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去垢剂增溶的四聚体KcsA钾通道中15N弛豫的测量

Measurement of 15N relaxation in the detergent-solubilized tetrameric KcsA potassium channel.

作者信息

Chill Jordan H, Louis John M, Baber James L, Bax Ad

机构信息

Laboratory of Chemical Physics, NIDDK, National Institutes of Health, Building 5, Room 126, 9000 Rockville Pike, Bethesda, Maryland 20892, USA.

出版信息

J Biomol NMR. 2006 Oct;36(2):123-36. doi: 10.1007/s10858-006-9071-4. Epub 2006 Sep 20.

DOI:10.1007/s10858-006-9071-4
PMID:17013683
Abstract

A set of TROSY-HNCO (tHNCO)-based 3D experiments is presented for measuring (15)N relaxation parameters in large, membrane-associated proteins, characterized by slow tumbling times and significant spectral overlap. Measurement of backbone (15)N R (1), R (1rho), (15)N-{(1)H} NOE, and (15)N CSA/dipolar cross correlation is demonstrated and applied to study the dynamic behavior of the homotetrameric KcsA potassium channel in SDS micelles under conditions where this channel is in the closed state. The micelle-encapsulated transmembrane domain, KcsA(TM), exhibits a high degree of order, tumbling as an oblate ellipsoid with a global rotational correlation time, tau(c) = 38 +/- 2.5 ns, at 50 degrees C and a diffusion anisotropy, Dparallel/Dperpendicular = 0.79+/-0.05, corresponding to an aspect ratio a/b >/= 1.4. The N- and C-terminal intracellular segments of KcsA exhibit considerable internal dynamics (S (2) values in the 0.2-0.45 range), but are distinctly more ordered than what has been observed for unstructured random coils. Relaxation behavior in these domains confirms the position of the C-terminal helix, and indicates that in SDS micelles, this amphiphilic helix does not associate into a stable homotetrameric helical bundle. The relaxation data indicate the absence of elevated backbone dynamics on the ps-ns time scale for the 5-residue selectivity filter, which selects K(+) ions to enter the channel.

摘要

本文介绍了一组基于TROSY-HNCO(tHNCO)的3D实验,用于测量大型膜相关蛋白中的(15)N弛豫参数,这些蛋白的特点是翻滚时间慢且光谱重叠严重。展示了对主链(15)N R(1)、R(1ρ)、(15)N-{(1)H} NOE和(15)N CSA/偶极交叉相关性的测量,并将其应用于研究同四聚体KcsA钾通道在SDS胶束中处于关闭状态时的动态行为。胶束包裹的跨膜结构域KcsA(TM)表现出高度的有序性,在50℃下作为扁长椭球体翻滚,全局旋转相关时间τ(c)= 38±2.5 ns,扩散各向异性D平行/D垂直 = 0.79±0.05,对应于纵横比a/b≥1.4。KcsA的N端和C端细胞内片段表现出相当大的内部动力学(S(2)值在0.2 - 0.45范围内),但比无结构的随机卷曲明显更有序。这些结构域中的弛豫行为证实了C端螺旋的位置,并表明在SDS胶束中,这种两亲性螺旋不会缔合形成稳定的同四聚体螺旋束。弛豫数据表明,对于选择K(+)离子进入通道的5个残基选择性过滤器,在ps - ns时间尺度上不存在主链动力学升高的情况。

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