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Synthetic peptide GRGDS induces dissociation of alpha-actinin and vinculin from the sites of focal contacts

机译:合成肽GRGDS诱导α-肌动蛋白和纽蛋白从局灶性接触部位解离

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摘要

The synthetic peptide Gly-Arg-Gly-Asp-Ser (GRGDS) mimics the cellular binding site of many adhesive proteins in the extracellular matrix and causes rounding and detachment of spread cells. We have studied whether its binding affects the associations of two major components, alpha- actinin and vinculin, at the adhesion plaque. Living 3T3 cells were microinjected with fluorescently labeled alpha-actinin and/or vinculin and observed using video microscopy before and after the addition of 50 micrograms/ml GRGDS. As soon as 5 min after treatment, fluorescent alpha-actinin and vinculin became dissociated simultaneously from the sites of many focal contacts. The proteins either moved away as discrete structures or dispersed from adhesion plaques. As a result, the enrichment of alpha-actinin and vinculin at these focal contacts was no longer detected. The focal contacts then faded away slowly without showing detectable movement. These data suggest that the binding state of integrin has a transmembrane effect on the distribution of cytoskeletal components. The dissociation of alpha- actinin and vinculin from adhesion plaques may in turn weaken the contacts and result in rounding and detachment of cells.
机译:合成肽Gly-Arg-Gly-Asp-Ser(GRGDS)模仿细胞外基质中许多粘附蛋白的细胞结合位点,并导致铺展的细胞变圆和脱离。我们已经研究了它的结合是否影响粘附斑块上两个主要成分,α-肌动蛋白和纽蛋白的结合。将活体3T3细胞显微注射荧光标记的α-肌动蛋白和/或纽蛋白,并在添加50微克/毫升GRGDS之前和之后使用视频显微镜观察。处理后5分钟,荧光α-肌动蛋白和纽蛋白同时从许多焦点接触部位解离。蛋白质要么以离散结构的形式移走,要么从粘附斑块分散开。结果,在这些焦点接触处不再检测到α-肌动蛋白和纽蛋白的富集。然后,焦点接触慢慢消失,而没有显示出可检测到的运动。这些数据表明整联蛋白的结合状态对细胞骨架成分的分布具有跨膜作用。 α-肌动蛋白和纽蛋白从粘附斑块上解离可能反过来削弱接触并导致细胞变圆和脱离。

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