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Switching states: dynamic remodelling of polarity complexes as a toolkit for cell polarization

机译:切换状态:极性复合物的动态重塑作为细胞偏振的工具包

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Polarity is defined by the segregation of cellular components along a defined axis. To polarize robustly, cells must be able to break symmetry and subsequently amplify these nascent asymmetries. Finally, asymmetric localization of signaling molecules must be translated into functional regulation of downstream effector pathways. Central to these behaviors are a diverse set of cell polarity networks. Within these networks, molecules exhibit varied behaviors, dynamically switching among different complexes and states, active versus inactive, bound versus unbound, immobile versus diffusive. This ability to switch dynamically between states is intimately connected to the ability of molecules to generate asymmetric patterns within cells. Focusing primarily on polarity pathways governed by the conserved PAR proteins, we discuss strategies enabled by these dynamic behaviors that are used by cells to polarize. We highlight not only how switching between states is linked to the ability of polarity proteins to localize asymmetrically, but also how cells take advantage of 'state switching' to regulate polarity in time and space.
机译:极性由沿着限定轴的蜂窝成分的分离来定义。为了稳健地偏离,电池必须能够破坏对称性并随后放大这些新生的不对称。最后,信号传导分子的不对称定位必须转化为下游效应途径的功能调节。这些行为的核心是一种多样化的细胞极性网络。在这些网络中,分子表现出各种行为,在不同的复合体和状态之间动态切换,活性与非活动,绑定与未绑定,不动的相比之异。这种在状态之间动态切换的能力密切相关于分子在细胞内产生不对称模式的能力。主要关注由保守的Par蛋白治理的极性途径,我们讨论了通过细胞使用的这些动态行为使能实现极化的策略。我们不仅突出了各国之间的切换与极性蛋白质的能力如何相似地联系起来,而且还要如何利用“状态切换”来调节时间和空间的极性。

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