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The More the Tubular: Dynamic Bundling of Actin Filaments for Membrane Tube Formation

机译:管状越多:肌动蛋白丝动态捆绑成膜管。

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摘要

Tubular protrusions are a common feature of living cells, arising from polymerization of stiff protein filaments against a comparably soft membrane. Although this process involves many accessory proteins in cells, in vitro experiments indicate that similar tube-like structures can emerge without them, through spontaneous bundling of filaments mediated by the membrane. Using theory and simulation of physical models, we have elaborated how nonequilibrium fluctuations in growth kinetics and membrane shape can yield such protrusions. Enabled by a new grand canonical Monte Carlo method for membrane simulation, our work reveals a cascade of dynamical transitions from individually polymerizing filaments to highly cooperatively growing bundles as a dynamical bottleneck to tube formation. Filament network organization as well as adhesion points to the membrane, which bias filament bending and constrain membrane height fluctuations, screen the effective attractive interactions between filaments, significantly delaying bundling and tube formation.
机译:管状突起是活细胞的共同特征,它是由刚性蛋白丝相对于相对较软的膜聚合而成的。尽管此过程涉及细胞中许多辅助蛋白,但体外实验表明,通过膜介导的细丝的自发捆扎,类似的管状结构可以在没有它们的情况下出现。使用物理模型的理论和模拟,我们详细说明了生长动力学和膜形状的非平衡波动如何产生此类突起。通过采用新的大经典蒙特卡洛方法进行膜模拟,我们的工作揭示了从单独聚合的长丝到高度协作生长的束的动态过渡级联,成为形成管的动态瓶颈。细丝网络的组织以及与膜的粘附点,可偏置细丝弯曲并限制膜的高度波动,筛选细丝之间的有效吸引相互作用,从而显着延迟束缚和管的形成。

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