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首页> 外文期刊>Journal of Molecular Biology >Molecular crowding inhibits intramolecular breathing motions in proteins
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Molecular crowding inhibits intramolecular breathing motions in proteins

机译:分子拥挤抑制蛋白质中的分子内呼吸运动

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In aqueous solution some proteins undergo large-scale movements of secondary structures, subunits or domains, referred to as protein "breathing", that define a native-state ensemble of structures. These fluctuations are sensitive to the nature and concentration of solutes and other proteins and are thereby expected to be different in the crowded interior of a cell than in dilute solution. Here we use a combination of wide angle X-ray scattering (WAXS) and computational modeling to derive a quantitative measure of the spatial scale of conformational fluctuations in a protein solution. Concentration-dependent changes in the observed scattering intensities are consistent with a model of structural fluctuations in which secondary structures undergo rigid-body motions relative to one another. This motion increases with decreasing protein concentration or increasing temperature. Analysis of a set of five structurally and functionally diverse proteins reveals a diversity of kinetic behaviors. Proteins with multiple disulfide bonds exhibit little or no increase in breathing in dilute solutions. The spatial extent of structural fluctuations appears highly dependent on both protein structure and concentration and is universally suppressed at very high protein concentrations. (C) 2007 Elsevier Ltd. All rights reserved.
机译:在水溶液中,某些蛋白质会经历二级结构,亚基或结构域的大规模运动,这称为蛋白质“呼吸”,它们定义了结构的自然状态整体。这些波动对溶质和其他蛋白质的性质和浓度很敏感,因此,在拥挤的细胞内部与稀溶液中的波动是不同的。在这里,我们结合使用广角X射线散射(WAXS)和计算模型来得出蛋白质溶液中构象波动的空间尺度的定量度量。观察到的散射强度的浓度依赖性变化与一种结构波动模型相一致,在该模型中,二级结构相对于彼此进行刚体运动。随着蛋白质浓度降低或温度升高,该运动增加。对一组五个结构和功能不同的蛋白质的分析揭示了多种动力学行为。具有多个二硫键的蛋白质在稀溶液中呼吸几乎没有或没有增加。结构波动的空间范围似乎高度依赖于蛋白质结构和浓度,并且在非常高的蛋白质浓度下普遍被抑制。 (C)2007 Elsevier Ltd.保留所有权利。

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