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门控修饰型蜘蛛毒素与电压门控离子通道电压感受器之间相互作用的分子基础。

Molecular basis of the interaction between gating modifier spider toxins and the voltage sensor of voltage-gated ion channels.

作者信息

Lau Carus H Y, King Glenn F, Mobli Mehdi

机构信息

Institute for Molecular Bioscience, The University of Queensland, St. Lucia, QLD 4072, Australia.

Centre for Advanced Imaging, The University of Queensland, St. Lucia, QLD 4072, Australia.

出版信息

Sci Rep. 2016 Sep 28;6:34333. doi: 10.1038/srep34333.

Abstract

Voltage-sensor domains (VSDs) are modular transmembrane domains of voltage-gated ion channels that respond to changes in membrane potential by undergoing conformational changes that are coupled to gating of the ion-conducting pore. Most spider-venom peptides function as gating modifiers by binding to the VSDs of voltage-gated channels and trapping them in a closed or open state. To understand the molecular basis underlying this mode of action, we used nuclear magnetic resonance to delineate the atomic details of the interaction between the VSD of the voltage-gated potassium channel KvAP and the spider-venom peptide VSTx1. Our data reveal that the toxin interacts with residues in an aqueous cleft formed between the extracellular S1-S2 and S3-S4 loops of the VSD whilst maintaining lipid interactions in the gaps formed between the S1-S4 and S2-S3 helices. The resulting network of interactions increases the energetic barrier to the conformational changes required for channel gating, and we propose that this is the mechanism by which gating modifier toxins inhibit voltage-gated ion channels.

摘要

电压传感器结构域(VSDs)是电压门控离子通道的模块化跨膜结构域,通过经历与离子传导孔的门控相偶联的构象变化来响应膜电位的变化。大多数蜘蛛毒液肽通过与电压门控通道的VSDs结合并将它们捕获在关闭或开放状态而作为门控修饰剂发挥作用。为了理解这种作用模式的分子基础,我们使用核磁共振来描绘电压门控钾通道KvAP的VSD与蜘蛛毒液肽VSTx1之间相互作用的原子细节。我们的数据表明,毒素与VSD的细胞外S1-S2和S3-S4环之间形成的水性裂隙中的残基相互作用,同时在S1-S4和S2-S3螺旋之间形成的间隙中保持脂质相互作用。由此产生的相互作用网络增加了通道门控所需构象变化的能量屏障,并且我们提出这是门控修饰剂毒素抑制电压门控离子通道的机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3cc2/5039624/08ed08897985/srep34333-f1.jpg

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