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G蛋白偶联信号通过控制非洲爪蟾早期胚胎中的钙黏蛋白表达来调控皮质肌动蛋白组装。

G-protein-coupled signals control cortical actin assembly by controlling cadherin expression in the early Xenopus embryo.

作者信息

Tao Qinghua, Nandadasa Sumeda, McCrea Pierre D, Heasman Janet, Wylie Christopher

机构信息

Children's Hospital Research Foundation, Division of Developmental Biology, and Molecular and Developmental Biology Graduate Program, University of Cincinnati College of Medicine, OH 45219, USA.

出版信息

Development. 2007 Jul;134(14):2651-61. doi: 10.1242/dev.002824. Epub 2007 Jun 13.

Abstract

During embryonic development, each cell of a multicellular organ rudiment polymerizes its cytoskeletal elements in an amount and pattern that gives the whole cellular population its characteristic shape and mechanical properties. How does each cell know how to do this? We have used the Xenopus blastula as a model system to study this problem. Previous work has shown that the cortical actin network is required to maintain shape and rigidity of the whole embryo, and its assembly is coordinated throughout the embryo by signaling through G-protein-coupled receptors. In this paper, we show that the cortical actin network colocalizes with foci of cadherin expressed on the cell surface. We then show that cell-surface cadherin expression is both necessary and sufficient for cortical actin assembly and requires the associated catenin p120 for this function. Finally, we show that the previously identified G-protein-coupled receptors control cortical actin assembly by controlling the amount of cadherin expressed on the cell surface. This identifies a novel mechanism for control of cortical actin assembly during development that might be shared by many multicellular arrays.

摘要

在胚胎发育过程中,多细胞器官原基的每个细胞都会以一定的数量和模式聚合其细胞骨架成分,从而使整个细胞群体具有其特有的形状和机械特性。每个细胞是如何知道该怎么做的呢?我们以非洲爪蟾囊胚作为模型系统来研究这个问题。先前的研究表明,皮质肌动蛋白网络对于维持整个胚胎的形状和刚性是必需的,并且其组装通过G蛋白偶联受体介导的信号传导在整个胚胎中得到协调。在本文中,我们表明皮质肌动蛋白网络与细胞表面表达的钙黏着蛋白焦点共定位。然后我们证明,细胞表面钙黏着蛋白的表达对于皮质肌动蛋白组装既是必要的也是充分的,并且该功能需要相关的连环蛋白p120。最后,我们表明先前鉴定出的G蛋白偶联受体通过控制细胞表面表达的钙黏着蛋白的量来控制皮质肌动蛋白组装。这确定了一种在发育过程中控制皮质肌动蛋白组装的新机制,这种机制可能为许多多细胞阵列所共有。

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