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表皮生长因子样短共有重复序列结构域介导的蛋白质-蛋白质相互作用的分子分析:CD97-CD55复合物的剖析

Molecular analysis of the epidermal growth factor-like short consensus repeat domain-mediated protein-protein interactions: dissection of the CD97-CD55 complex.

作者信息

Lin H H, Stacey M, Saxby C, Knott V, Chaudhry Y, Evans D, Gordon S, McKnight A J, Handford P, Lea S

机构信息

Sir William Dunn School of Pathology, South Parks Road, Oxford, United Kingdom.

出版信息

J Biol Chem. 2001 Jun 29;276(26):24160-9. doi: 10.1074/jbc.M101770200. Epub 2001 Apr 10.

DOI:10.1074/jbc.M101770200
PMID:11297558
Abstract

Epidermal growth factor-like (EGF) and short consensus repeat (SCR) domains are commonly found in cell surface and soluble proteins that mediate specific protein-protein recognition events. Unlike the immunoglobulin (Ig) superfamily, very little is known about the general properties of intermolecular interactions encoded by these common modules, and in particular, how specificity of binding is achieved. We have dissected the binding of CD97 (a member of the EGF-TM7 family) to the complement regulator CD55, two cell surface modular proteins that contain EGF and SCR domains, respectively. We demonstrate that the interaction is mediated solely by these domains and is characterized by a low affinity (86 microm) and rapid off-rate (at least 0.6 s(-1)). The interaction is Ca(2+) -dependent but is unaffected by glycosylation of the EGF domains. Using biotinylated multimerized peptides in cell binding assays and surface plasmon resonance, we show that a CD97-related EGF-TM7 molecule (termed EMR2), differing by only three amino acids within the EGF domains, binds CD55 with a K(D) at least an order of magnitude weaker than that of CD97. These results suggest that low affinity cell-cell interactions may be a general feature of highly expressed cell surface proteins and that specificity of SCR-EGF binding can be finely tuned by a small number of amino acid changes on the EGF module surface.

摘要

表皮生长因子样(EGF)和短共有重复序列(SCR)结构域常见于介导特定蛋白质-蛋白质识别事件的细胞表面和可溶性蛋白质中。与免疫球蛋白(Ig)超家族不同,对于这些常见模块所编码的分子间相互作用的一般特性,尤其是结合特异性是如何实现的,我们了解得很少。我们剖析了CD97(EGF-TM7家族成员)与补体调节因子CD55的结合,这两种细胞表面模块化蛋白质分别含有EGF和SCR结构域。我们证明这种相互作用仅由这些结构域介导,其特征是亲和力低(86微摩尔)和解离速率快(至少0.6秒-1)。这种相互作用依赖于Ca(2+),但不受EGF结构域糖基化的影响。在细胞结合试验和表面等离子体共振中使用生物素化的多聚化肽,我们发现一种与CD97相关的EGF-TM7分子(称为EMR2),其EGF结构域内仅有三个氨基酸不同,与CD55结合的K(D)比CD97至少弱一个数量级。这些结果表明,低亲和力的细胞-细胞相互作用可能是高表达细胞表面蛋白质的一个普遍特征,并且SCR-EGF结合的特异性可以通过EGF模块表面少量的氨基酸变化进行精细调节。

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