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二价阳离子对整合素α5β1-纤连蛋白相互作用的调节。锰离子、镁离子和钙离子不同类型结合位点的证据。

Regulation of integrin alpha 5 beta 1-fibronectin interactions by divalent cations. Evidence for distinct classes of binding sites for Mn2+, Mg2+, and Ca2+.

作者信息

Mould A P, Akiyama S K, Humphries M J

机构信息

Wellcome Trust Centre for Cell-Matrix Research, School of Biological Sciences, University of Manchester, United Kingdom.

出版信息

J Biol Chem. 1995 Nov 3;270(44):26270-7. doi: 10.1074/jbc.270.44.26270.

DOI:10.1074/jbc.270.44.26270
PMID:7592835
Abstract

Integrin-ligand interactions are known to be dependent on divalent cations, although the precise role of cations in ligand binding is still unclear. Using the interaction between alpha 5 beta 1 and fibronectin as a model system, we have performed a comprehensive analysis of the effects of Mn2+, Mg2+, and Ca2+ on ligand binding. Each cation had distinct effects on the ligand-binding capacity of alpha 5 beta 1:Mn2+ promoted high levels of ligand binding, Mg2+ promoted low levels of binding, and Ca2+ failed to support binding. Studies of the effects of different combinations of cations on ligand binding indicated that the cation-binding sites within alpha 5 beta 1 are not all identical, or of broad specificity, but instead each site shows a distinct preference for one or more cations. Ca2+ strongly inhibited Mn(2+)-supported ligand binding, but this inhibition was noncompetitive, suggesting that Ca2+ recognizes different cation-binding sites to Mn2+. In contrast, Ca2+ acted as a direct competitive inhibitor of Mg(2+)-supported ligand binding, implying that Ca2+ can displace Mg2+ from the integrin. However, low concentrations of Ca2+ greatly increased the apparent affinity of Mg2+ for its binding site, suggesting the existence of a distinct high affinity Ca(2+)-binding site. Taken together, our results imply that the ligand-binding capacity of alpha 5 beta 1 can be regulated in a complex manner through separate classes of binding sites for Mn2+, Mg2+, and Ca2+.

摘要

已知整合素-配体相互作用依赖于二价阳离子,尽管阳离子在配体结合中的精确作用仍不清楚。以α5β1与纤连蛋白之间的相互作用作为模型系统,我们对Mn2+、Mg2+和Ca2+对配体结合的影响进行了全面分析。每种阳离子对α5β1的配体结合能力都有不同影响:Mn2+促进高水平的配体结合,Mg2+促进低水平的结合,而Ca2+无法支持结合。对不同阳离子组合对配体结合影响的研究表明,α5β1内的阳离子结合位点并非全部相同或具有广泛特异性,而是每个位点对一种或多种阳离子表现出明显的偏好。Ca2+强烈抑制Mn(2+)支持的配体结合,但这种抑制是非竞争性的,表明Ca2+识别与Mn2+不同的阳离子结合位点。相反,Ca2+作为Mg(2+)支持的配体结合的直接竞争性抑制剂,这意味着Ca2+可以从整合素中取代Mg2+。然而,低浓度的Ca2+大大增加了Mg2+对其结合位点的表观亲和力,表明存在一个独特的高亲和力Ca(2+)结合位点。综上所述,我们的结果表明,α5β1的配体结合能力可以通过Mn2+、Mg2+和Ca2+的不同结合位点以复杂的方式进行调节。

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