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Symmetry considerations elucidate the roles of global shape and local interactions in the equilibrium fluctuations and cooperativity of protein assemblies

机译:对称考虑阐明了全球形状和局部相互作用在均衡波动和蛋白质组合的合作性中的作用

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Shape had been intuitively recognized to play a dominant role in determining the global motion patterns of bio-molecular assemblies. However, it is not clear exactly how shape determines the motion patterns. What about the local interactions that hold a structure together to a certain shape? The contributions of global shape and local interactions usually mix together and are difficult to tease part. In this work, we use symmetry to elucidate the distinct roles of global shape and local interactions in protein dynamics. Symmetric complexes provide an ideal platform for this task since in them the effects of local interactions and global shape are separable, allowing their distinct roles to be identified. Our key findings based on symmetric assemblies are: (i) the motion patterns of each subunit are determined primarily by intra-subunit interactions (IRSi), and secondarily by inter-subunit interactions (IESi); (ii) the motion patterns of the whole assembly are fully dictated by the global symmetry/shape and have nothing to do with local iESi or IRSi. This is followed by a discussion on how the findings may be generalized to complexes in any shape, with or without symmetry.
机译:形状直观地认识到在确定生物分子组件的全球运动模式方面发挥着主导作用。但是,目前尚不清楚地确定如何确定运动模式。局部相互作用如何将结构持有一定的形状?全球形状和局部相互作用的贡献通常混合在一起,难以梳理部分。在这项工作中,我们使用对称性来阐明全球形状和局部相互作用在蛋白质动态的不同作用。对称复合部分为此任务提供了理想的平台,因为在它们中,局部交互和全局形状的效果是可分离的,允许识别其不同的作用。我们基于对称组件的关键发现是:(i)每个亚基的运动模式主要通过亚基间相互作用(IRSI),并通过亚基间相互作用(IESI); (ii)全部大会的运动模式由全球对称/形状完全决定,与本地IESI或IRSI无关。接下来,讨论如何将发现如何以任何形状,有或不具有对称性的。

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