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全长整合素激活的粗粒化模拟。

Coarse-Grained Simulation of Full-Length Integrin Activation.

机构信息

Department of Chemistry, Institute for Biophysical Dynamics, and James Franck Institute, The University of Chicago, Chicago, Illinois.

Yale Cardiovascular Research Center and Department of Internal Medicine (Section of Cardiovascular Medicine), Yale School of Medicine, New Haven, Connecticut.

出版信息

Biophys J. 2019 Mar 19;116(6):1000-1010. doi: 10.1016/j.bpj.2019.02.011. Epub 2019 Feb 22.

Abstract

Integrin conformational dynamics are critical to their receptor and signaling functions in many cellular processes, including spreading, adhesion, and migration. However, assessing integrin conformations is both experimentally and computationally challenging because of limitations in resolution and dynamic sampling. Thus, structural changes that underlie transitions between conformations are largely unknown. Here, focusing on integrin αvβ, we developed a modified form of the coarse-grained heterogeneous elastic network model (hENM), which allows sampling conformations at the onset of activation by formally separating local fluctuations from global motions. Both local fluctuations and global motions are extracted from all-atom molecular dynamics simulations of the full-length αvβ bent integrin conformer, but whereas the former are incorporated in the hENM as effective harmonic interactions between groups of residues, the latter emerge by systematically identifying and treating weak interactions between long-distance domains with flexible and anharmonic connections. The new hENM model allows integrins and single-point mutant integrins to explore various conformational states, including the initiation of separation between α- and β-subunit cytoplasmic regions, headpiece extension, and legs opening.

摘要

整合素构象动力学对于其在许多细胞过程中的受体和信号功能至关重要,包括扩散、黏附和迁移。然而,由于分辨率和动态采样的限制,评估整合素构象在实验和计算上都具有挑战性。因此,构象转变所依赖的结构变化在很大程度上是未知的。在这里,我们专注于整合素 αvβ,开发了一种粗粒化非均匀弹性网络模型(hENM)的改进形式,该模型通过正式将局部波动与整体运动分开,允许在激活开始时采样构象。局部波动和整体运动都是从全长 αvβ 弯曲整合素构象的全原子分子动力学模拟中提取出来的,但前者作为组间有效谐波相互作用被纳入 hENM,而后者则通过系统地识别和处理具有柔性和非谐连接的长程域之间的弱相互作用而出现。新的 hENM 模型允许整合素和单点突变整合素探索各种构象状态,包括 α-和 β-亚基胞质区域之间分离的开始、头结构延伸和腿的张开。

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