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首页> 外文期刊>Journal of Cell Science >Recruitment of vimentin to the cell surface by beta3 integrin and plectin mediates adhesion strength.
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Recruitment of vimentin to the cell surface by beta3 integrin and plectin mediates adhesion strength.

机译:β3整联蛋白和凝集素可将波形蛋白募集到细胞表面,从而介导粘附强度。

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摘要

Much effort has been expended on analyzing how microfilament and microtubule cytoskeletons dictate the interaction of cells with matrix at adhesive sites called focal adhesions (FAs). However, vimentin intermediate filaments (IFs) also associate with the cell surface at FAs in endothelial cells. Here, we show that IF recruitment to FAs in endothelial cells requires beta3 integrin, plectin and the microtubule cytoskeleton, and is dependent on microtubule motors. In CHO cells, which lack beta3 integrin but contain vimentin, IFs appear to be collapsed around the nucleus, whereas in CHO cells expressing beta3 integrin (CHOwtbeta3), vimentin IFs extend to FAs at the cell periphery. This recruitment is regulated by tyrosine residues in the beta3 integrin cytoplasmic tail. Moreover, CHOwtbeta3 cells exhibit significantly greater adhesive strength than CHO or CHO cells expressing mutated beta3 integrin proteins. These differences require an intact vimentin network. Therefore, vimentin IF recruitment to the cell surface is tightly regulated and modulates the strength of adhesion of cells to their substrate.
机译:在分析微丝和微管细胞骨架如何决定细胞与基质在称为粘着斑(FAs)的粘着点之间的相互作用方面已经花费了很多精力。但是,波形蛋白中间丝(IFs)也与内皮细胞FAs的细胞表面结合。在这里,我们显示,如果将IF募集到内皮细胞中的FA,则需要beta3整合素,plectin和微管细胞骨架,并且依赖于微管马达。在缺少beta3整合素但含有波形蛋白的CHO细胞中,IFs似乎在细胞核周围塌陷,而在表达beta3整合蛋白(CHOwtbeta3)的CHO细胞中,波形蛋白IFs延伸至细胞外围的FAs。这种募集受到beta3整合素胞质尾中酪氨酸残基的调控。而且,CHOwtbeta3细胞比表达突变的beta3整联蛋白的CHO或CHO细胞表现出明显更高的粘附强度。这些差异需要完整的波形蛋白网络。因此,波形蛋白IF募集到细胞表面受到严格调节,并调节细胞与其底物的粘附强度。

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