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由R-ras介导的整合素激活

Integrin activation by R-ras.

作者信息

Zhang Z, Vuori K, Wang H, Reed J C, Ruoslahti E

机构信息

La Jolla Cancer Research Center, The Burnham Institute, California 92037, USA.

出版信息

Cell. 1996 Apr 5;85(1):61-9. doi: 10.1016/s0092-8674(00)81082-x.

Abstract

Expression of a constitutively active R-ras converted two cell lines that grow in suspension into highly adherent cells. There was little change in cell surface expression of integrins, but attachment to surfaces coated with the integrin ligands was greatly enhanced. Cells transfected with activated R-ras bound integrin ligands from solution with higher affinities and assembled severalfold more fibronectin matrix than control transfectants. Introduction of a dominant negative R-ras into adherent cells reduced the adhesiveness of the cells, indicating that endogenous R-ras can control the ligand-binding activity of integrins. These results provide a mechanism for the modulation of integrin ligand-binding activity as well as novel function for R-ras.

摘要

组成型激活的R-ras的表达将两种悬浮生长的细胞系转化为高度贴壁的细胞。整合素的细胞表面表达几乎没有变化,但与包被有整合素配体的表面的附着显著增强。用激活的R-ras转染的细胞以更高的亲和力从溶液中结合整合素配体,并且比对照转染细胞组装的纤连蛋白基质多几倍。将显性负性R-ras导入贴壁细胞会降低细胞的黏附性,表明内源性R-ras可以控制整合素的配体结合活性。这些结果为整合素配体结合活性的调节提供了一种机制,也为R-ras的新功能提供了依据。

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