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质膜-细胞质界面的液-液相分离:黏附、迁移和突触功能中的共同参与者。

Liquid-Liquid Phase Separation at the Plasma Membrane-Cytosol Interface: Common Players in Adhesion, Motility, and Synaptic Function.

机构信息

Vita-Salute San Raffaele University and San Raffaele Scientific Institute, Via Olgettina, 58, 20132 Milano, Italy.

出版信息

J Mol Biol. 2022 Jan 15;434(1):167228. doi: 10.1016/j.jmb.2021.167228. Epub 2021 Sep 4.

DOI:10.1016/j.jmb.2021.167228
PMID:34487789
Abstract

Networks of scaffold proteins and enzymes assemble at the interface between the cytosol and specific sites of the plasma membrane, where these networks guide distinct cellular functions. Some of these plasma membrane-associated platforms (PMAPs) include shared core components that are able to establish specific protein-protein interactions, to produce distinct supramolecular assemblies regulating dynamic processes as diverse as cell adhesion and motility, or the formation and function of neuronal synapses. How cells organize such dynamic networks is still an open question. In this review we introduce molecular networks assembling at the edge of migrating cells, and at pre- and postsynaptic sites, which share molecular players that can drive the assembly of biomolecular condensates. Very recent experimental evidence has highlighted the emerging role of some of these multidomain/scaffold proteins belonging to the GIT, liprin-α and ELKS/ERC families as drivers of liquid-liquid phase separation (LLPS). The data point to an important role of LLPS: (i) in the formation of PMAPs at the edge of migrating cells, where LLPS appears to be involved in promoting protrusion and the turnover of integrin-mediated adhesions, to allow forward cell translocation; (ii) in the assembly of the presynaptic active zone and of the postsynaptic density deputed to the release and reception of neurotransmitter signals, respectively. The recent results indicate that LLPS at cytosol-membrane interfaces is suitable not only for the regulation of active cellular processes, but also for the continuous spatial rearrangements of the molecular interactions involved in these dynamic processes.

摘要

支架蛋白和酶的网络在细胞质和质膜特定部位的界面处组装,这些网络指导着不同的细胞功能。这些质膜相关平台(PMAPs)中的一些包含共享的核心成分,这些成分能够建立特定的蛋白质-蛋白质相互作用,产生不同的超分子组装体,调节细胞黏附和运动等多样化的动态过程,或神经元突触的形成和功能。细胞如何组织这些动态网络仍然是一个悬而未决的问题。在这篇综述中,我们介绍了在迁移细胞边缘以及在突触前和突触后部位组装的分子网络,这些网络共享能够驱动生物分子凝聚物组装的分子伴侣。最近的实验证据强调了属于 GIT、liprin-α 和 ELKS/ERC 家族的一些多结构域/支架蛋白作为液-液相分离(LLPS)驱动力的新兴作用。这些数据表明 LLPS 起着重要作用:(i)在迁移细胞边缘 PMAPs 的形成中,LLPS 似乎参与促进突起和整合素介导的黏附的周转,以允许细胞向前迁移;(ii)在突触前活性区和突触后密度的组装中,分别负责神经递质信号的释放和接收。最近的结果表明,质膜界面处的 LLPS 不仅适合于调节活跃的细胞过程,而且适合于涉及这些动态过程的分子相互作用的连续空间重排。

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