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αVβ1整合素表达的选择性调控基于含αV异二聚体的分级形成。

The selective regulation of alpha Vbeta 1 integrin expression is based on the hierarchical formation of alpha V-containing heterodimers.

作者信息

Koistinen Pekka, Heino Jyrki

机构信息

MediCity Research Laboratory and the Department of Medical Biochemistry, Turku Graduate School of Biomedical Sciences, University of Turku, FIN-20520 Turku, Finland.

出版信息

J Biol Chem. 2002 Jul 5;277(27):24835-41. doi: 10.1074/jbc.M203149200. Epub 2002 May 7.

DOI:10.1074/jbc.M203149200
PMID:11997396
Abstract

The integrin beta1 subunit can form a heterodimer with 12 different alpha subunits. According to the present model, the expression level of any alphabeta complex is regulated by the availability of the specific alpha subunit, whereas beta1 subunit is constantly present in a large excess. The expression of several heterodimers containing the alphaV subunit seems to be regulated by an identical mechanism. The fact that many cells express alphaVbeta1 heterodimer, and that this fibronectin/vitronectin receptor may be selectively regulated, compromises the present model of the regulation of beta1 and alphaV integrins. We have tried to solve this problem by assuming that distinct alphabeta heterodimers are formed with different tendency. To test the hypothesis, we analyzed WM-266-4 melanoma cells transfected with a cDNA construct coding for an intracellular single-chain anti-alphaV integrin antibody. We could see 70-80% reduction in the cell surface expression of alphaV subunit. However, the only one of the alphaV integrins reduced on the cell surface was alphaVbeta1. This suggests that the cell surface expression level of alphaVbeta1 is dependent on the number of alphaV subunits available after the formation of other alphaV-containing heterodimers. Thus, there seems to be a hierarchy in the complex formation between alphaV and its different beta-partners. These observations explain how alphaVbeta1 can be specifically regulated without concomitant changes in the expression of other alphaV or beta1 integrins.

摘要

整合素β1亚基可与12种不同的α亚基形成异二聚体。根据目前的模型,任何αβ复合物的表达水平都由特定α亚基的可利用性调节,而β1亚基则大量过剩地持续存在。几种含有αV亚基的异二聚体的表达似乎受相同机制调节。许多细胞表达αVβ1异二聚体,且这种纤连蛋白/玻连蛋白受体可能受到选择性调节,这一事实对目前β1和αV整合素的调节模型提出了挑战。我们试图通过假设不同的αβ异二聚体以不同倾向形成来解决这个问题。为了验证这一假设,我们分析了用编码细胞内单链抗αV整合素抗体的cDNA构建体转染的WM-266-4黑色素瘤细胞。我们可以看到αV亚基的细胞表面表达减少了70 - 80%。然而,细胞表面减少的唯一一种αV整合素是αVβ1。这表明αVβ1的细胞表面表达水平取决于在形成其他含αV的异二聚体后可利用的αV亚基数量。因此,αV与其不同β伙伴之间的复合物形成似乎存在等级关系。这些观察结果解释了αVβ1如何能够被特异性调节,而其他αV或β1整合素的表达却没有随之改变。

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