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人类B淋巴细胞定义了一种与纤连蛋白结合的替代机制。α4β1整合素与III型连接段的LHGPEILDVPST序列相互作用足以促进细胞附着。

Human B lymphocytes define an alternative mechanism of adhesion to fibronectin. The interaction of the alpha 4 beta 1 integrin with the LHGPEILDVPST sequence of the type III connecting segment is sufficient to promote cell attachment.

作者信息

Garcia-Pardo A, Wayner E A, Carter W G, Ferreira O C

机构信息

Mononuclear Cell Biology, New York Blood Center, NY 10021.

出版信息

J Immunol. 1990 May 1;144(9):3361-6.

PMID:2139453
Abstract

In this report we have studied the mechanism of human B lymphocyte adhesion to fibronectin and to proteolytic fragments of this protein. B cells adhered to fibronectin and to a 38-kDa fragment, derived from the A chain, containing the Hep II domain and most of the type III connecting segment, IIICS, of fibronectin. Cells did not bind to an 80-kDa fragment containing the RGD adhesive sequence of fibronectin. Attachment to fibronectin or to the 38-kDa fragment was not affected by the 80-kDa fragment, the GRGDSPC synthetic peptide, or by a mAb specific for the alpha chain of the RGD-dependent fibronectin receptor, alpha 5 beta 1. However, B cell adhesion to fibronectin was inhibited by the synthetic peptides CS-1, comprising the first 25 amino acids of IIICS and B12, containing the sequence LHGPEILDVPST of CS-1 (residues 14-25). Moreover, this sequence was shown to be sufficient to induce stable cell adhesion when coated on plastic surfaces. A mAb specific for the alpha-subunit of the alpha 4 beta 1 integrin, completely inhibited B cell attachment to B12, CS-1, 38 kDa, and fibronectin coated substrata. These data clearly indicate that adhesion of B lymphocytes to fibronectin is exclusively mediated by the interaction of alpha 4 beta 1 with residues 14-25 of the IIICS region in fibronectin. Therefore this interaction constitutes an alternative pathway of adhesion to fibronectin, independent of RGD and alpha 5 beta 1.

摘要

在本报告中,我们研究了人B淋巴细胞与纤连蛋白及其蛋白水解片段的黏附机制。B细胞可黏附于纤连蛋白以及源自A链的一个38 kDa片段,该片段包含纤连蛋白的Hep II结构域和大部分III型连接段(IIICS)。细胞不与含有纤连蛋白RGD黏附序列的80 kDa片段结合。对纤连蛋白或38 kDa片段的黏附不受80 kDa片段、GRGDSPC合成肽或针对RGD依赖性纤连蛋白受体α5β1的α链的单克隆抗体的影响。然而,B细胞对纤连蛋白的黏附受到合成肽CS-1的抑制,CS-1由IIICS的前25个氨基酸组成,以及B12,其包含CS-1的序列LHGPEILDVPST(第14 - 25位氨基酸)。此外,当包被在塑料表面时,该序列被证明足以诱导稳定的细胞黏附。一种针对α4β1整合素α亚基的单克隆抗体完全抑制了B细胞对包被有B12、CS-1、38 kDa和纤连蛋白底物的黏附。这些数据清楚地表明,B淋巴细胞与纤连蛋白的黏附完全是由α4β1与纤连蛋白IIICS区域第14 - 25位氨基酸残基的相互作用介导的。因此,这种相互作用构成了一种独立于RGD和α5β1的与纤连蛋白黏附的替代途径。

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