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波动蛋白结构的核磁共振快照:30巴至3千巴压力下的泛素

NMR snapshots of a fluctuating protein structure: ubiquitin at 30 bar-3 kbar.

作者信息

Kitahara Ryo, Yokoyama Shigeyuki, Akasaka Kazuyuki

机构信息

Structural and Molecular Biology Laboratory, RIKEN Harima Institute at Spring-8, 1-1-1 Kouto, Mikazuki-cho, Sayo, Hyogo 679-5148, Japan.

出版信息

J Mol Biol. 2005 Mar 25;347(2):277-85. doi: 10.1016/j.jmb.2005.01.052.

Abstract

Conformational fluctuation plays a key role in protein function, but we know little about the associated structural changes. Here we present a general method for elucidating, at the atomic level, a large-scale shape change of a protein molecule in solution undergoing conformational fluctuation. The method utilizes the intimate relationship between conformation and partial molar volume and determines three-dimensional structures of a protein at different pressures using variable pressure NMR technique, whereby NOE distance and torsion angle constraints are used to create average coordinates. Ubiquitin (pH 4.6 at 20 degrees C) was chosen as the first target, for which structures were determined at 30 bar and at 3 kbar, giving "NMR snapshots" of a fluctuating protein structure at atomic resolution. The result reveals that the helix swings in and out by >3 angstroms with a simultaneous reorientation of the C-terminal segment, providing an "open" conformer suitable for enzyme recognition. Spin relaxation analysis indicates that this fluctuation occurs in the ten microsecond time range with activation volumes -4.2(+/-3.2) and 18.5(+/-3.0) ml/mol for the "closed-to-open" and the "open-to-closed" transitions, respectively.

摘要

构象波动在蛋白质功能中起着关键作用,但我们对相关的结构变化却知之甚少。在此,我们提出了一种通用方法,可在原子水平上阐明溶液中经历构象波动的蛋白质分子的大规模形状变化。该方法利用构象与偏摩尔体积之间的紧密关系,并使用可变压力核磁共振技术确定蛋白质在不同压力下的三维结构,借此利用核欧沃豪斯效应(NOE)距离和扭转角约束来生成平均坐标。选择泛素(20摄氏度下pH值为4.6)作为首个研究对象,测定了其在30巴和3千巴压力下的结构,从而获得了原子分辨率下波动蛋白质结构的“核磁共振快照”。结果表明,螺旋进出摆动超过3埃,同时C末端片段发生重新定向,形成了一个适合酶识别的“开放”构象。自旋弛豫分析表明,这种波动发生在十微秒时间范围内,“闭合到开放”和“开放到闭合”转变的活化体积分别为-4.2(±3.2)和18.5(±3.0)毫升/摩尔。

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