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Membrane Sculpting by F-BAR Domains Studied by Molecular Dynamics Simulations

机译:分子动力学模拟研究F-BAR结构域的膜雕刻

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摘要

Interplay between cellular membranes and their peripheral proteins drives many processes in eukaryotic cells. Proteins of the Bin/Amphiphysin/Rvs (BAR) domain family, in particular, play a role in cellular morphogenesis, for example curving planar membranes into tubular membranes. However, it is still unclear how F-BAR domain proteins act on membranes. Electron microscopy revealed that, in vitro, F-BAR proteins form regular lattices on cylindrically deformed membrane surfaces. Using all-atom and coarse-grained (CG) molecular dynamics simulations, we show that such lattices, indeed, induce tubes of observed radii. A 250 ns all-atom simulation reveals that F-BAR domain curves membranes via the so-called scaffolding mechanism. Plasticity of the F-BAR domain permits conformational change in response to membrane interaction, via partial unwinding of the domains 3-helix bundle structure. A CG simulation covering more than 350 µs provides a dynamic picture of membrane tubulation by lattices of F-BAR domains. A series of CG simulations identified the optimal lattice type for membrane sculpting, which matches closely the lattices seen through cryo-electron microscopy.
机译:细胞膜及其外围蛋白之间的相互作用推动了真核细胞的许多过程。 Bin /双亲蛋白/ Rvs(BAR)域家族的蛋白质尤其在细胞形态发生中起作用,例如将平面膜弯曲成管状膜。然而,仍不清楚F-BAR结构域蛋白如何作用于膜。电子显微镜显示,在体外,F-BAR蛋白在圆柱形变形的膜表面上形成规则的晶格。使用全原子和粗粒(CG)分子动力学模拟,我们表明这种晶格确实会诱发观察半径的管。 250 ns的全原子模拟显示F-BAR域通过所谓的支架机制使膜弯曲。 F-BAR结构域的可塑性允许通过膜结构域3螺旋束结构的部分展开来响应膜相互作用的构象变化。超过350 µs的CG模拟提供了F-BAR域晶格对膜微管形成的动态描绘。一系列CG模拟确定了用于膜雕刻的最佳晶格类型,该晶格类型与通过低温电子显微镜观察到的晶格紧密匹配。

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