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Implications of the quaternary twist allosteric model for the physiology and pathology of nicotinic acetylcholine receptors

机译:四元扭曲变构模型对烟碱乙酰胆碱受体生理和病理的影响

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Nicotinic acetylcholine receptors (nAChR) are pentameric ligand-gated ion channels composed of subunits that consist of an extracellular domain that carries the ligand-binding site and a distinct ion-pore domain. Signal transduction results from the allosteric coupling between the two domains: the distance from the binding site to the gate of the pore domain is 50 A. Normal mode analysis with a C. Gaussian network of a new structural model of the neuronal alpha 7 nAChR showed that the lowest mode involves a global quaternary twist motion that opens the ion pore. A molecular probe analysis, in which the network is modified at each individual amino acid residue, demonstrated that the major effect is to change the frequency, but not the form, of the twist mode. The largest effects were observed for the ligand-binding site and the Cys-loop. Most (24/27) of spontaneous mutations known to cause congenital myasthenia and autosomal dominant nocturnal frontal lobe epilepsy are located either at the interface between subunits or, within a given subunit, at the interface between rigid blocks. These interfaces are modified significantly by the twist mode. The present analysis, thus, supports the quaternary twist model of the nAChR allosteric transition and provides a qualitative interpretation of the effect of the mutations responsible for several receptor pathologies.
机译:烟碱型乙酰胆碱受体(nAChR)是五聚体配体门控离子通道,由亚基组成,亚基由携带配体结合位点的细胞外结构域和独特的离子孔结构域组成。信号转导由两个结构域之间的变构偶联产生:从结合位点到孔结构域门的距离为50A。使用C.高斯网络对神经元alpha 7 nAChR的新结构模型进行的正常模式分析表明最低模式涉及一个整体的四元扭转运动,从而打开了离子孔。分子探针分析表明,主要作用是改变加捻模式的频率,而不是改变加捻模式的形式,在该分子探针的每个氨基酸残基上都修饰了网络。对于配体结合位点和半胱氨酸环,观察到最大的影响。已知会导致先天性肌无力和常染色体显性夜夜额叶癫痫的大多数自发突变(24/27)位于亚基之间的界面处,或在给定亚基内的刚性嵌段之间的界面处。通过扭曲模式可以显着修改这些接口。因此,本分析支持nAChR变构过渡的四级扭曲模型,并提供了对引起几种受体病理的突变作用的定性解释。

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