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Large Protein Dynamics Described by Hierarchical-Component Mode Synthesis

机译:分层组件模式合成描述的大蛋白质动态

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Protein dynamics has played a pivotal role in understanding the biological function of protein. For investigation of such dynamics, normal-mode analysis (NMA) has been broadly employed with atomistic model and/or coarse-grained models such as elastic network model (ENM). For large protein complexes, NMA with even ENM encounters the expensive computational process such as diagonalization of Hessian (stiffness) matrix. Here, we suggest the hierarchical-component mode synthesis (hCMS), which allows the fast computation of low- frequency normal modes related to conformational change. Specifically, a large protein structure is regarded as a combination of several structural units, for which the eigen-value problem is utilized for obtaining the frequencies and their normal modes for each structural unit, and consequently, such frequencies and normal modes are assembled with geometrical constraint for interface between structural units in order to find the low-frequency normal modes of a large protein complex. It is shown that hCMS is able to provide the normal modes with accuracy, quantitatively comparable to those of original NMA. This implies that hCMS may enable the computationally efficient analysis of large protein dynamics.
机译:蛋白质动态在理解蛋白质的生物学功能方面发挥了枢转作用。为了调查这种动态,通常使用原子模型和/或粗粒模型(如弹性网络模型)(eNM)广泛使用正常模式分析(NMA)。对于大蛋白质复合物,NMA甚至enm遇到昂贵的计算过程,例如黑森州(刚度)矩阵的对角化。在这里,我们建议分层组件模式合成(HCM),其允许快速计算与构象变化相关的低频正常模式。具体地,大蛋白质结构被认为是若干结构单元的组合,其中用于获得每个结构单元的频率和它们的正常模式的特征值问题,因此,这种频率和正常模式与几何形式组装结构单元之间的接口约束,以找到大蛋白质复合物的低频正常模式。结果表明,HCM能够以精确度提供正常模式,定量与原始NMA的准确性相当。这意味着HCM可以实现对大蛋白质动态的计算有效分析。

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