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A Highlights from MBoC Selection: α-Catenin contributes to the strength of E-cadherin–p120 interactions

机译:MBoC选择的亮点:α-连环蛋白有助于增强E-钙粘蛋白与p120的相互作用

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摘要

Cadherin–catenin interactions play an important role in cadherin-mediated adhesion. Here we present strong evidence that in the cadherin–catenin complex α-catenin contributes to the binding strength of another catenin, p120, to the same complex. Specifically, we found that a β-catenin–uncoupled cadherin mutant interacts much more weakly with p120 than its full-size counterpart and that it is rapidly endocytosed from the surface of A-431 cells. We also showed that p120 overexpression stabilizes this mutant on the cell surface. Examination of the α-catenin–deficient MDA-MB-468 cells and their derivates in which α-catenin was reintroduced showed that α-catenin reinforces E-cadherin–p120 association. Finally, a cross-linking analysis of the cadherin–catenin complex indicated that a large loop located in the middle of the p120 arm-repeat domain is in close spatial vicinity to the amino-terminal VH1 domain of α-catenin. The six amino acid–long extension of this loop, caused by an alternative splicing, weakens p120 binding to cadherin. The data suggest that α-catenin–p120 contact within the cadherin–catenin complex can regulate cadherin trafficking.
机译:钙黏着蛋白与catenin的相互作用在钙黏着蛋白介导的黏附中起重要作用。在这里,我们提供有力的证据表明,在钙粘蛋白-连环蛋白复合物中,α-连环蛋白有助于另一种连环蛋白p120与同一复合物的结合强度。特别是,我们发现,β-catenin-uncoupledcadherin突变体与p120的相互作用比全尺寸突变体弱得多,并且它被A-431细胞表面快速内吞。我们还显示p120过表达稳定了该突变体在细胞表面的表达。对α-catenin缺陷的MDA-MB-468细胞及其衍生物进行了重新检查,结果表明,α-catenin增强了E-cadherin-p120的结合。最后,对钙粘蛋白-连环蛋白复合物的交联分析表明,位于p120臂重复结构域中间的大环在空间上紧邻α-连环蛋白的氨基末端VH1结构域。由另一种剪接引起的该环的六个氨基酸长的延伸减弱了p120与钙黏着蛋白的结合。数据表明,钙粘蛋白-catenin复合物中的α-catenin-p120接触可以调节钙粘蛋白的运输。

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