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足细胞内联蛋白的磷酸化诱导了通过肌动球蛋白收缩运动的相分离域。

Phosphorylation of nephrin induces phase separated domains that move through actomyosin contraction.

机构信息

Department of Biophysics and Howard Hughes Medical Institute, University of Texas Southwestern Medical Center, Dallas, TX 75390.

The HHMI/MBL Summer Institute, Marine Biological Laboratory, Woods Hole, MA 02543.

出版信息

Mol Biol Cell. 2019 Nov 15;30(24):2996-3012. doi: 10.1091/mbc.E18-12-0823. Epub 2019 Oct 10.

Abstract

The plasma membrane of eukaryotic cells is organized into lipid and protein microdomains, whose assembly mechanisms and functions are incompletely understood. We demonstrate that proteins in the nephrin/Nck/N-WASP actin-regulatory pathway cluster into micron-scale domains at the basal plasma membrane upon triggered phosphorylation of transmembrane protein nephrin. The domains are persistent but readily exchange components with their surroundings, and their formation is dependent on the number of Nck SH3 domains, suggesting they are phase separated polymers assembled through multivalent interactions among the three proteins. The domains form independent of the actin cytoskeleton, but acto-myosin contractility induces their rapid lateral movement. Nephrin phosphorylation induces larger clusters at the cell periphery, which are associated with extensive actin assembly and dense filopodia. Our studies illustrate how multivalent interactions between proteins at the plasma membrane can produce micron-scale organization of signaling molecules, and how the resulting clusters can both respond to and control the actin cytoskeleton.

摘要

真核细胞的质膜组织成脂质和蛋白质微区,其组装机制和功能尚未完全了解。我们证明,在跨膜蛋白nephrin 被触发磷酸化后,nephrin/Nck/N-WASP 肌动蛋白调节途径中的蛋白质会在基底质膜上聚集到微米级的域中。这些域是持久的,但可以与周围环境交换组件,并且它们的形成依赖于 Nck SH3 结构域的数量,这表明它们是通过三种蛋白质之间的多价相互作用组装而成的相分离聚合物。这些域的形成与肌动球蛋白收缩无关,但肌动球蛋白收缩会诱导它们快速横向运动。nephrin 磷酸化诱导细胞边缘的更大簇,与广泛的肌动蛋白组装和密集的丝状伪足相关。我们的研究说明了质膜上蛋白质之间的多价相互作用如何产生信号分子的微米级组织,以及由此产生的簇如何既能响应又能控制肌动球蛋白细胞骨架。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9844/6857567/bf1a3c4ea6dd/mbc-30-2996-g001.jpg

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