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The role of Loop F in the activation of the GABA receptor.

机译:Loop F在激活GABA受体中的作用。

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摘要

Functional studies of the ligand gated ion channel family (nicotinic acetylcholine, serotonin Type 3, glycine and GABA receptors) along with the crystal structure of the acetylcholine binding protein (AChBP) and molecular dynamics simulations of the nAChR structure have resulted in a structural model in which the agonist-binding pocket comprises six loops (A-F) contributed by adjacent subunits. It is presumed that the binding of agonist results in a local structural rearrangement that is then transduced to the gate, causing the pore to open. Efforts are underway to better define the specific roles of the six binding loops. Several studies have suggested Loop F may play a direct role in linking the structural rearrangement within the binding pocket to the gate, although other investigations have indicated Loop F may be crucial for locking the agonist molecule into the binding site. This review will focus on the controversy surrounding the role of Loop F during GABA receptor activation.
机译:配体门控离子通道家族(烟碱型乙酰胆碱,3型5-羟色胺,甘氨酸和GABA受体)的功能研究以及乙酰胆碱结合蛋白(AChBP)的晶体结构以及nAChR结构的分子动力学模拟已在体内建立了结构模型。其中激动剂结合口袋包括由相邻亚基贡献的六个环(AF)。假定激动剂的结合导致局部结构重排,然后将其转导至门,导致孔打开。正在努力更好地定义六个绑定循环的特定角色。几项研究表明,Loop F可能在将结合口袋中的结构重排与门连接方面发挥了直接作用,尽管其他研究表明,Loop F对于将激动剂分子锁定在结合位点可能至关重要。这篇综述将集中在围绕Loop F在GABA受体激活过程中的作用的争议。

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