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首页> 外文期刊>Proteins: Structure, Function, and Genetics >Predicting order of conformational changes during protein conformational transitions using an interpolated elastic network model.
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Predicting order of conformational changes during protein conformational transitions using an interpolated elastic network model.

机译:使用插值弹性网络模型预测蛋白质构象转变过程中构象变化的顺序。

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摘要

The decryption of sequence of structural events during protein conformational transitions is essential to a detailed understanding of molecular functions of various biological nanomachines. Coarse-grained models have proven useful by allowing highly efficient simulations of protein conformational dynamics. By combining two coarse-grained elastic network models constructed based on the beginning and end conformations of a transition, we have developed an interpolated elastic network model to generate a transition pathway between the two protein conformations. For validation, we have predicted the order of local and global conformational changes during key ATP-driven transitions in three important biological nanomachines (myosin, F(1) ATPase and chaperonin GroEL). We have found that the local conformational change associated with the closing of active site precedes the global conformational change leading to mechanical motions. Our finding is in good agreement with the distribution of intermediate experimental structures, and it supports the importance of local motions at active site to drive or gate various conformational transitions underlying the workings of a diverse range of biological nanomachines.
机译:蛋白质构象转变过程中结构事件序列的解密对于详细理解各种生物纳米机器的分子功能至关重要。通过允许高效模拟蛋白质构象动力学,已证明粗粒度模型很有用。通过结合基于过渡的起点和末端构象构建的两个粗粒度弹性网络模型,我们开发了一个内插的弹性网络模型以在两个蛋白质构象之间生成过渡路径。为了验证,我们已经预测了在三个重要的生物纳米机器(肌球蛋白,F(1)ATPase和伴侣蛋白GroEL)中由ATP驱动的关键转变过程中局部和全局构象变化的顺序。我们发现与活动位点关闭相关的局部构象变化先于导致机械运动的全局构象变化。我们的发现与中间实验结构的分布非常吻合,它支持了在活动部位进行局部运动以驱动或控制各种生物学纳米机器工作基础上的各种构象转变的重要性。

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