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首页> 外文期刊>Proteins: Structure, Function, and Genetics >Protein conformational transitions explored by mixed elastic network models.
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Protein conformational transitions explored by mixed elastic network models.

机译:通过混合弹性网络模型探索蛋白质构象转变。

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摘要

We develop a mixed elastic network model (MENM) to study large-scale conformational transitions of proteins between two (or more) known structures. Elastic network potentials for the beginning and end states of a transition are combined, in effect, by adding their respective partition functions. The resulting effective MENM energy function smoothly interpolates between the original surfaces, and retains the beginning and end structures as local minima. Saddle points, transition paths, potentials of mean force, and partition functions can be found efficiently by largely analytic methods. To characterize the protein motions during a conformational transition, we follow "transition paths" on the MENM surface that connect the beginning and end structures and are invariant to parameterizations of the model and the mathematical form of the mixing scheme. As illustrations of the general formalism, we study large-scale conformation changes of the motor proteins KIF1A kinesin and myosin II. We generate possibletransition paths for these two proteins that reveal details of their conformational motions. The MENM formalism is computationally efficient and generally applicable even for large protein systems that undergo highly collective structural changes.
机译:我们开发了一种混合弹性网络模型(MENM),以研究蛋白质在两个(或多个)已知结构之间的大规模构象转变。实际上,通过添加它们各自的分区功能,可以将过渡的开始状态和结束状态的弹性网络电位组合在一起。产生的有效MENM能量函数在原始曲面之间平滑地插值,并将起始和结束结构保留为局部最小值。鞍点,过渡路径,平均力势和分隔函数可以通过大量的分析方法有效地找到。为了表征构象转变期间的蛋白质运动,我们在MENM表面上遵循“转变路径”,该路径连接了开始和末端结构,并且对于模型的参数化和混合方案的数学形式不变。作为一般形式主义的例证,我们研究了运动蛋白KIF1A驱动蛋白和肌球蛋白II的大规模构象变化。我们为这两种蛋白质生成了可能的转变路径,揭示了它们构象运动的细节。 MENM形式主义在计算上是有效的,并且甚至适用于经历高度集体结构变化的大型蛋白质系统。

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