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细胞与肌腱蛋白-X的黏附:细胞黏附位点的定位及整合素受体的鉴定

Cell adhesion to tenascin-X mapping of cell adhesion sites and identification of integrin receptors.

作者信息

Elefteriou F, Exposito J Y, Garrone R, Lethias C

机构信息

Institut de Biologie et Chimie des Protéines, CNRS, Unité Propre de Recherche 412, Université Claude Bernard, Lyon, France.

出版信息

Eur J Biochem. 1999 Aug;263(3):840-8. doi: 10.1046/j.1432-1327.1999.00563.x.

Abstract

Adhesive properties of tenascin-X (TN-X) were investigated using TN-X purified from bovine skin and recombinant proteins encompassing the RGD sequence located within the tenth fibronectin type-III domain, and the fibrinogen-like domain. Osteosarcoma (MG63) and bladder carcinoma cells (ECV304) cells were shown to adhere to purified TN-X, but did not spread and did not assemble actin stress fibers. Both cell types adhered to recombinant proteins harboring the contiguous fibronectin type-III domains 9 and 10 (FNX 9-10) but not to the FNX 10 domain alone. This adhesion to FNX 9-10 was shown to be mediated by alphavbeta3 integrin, was inhibited by RGD peptides and was strongly reduced in proteins mutated within the RGD site. As antibodies against alphavbeta3 integrin had no effects on cell adhesion to purified TN-X, we suggest that the RGD sequence is masked in intact TN-X. Cell attachment to the recombinant TN-X fibrinogen domain (FbgX) and to purified TN-X was greater for MG63 than for ECV304 cells. A beta1-containing integrin was shown to be involved in MG63 cell attachment to FbgX and to purified TN-X. Although the existence of other cell interaction sites is likely in this huge molecule, these similar patterns of adhesion and inhibition suggest that the fibrinogen domain might be a dominant site in the whole molecule.

摘要

使用从牛皮中纯化得到的腱生蛋白-X(TN-X)以及包含位于第十个III型纤连蛋白结构域内的RGD序列和纤维蛋白原样结构域的重组蛋白,对腱生蛋白-X(TN-X)的黏附特性进行了研究。骨肉瘤(MG63)细胞和膀胱癌细胞(ECV304)显示出能黏附于纯化的TN-X,但不会铺展,也不会组装肌动蛋白应力纤维。这两种细胞类型都能黏附于含有连续的III型纤连蛋白结构域9和10的重组蛋白(FNX 9-10),但单独对FNX 10结构域则无黏附作用。已证明这种对FNX 9-10的黏附是由αvβ3整合素介导的,受RGD肽抑制,并且在RGD位点发生突变的蛋白中黏附作用大幅降低。由于抗αvβ3整合素抗体对细胞黏附纯化的TN-X没有影响,我们认为在完整的TN-X中RGD序列被掩盖了。MG63细胞对重组TN-X纤维蛋白原样结构域(FbgX)和纯化TN-X的细胞黏附作用比对ECV304细胞更强。已证明一种含β1的整合素参与了MG63细胞对FbgX和纯化TN-X的黏附。尽管在这个巨大的分子中可能存在其他细胞相互作用位点,但这些相似的黏附模式和抑制模式表明纤维蛋白原样结构域可能是整个分子中的主要位点。

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