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指状膜突由肌动蛋白网络的非均一性所偏好。

Finger-like membrane protrusions are favored by heterogeneities in the actin network.

机构信息

Department of Chemical Engineering, Ilse Kats Institute for Nanoscale Science and Technology, Ben Gurion University of the Negev, Beer-Sheva, Israel.

出版信息

Soft Matter. 2020 Aug 21;16(31):7222-7230. doi: 10.1039/c9sm02444a. Epub 2020 May 21.

Abstract

Finger-like protrusions in cells are mostly generated by an active actin cytoskeleton pushing against the cell membrane. Conventional filopodia, localized at the leading edge of the cells, are long and thin protrusions composed of parallel actin filaments that emanate from a branched actin network. In contrast, dendritic filopodia, precursors of dendritic spines in neurons, are entirely filled in with a branched actin network. Here, we investigate in vitro how the dynamics of branched actin structures, polymerized at a membrane surface, trigger the formation of both protrusion types. Using supported bilayers and liposomes, we show that a decrease in the amount of activation sites at the membrane surface leads to the appearance of heterogeneities in the actin network coverage. Such heterogeneities promote the formation of membrane protrusions, and the size of heterogeneity patches matches the one of the protrusion base. Protrusion shape, cylindrical or conical, directly correlates with the absence or the presence of actin branches, respectively.

摘要

细胞中的指状突起主要是由活跃的肌动蛋白细胞骨架推动细胞膜产生的。传统的丝状伪足位于细胞的前缘,是由从分支肌动蛋白网络中伸出的平行肌动蛋白丝组成的长而细的突起。相比之下,树突状丝状伪足是神经元树突棘的前体,完全由分支肌动蛋白网络填充。在这里,我们在体外研究了在膜表面聚合的分支肌动蛋白结构的动力学如何引发这两种突起类型的形成。使用支撑双层膜和脂质体,我们表明,膜表面激活位点数量的减少会导致肌动蛋白网络覆盖的异质性出现。这种异质性促进了膜突起的形成,并且异质性斑块的大小与突起基部的大小相匹配。突起的形状,圆柱形或圆锥形,分别与肌动蛋白分支的存在或不存在直接相关。

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