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玻连蛋白受体αvβ3可结合纤连蛋白,并与α5β1协同作用,促进细胞在纤连蛋白上的黏附和铺展。

The vitronectin receptor alpha v beta 3 binds fibronectin and acts in concert with alpha 5 beta 1 in promoting cellular attachment and spreading on fibronectin.

作者信息

Charo I F, Nannizzi L, Smith J W, Cheresh D A

机构信息

COR Therapeutics, Inc., South San Francisco, California 94080.

出版信息

J Cell Biol. 1990 Dec;111(6 Pt 1):2795-800. doi: 10.1083/jcb.111.6.2795.

Abstract

The vitronectin receptor (alpha v beta 3) is a member of the integrin superfamily of adhesive protein receptors that mediate a wide spectrum of adhesive cellular interactions, including attachment to vitronectin, von Willebrand factor, fibrinogen, and thrombospondin. We have studied the binding of fibronectin to the purified vitronectin receptor, and the role of this receptor in the attachment of cells to fibronectin. A solid-phase microtiter assay was developed to investigate the binding properties of the vitronectin receptor. Purified alpha v beta 3 bound fibronectin with high affinity in a saturable, divalent cation-dependent manner. Binding was inhibited by soluble vitronectin, by RGD-containing peptides, and by LM609, a monoclonal antibody against the vitronectin receptor known to inhibit the binding of adhesive proteins to alpha v beta 3. Immunoinhibition experiments showed that M21 human melanoma cells, which express the fibronectin receptor, alpha 5 beta 1, as well as alpha v beta 3, used both of these integrins to attach and spread on fibronectin. In support of this finding, M21-L cells, a variant cell line that specifically lacks alpha v beta 3 but expresses alpha v beta 1, attached and spread poorly on fibronectin. In addition, alpha v beta 3 from surface-labeled M21 cells was retained, and selectively eluted by RGDS from a fibronectin affinity column. These results indicate that alpha v beta 3 acts in concert with alpha 5 beta 1 in promoting fibronectin recognition by these cells. We conclude that fibronectin binds to the alpha v beta 3 vitronectin receptor specifically and with high affinity, and that this interaction is biologically relevant in supporting cell adhesion to matrix proteins.

摘要

玻连蛋白受体(αvβ3)是黏附蛋白受体整合素超家族的成员,介导多种黏附性细胞相互作用,包括与玻连蛋白、血管性血友病因子、纤维蛋白原和血小板反应蛋白的黏附。我们研究了纤连蛋白与纯化的玻连蛋白受体的结合,以及该受体在细胞与纤连蛋白黏附中的作用。开发了一种固相微量滴定法来研究玻连蛋白受体的结合特性。纯化的αvβ3以可饱和的、二价阳离子依赖性方式与纤连蛋白高亲和力结合。可溶性玻连蛋白、含RGD的肽以及LM609(一种已知可抑制黏附蛋白与αvβ3结合的抗玻连蛋白受体单克隆抗体)可抑制结合。免疫抑制实验表明,表达纤连蛋白受体α5β1以及αvβ3的M21人黑色素瘤细胞利用这两种整合素来在纤连蛋白上黏附并铺展。支持这一发现的是,M21-L细胞是一种特异性缺乏αvβ3但表达αvβ1的变异细胞系,其在纤连蛋白上的黏附及铺展较差。此外,来自表面标记的M21细胞的αvβ3被保留,并被RGDS从纤连蛋白亲和柱上选择性洗脱。这些结果表明,αvβ3与α5β1协同作用促进这些细胞对纤连蛋白的识别。我们得出结论,纤连蛋白与αvβ3玻连蛋白受体特异性且高亲和力结合,并且这种相互作用在支持细胞与基质蛋白的黏附中具有生物学相关性。

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本文引用的文献

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Integrins: a family of cell surface receptors.整合素:一类细胞表面受体。
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