Epitope mapping of a function-blocking beta 1 integrin antibody by phage display.

S T Ryan, G Chi-Rosso, L L Bonnycastle, J K Scott, V Koteliansky, S Pollard, P J Gotwals
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引用次数: 4

Abstract

Integrins are a major class of cell surface receptors involved in cell-cell and cell-matrix adhesion and communication. Ha2/11 is a function-blocking anti-rat beta 1 integrin hamster IgM that should be a useful reagent for understanding beta 1 integrin function. We demonstrate that Ha2/11 cross reacts with human, Xenopus, and Drosophila beta 1 integrins, and use phage display to map the epitope for Ha2/11 to residues within the sequence LRSGEPQTF which lies 18 amino acids proximal to the putative I domain in beta 1 integrins. Monoclonal antibody mapping experiments, mutational analyses, and direct binding assays have implicated integrin I domains in both cation and ligand binding. Our data therefore suggest that Ha2/11 blocks beta 1 integrin function by interfering with I domain-mediated ligand binding.

功能阻断β 1整合素抗体的噬菌体展示表位定位。
整合素是一类主要的细胞表面受体,参与细胞-细胞和细胞-基质的粘附和通讯。Ha2/11是一种功能阻断的抗大鼠β 1整合素仓鼠IgM,应该是了解β 1整合素功能的有用试剂。我们证明了Ha2/11与人类、非洲蟾和果蝇β 1整合素发生交叉反应,并利用噬菌体展示将Ha2/11的表位定位到序列LRSGEPQTF内的残基,该序列位于β 1整合素假定的I结构域附近18个氨基酸。单克隆抗体定位实验、突变分析和直接结合分析都涉及到整合素I结构域在阳离子和配体结合中的作用。因此,我们的数据表明,Ha2/11通过干扰I结构域介导的配体结合来阻断β 1整合素的功能。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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