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CD9四跨膜蛋白上一个功能相关的构象表位取决于与活化的β1整合素的结合。

A functionally relevant conformational epitope on the CD9 tetraspanin depends on the association with activated beta1 integrin.

作者信息

Gutierrez-Lopez Maria Dolores, Ovalle Susana, Yanez-Mo Maria, Sanchez-Sanchez Noelia, Rubinstein Eric, Olmo Nieves, Lizarbe Maria Antonia, Sanchez-Madrid Francisco, Cabanas Carlos

机构信息

Instituto de Farmacologia y Toxicologia CSIC-UCM, Facultad de Medicina, Universidad Complutense, 28040 Madrid, Spain.

出版信息

J Biol Chem. 2003 Jan 3;278(1):208-18. doi: 10.1074/jbc.M207805200. Epub 2002 Oct 30.

DOI:10.1074/jbc.M207805200
PMID:12411441
Abstract

Tetraspanins associate on the cell membrane with several transmembrane proteins, including members of the integrin superfamily. The tetraspanin CD9 has been implicated in cell motility, metastasis, and sperm-egg fusion. In this study we characterize the first CD9 conformation-dependent epitope (detected by monoclonal antibody (mAb) PAINS-13) whose expression depends on changes in the activation state of associated beta(1) integrins. MAb PAINS-13 precipitates CD9 under conditions that preserve the association of this tetraspanin with integrins, but not under conditions that disrupt these interactions. Induction of activation of beta(1) integrins by temperature, divalent cation Mn(2+), or mAb TS2/16 correlated with enhanced expression of the PAINS-13 epitope on a variety of cells. Through the use of different K562 myeloid leukemia transfectant cells expressing specific members of the beta(1) integrin subfamily we show that the expression of the PAINS-13 epitope depends on CD9 association with alpha(6)beta(1) integrin. The mAb PAINS-13 reactivity has been mapped to the CD9 region comprising residues 112-154 in the NH(2) half of the large extracellular loop. Also, we show that the CD9 conformation recognized by mAb PAINS-13 is functionally relevant in beta(1) integrin-mediated cellular processes including wound healing migration, tubular morphogenesis, cell adhesion and spreading and in signal transduction involving phosphatidylinositol 3-kinase activation.

摘要

四跨膜蛋白在细胞膜上与多种跨膜蛋白相互作用,包括整合素超家族的成员。四跨膜蛋白CD9与细胞运动、转移以及精卵融合有关。在本研究中,我们鉴定了首个CD9构象依赖性表位(由单克隆抗体(mAb)PAINS - 13检测),其表达依赖于相关β(1)整合素激活状态的变化。单克隆抗体PAINS - 13在能保持该四跨膜蛋白与整合素结合的条件下沉淀CD9,但在破坏这些相互作用的条件下则不能。通过温度、二价阳离子Mn(2+)或单克隆抗体TS2/16诱导β(1)整合素激活,与多种细胞上PAINS - 13表位的表达增强相关。通过使用表达β(1)整合素亚家族特定成员的不同K562髓系白血病转染细胞,我们表明PAINS - 13表位的表达依赖于CD9与α(6)β(1)整合素的结合。单克隆抗体PAINS - 13的反应活性已定位到CD9的一个区域,该区域位于大细胞外环NH(2)端的112 - 154位残基。此外,我们表明单克隆抗体PAINS - 13识别的CD9构象在β(1)整合素介导的细胞过程中具有功能相关性,这些过程包括伤口愈合迁移、管状形态发生、细胞黏附与铺展以及涉及磷脂酰肌醇3激酶激活的信号转导。

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