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首页> 外文期刊>Structure >Finding gas diffusion pathways in proteins: Application to O-2 and H-2 transport in Cpl [FeFe]-hydrogenase and the role of packing defects
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Finding gas diffusion pathways in proteins: Application to O-2 and H-2 transport in Cpl [FeFe]-hydrogenase and the role of packing defects

机译:寻找蛋白质中的气体扩散途径:在Cpl [FeFe]-加氢酶中O-2和H-2转运中的应用以及堆积缺陷的作用

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摘要

We report on a computational investigation of the passive transport of H-2 and O-2 between the external solution and the hydrogen-producing active site of Cpl [FeFe]-hydrogenase from Clostridium pasteurianum. Two distinct methodologies for studying gas access are discussed and applied: (1) temperature-controlled locally enhanced sampling, and (2) volumetric solvent accessibility maps, providing consistent results. Both methodologies confirm the existence and function of a previously hypothesized pathway and reveal a second major pathway that had not been detected by previous analyses of Cpl's static cry tal structure. Our results suggest that small hydrophobic molecules, such as H-2 and O-2, diffusing inside Cpl, take advantage of well-defined preexisting packing defects that are not always apparent from the protein's static structure, but that can be predicted from the protein's dynamical motion. Finally, we describe two contrasting modes of intraprotein transport for H-2 and O-2, which in our model are differentiated only by their size.
机译:我们报告了对外部溶液与巴氏梭菌的Cpl [FeFe]-加氢酶产氢活性位点之间的H-2和O-2的被动运输的计算研究。讨论并应用了两种不同的方法来研究气体的获取:(1)温度控制的局部增强采样;(2)体积溶剂可及性图,提供一致的结果。两种方法都证实了先前假设的途径的存在和功能,并揭示了第二种主要途径,而先前对Cpl的静态晶体结构的分析并未发现这种途径。我们的结果表明,小的疏水分子(例如H-2和O-2)在Cpl中扩散,利用了明确定义的堆积缺陷,这种缺陷在蛋白质的静态结构中并不总是很明显,但可以从蛋白质的静态结构中预测出来动力运动。最后,我们描述了H-2和O-2的两种不同的蛋白内运输模式,在我们的模型中仅根据它们的大小进行区分。

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