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Tug-of-war between actomyosin-driven antagonistic forces determines the positioning symmetry in cell-sized confinement

机译:Actomyosin驱动的敌对力之间的拔河决定了细胞大小限制中的定位对称性

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Symmetric or asymmetric positioning of intracellular structures including the nucleus and mitotic spindle steers various biological processes such as cell migration, division, and embryogenesis. In typical animal cells, both a sparse actomyosin meshwork in the cytoplasm and a dense actomyosin cortex underneath the cell membrane participate in the intracellular positioning. However, it remains unclear how these coexisting actomyosin structures regulate the positioning symmetry. To reveal the potential mechanism, we construct an in vitro model composed of cytoplasmic extracts and nucleus-like clusters confined in droplets. Here we find that periodic centripetal actomyosin waves contract from the droplet boundary push clusters to the center in large droplets, while network percolation of bulk actomyosin pulls clusters to the edge in small droplets. An active gel model quantitatively reproduces molecular perturbation experiments, which reveals that the tug-of-war between two distinct actomyosin networks with different maturation time-scales determines the positioning symmetry.
机译:细胞内结构的对称或不对称定位,包括核和有丝分裂主轴带操纵各种生物方法,例如细胞迁移,分裂和胚胎发生。在典型的动物细胞中,细胞质中的稀疏Actomyosin网状物和在细胞膜下方的致密肌动酶皮质中参与细胞内定位。然而,它仍然不明确于这些共存的抗型素结构如何调节定位对称性。为了揭示潜在的机制,我们构建由细胞质提取物和限制在液滴中的细胞质提取物和核状簇组成的体外模型。在这里,我们发现周期的离心肌肌蛋白波从液滴边界推动到大型液滴中的中心,而散装肌动素的网络渗流将簇拉到小液滴中的边缘。有源凝胶模型定量再现分子扰动实验,这揭示了具有不同成熟时间尺度的两个不同的血小杂素网络之间的脱瓦 - 导数决定了定位对称性。

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