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Conformational flexibility and the mechanisms of allosteric transitions in topologically similar proteins

机译:拓扑相似蛋白的构象灵活性和变构转变机理

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Conformational flexibility plays a central role in allosteric transition of proteins. In this paper, we extend the analysis of our previous study [S. Tripathi and J. J. Portman, Proc. Natl. Acad. Sci. U.S.A. 106, 2104 (2009)] to investigate how relatively minor structural changes of the meta-stable states can significantly influence the conformational flexibility and allosteric transition mechanism. We use the allosteric transitions of the domains of calmodulin as an example system to highlight the relationship between the transition mechanism and the inter-residue contacts present in the meta-stable states. In particular, we focus on the origin of transient local unfolding (cracking), a mechanism that can lower free energy barriers of allosteric transitions, in terms of the inter-residue contacts of the meta-stable states and the pattern of local strain that develops during the transition. We find that the magnitude of the local strain in the protein is not the sole factor determining whether a region will ultimately crack during the transition. These results emphasize that the residue interactions found exclusively in one of the two meta-stable states is the key in understanding the mechanism of allosteric conformational change.
机译:构象柔韧性在蛋白质的变构转变中起核心作用。在本文中,我们扩展了对先前研究的分析[S. Tripathi和J. J. Portman,过程。 Natl。学院科学[U.S.A. 106,2104(2009)],研究亚稳态的相对较小的结构变化如何显着影响构象柔韧性和变构过渡机制。我们使用钙调蛋白域的变构过渡作为一个示例系统,以突出过渡机制与存在于亚稳定状态的残基间接触之间的关系。特别地,我们关注瞬态局部展开(裂纹)的起源,这种机制可以通过亚稳态的残基间接触和形成的局部应变模式来降低变构过渡的自由能垒。在过渡期间。我们发现蛋白质中局部应变的大小不是确定区域在过渡过程中最终是否会破裂的唯一因素。这些结果强调,仅在两个亚稳定状态之一中发现的残基相互作用是理解变构构象变化机理的关键。

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