肌动蛋白皮层中的刚性渗流和主动平流协同驱动变形虫细胞运动

IF 10.7 1区 生物学 Q1 CELL BIOLOGY
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引用次数: 0

摘要

自发运动是大多数类门类动物细胞的共同特征,通常归因于肌动蛋白网络的特性。对这一产生力量的机制的研究已经深入到最微小的分子细节,特别是在薄壁细胞膜驱动的迁移中。然而,肌动蛋白网络如何在收缩驱动的变形虫细胞内工作仍然缺乏统一的原理。在这里,我们以 HeLa 细胞中的稳定运动出血点作为变形虫运动系统模型,在单丝水平上对肌动蛋白皮层的动态进行了成像,并揭示了三种不同流变阶段的共存。我们引入了 "平流渗滤",这是一个刚性渗滤和主动平流协同作用的过程,在空间上将肌动蛋白网络的机械特性组织成一种最小的通用运动机制。根据我们对简化系统的观察,我们推测这一模型可以解释单根肌动蛋白丝水平的变形细胞(如癌细胞或免疫细胞)如何在复杂的三维环境中有效推进。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Rigidity percolation and active advection synergize in the actomyosin cortex to drive amoeboid cell motility

Rigidity percolation and active advection synergize in the actomyosin cortex to drive amoeboid cell motility

Spontaneous locomotion is a common feature of most metazoan cells, generally attributed to the properties of actomyosin networks. This force-producing machinery has been studied down to the most minute molecular details, especially in lamellipodium-driven migration. Nevertheless, how actomyosin networks work inside contraction-driven amoeboid cells still lacks unifying principles. Here, using stable motile blebs from HeLa cells as a model amoeboid motile system, we imaged the dynamics of the actin cortex at the single filament level and revealed the co-existence of three distinct rheological phases. We introduce “advected percolation,” a process where rigidity percolation and active advection synergize, spatially organizing the actin network’s mechanical properties into a minimal and generic locomotion mechanism. Expanding from our observations on simplified systems, we speculate that this model could explain, down to the single actin filament level, how amoeboid cells, such as cancer or immune cells, can propel efficiently through complex 3D environments.

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来源期刊
Developmental cell
Developmental cell 生物-发育生物学
CiteScore
18.90
自引率
1.70%
发文量
203
审稿时长
3-6 weeks
期刊介绍: Developmental Cell, established in 2001, is a comprehensive journal that explores a wide range of topics in cell and developmental biology. Our publication encompasses work across various disciplines within biology, with a particular emphasis on investigating the intersections between cell biology, developmental biology, and other related fields. Our primary objective is to present research conducted through a cell biological perspective, addressing the essential mechanisms governing cell function, cellular interactions, and responses to the environment. Moreover, we focus on understanding the collective behavior of cells, culminating in the formation of tissues, organs, and whole organisms, while also investigating the consequences of any malfunctions in these intricate processes.
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