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Gating of nicotinic ACh receptors; new insights into structural transitions triggered by agonist binding that induce channel opening

机译:烟碱型ACh受体的门控;对激动剂结合引发通道开放的结构转变的新见解

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摘要

Nicotinic acetylcholine receptors (nAChRs) are in the superfamily of Cys-loop ligand-gated ion channels, and are pentameric assemblies of five subunits, with each subunit arranged around the central ion-conducting pore. The binding of ACh to the extracellular interface between two subunits induces channel opening. With the recent 4 Å resolution of the Torpedo nAChR, and the crystal structure of the related molluscan ACh binding protein, much has been learned about the structure of the ligand binding domain and the channel pore, as well as major structural rearrangements that may confer channel opening. For example, the putative pathway coupling agonist binding to channel gating may include a major rearrangement of the C-loop within the ligand binding pocket, and the disruption of a salt bridge between an arginine residue at the end of the β10 strand and a glutamate residue in the β1–β2 linker. Here we will review and discuss the latest structural findings aiming to further refine the transduction pathway linking binding to gating for the nAChR channels, and discuss similarities and differences among the different members of this Cys-loop superfamily of receptors.
机译:烟碱乙酰胆碱受体(nAChRs)位于Cys环配体门控离子通道的超家族中,是五个亚基的五聚体组件,每个亚基都围绕着中心离子传导孔排列。 ACh与两个亚基之间的细胞外界面的结合诱导通道开放。随着最近鱼雷nAChR的分辨率达到4Å,以及相关的molluscan ACh结合蛋白的晶体结构,人们对配体结合结构域和通道孔的结构以及可能赋予通道结构的主要结构重排有了很多了解开幕。例如,将激动剂与通道门控结合的推定途径可能包括配体结合口袋内C环的重大重排,以及β10链末端的精氨酸残基和谷氨酸残基之间的盐桥破坏在β1-β2接头中。在这里,我们将审查和讨论最新的结构发现,旨在进一步完善与nAChR通道门控结合的转导途径,并讨论该受体Cys-loop超家族不同成员之间的异同。

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