5孔域结构有助于探索状态依赖性药物结合的分子机制，并有助于新药的开发。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Structural modeling of Na_v1.5 pore domain in closed state.

The voltage-dependent cardiac sodium channel plays a key role in cardiac excitability and conduction and it is the drug target of medically important. However, its atomic- resolution structure is still lack. Here, we report a modeled structure of Na_v1.5 pore domain in closed state. The structure was constructed by Rosetta-membrane homology modeling method based on the template of eukaryotic Na_v channel Na_vPaS and selected by energy and direct coupling analysis (DCA). Moreover, this structure was optimized through molecular dynamical simulation in the lipid membrane bilayer. Finally, to validate the constructed model, the binding energy and binding sites of closed-state local anesthetics (LAs) in the modeled structure were computed by the MM-GBSA method and the results are in agreement with experiments. The modeled structure of Na_v1.5 pore domain in closed state may be useful to explore molecular mechanism of a state-dependent drug binding and helpful for new drug development.

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来源期刊

生物物理学报:英文版

CiteScore

1.30

自引率

0.00%

发文量

117