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Centering and symmetry breaking in confined contracting actomyosin networks

机译:局限性收缩肌动球蛋白网络的定中心和对称性破坏

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摘要

Centering and decentering of cellular components is essential for internal organization of cells and their ability to perform basic cellular functions such as division and motility. How cells achieve proper localization of their organelles is still not well-understood, especially in large cells such as oocytes. Here, we study actin-based positioning mechanisms in artificial cells with persistently contracting actomyosin networks, generated by encapsulating cytoplasmic egg extracts into cell-sized ‘water-in-oil’ droplets. We observe size-dependent localization of the contraction center, with a symmetric configuration in larger cells and a polar one in smaller cells. Centering is achieved via a hydrodynamic mechanism based on Darcy friction between the contracting network and the surrounding cytoplasm. During symmetry breaking, transient attachments to the cell boundary drive the contraction center to a polar location. The centering mechanism is cell-cycle dependent and weakens considerably during interphase. Our findings demonstrate a robust, yet tunable, mechanism for subcellular localization.
机译:细胞成分的居中和偏心对于细胞的内部组织及其执行基本细胞功能(例如分裂和运动)的能力至关重要。细胞如何实现其细胞器的正确定位仍不为人所知,尤其是在诸如卵母细胞之类的大细胞中。在这里,我们研究了在肌动蛋白网络不断收缩的人造细胞中基于肌动蛋白的定位机制,这种肌动蛋白网络是通过将细胞质卵提取物封装到细胞大小的“油包水”液滴中而产生的。我们观察到收缩中心的大小依赖性定位,在大细胞中具有对称构型,在小细胞中具有极性构型。通过基于收缩网络和周围细胞质之间的达西摩擦的流体力学机制实现对中。在对称破坏过程中,细胞边界的瞬时附着将收缩中心驱至极点。定心机制是细胞周期依赖性的,在相间期明显减弱。我们的发现表明亚细胞定位的鲁棒但可调的机制。

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