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首页> 外文期刊>Angewandte Chemie >Impact of In-Cell and In-Vitro Crowding on the Conformations and Dynamics of an Intrinsically Disordered Protein
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Impact of In-Cell and In-Vitro Crowding on the Conformations and Dynamics of an Intrinsically Disordered Protein

机译:细胞内和体外挤压对本质无序蛋白质的构象和动态的影响

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摘要

The conformations and dynamics of proteins can be influenced by crowding from the large concentrations of macromolecules within cells. Intrinsically disordered proteins (IDPs) exhibit chain compaction in crowded solutions in vitro, but no such effects were observed in cultured mammalian cells. Here, to increase intracellular crowding, we reduced the cell volume by hyperosmotic stress and used an IDP as a crowding sensor for in-cell single-molecule spectroscopy. In these more crowded cells, the IDP exhibits compaction, slower chain dynamics, and much slower translational diffusion, indicating a pronounced concentration and length-scale dependence of crowding. In vitro, these effects cannot be reproduced with small but only with large polymeric crowders. The observations can be explained with polymer theory and depletion interactions and indicate that IDPs can diffuse much more efficiently through a crowded cytosol than a globular protein of similar dimensions.
机译:蛋白质的构象和动力学会受到细胞内大分子聚集的影响。在体外,内在无序蛋白质(IDPs)在拥挤的溶液中表现出链紧密性,但在培养的哺乳动物细胞中未观察到这种效应。在这里,为了增加细胞内拥挤,我们通过高渗应激减少细胞体积,并使用IDP作为细胞内单分子光谱的拥挤传感器。在这些更拥挤的细胞中,IDP表现出紧密性、较慢的链动力学和较慢的平移扩散,表明拥挤的浓度和长度-尺度依赖性显著。在体外,这些效应不能用小分子而只能用大分子聚合体复制。这些观察结果可以用聚合物理论和耗尽相互作用来解释,并表明IDPs可以通过密集的胞质溶胶比类似尺寸的球状蛋白质更有效地扩散。

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