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ephrin-A5 中的三个不同分子表面对于与 EphA3 的功能性相互作用至关重要。

Three distinct molecular surfaces in ephrin-A5 are essential for a functional interaction with EphA3.

作者信息

Day Bryan, To Catherine, Himanen Juha-Pekka, Smith Fiona M, Nikolov Dimitar B, Boyd Andrew W, Lackmann Martin

机构信息

Queensland Institute of Medical Research, P. O. Royal Brisbane Hospital 4029, Queensland, Australia.

出版信息

J Biol Chem. 2005 Jul 15;280(28):26526-32. doi: 10.1074/jbc.M504972200. Epub 2005 May 18.

DOI:10.1074/jbc.M504972200
PMID:15901737
Abstract

Eph receptor tyrosine kinases (Ephs) function as molecular relays that interact with cell surface-bound ephrin ligands to direct the position of migrating cells. Structural studies revealed that, through two distinct contact surfaces on opposite sites of each protein, Eph and ephrin binding domains assemble into symmetric, circular heterotetramers. However, Eph signal initiation requires the assembly of higher order oligomers, suggesting additional points of contact. By screening a random library of EphA3 binding-compromised ephrin-A5 mutants, we have now determined ephrin-A5 residues that are essential for the assembly of high affinity EphA3 signaling complexes. In addition to the two interfaces predicted from the crystal structure of the homologous EphB2.ephrin-B2 complex, we identified a cluster of 10 residues on the ephrin-A5 E alpha-helix, the E-F loop, the underlying H beta-strand, as well as the nearby B-C loop, which define a distinct third surface required for oligomerization and activation of EphA3 signaling. Together with a corresponding third surface region identified recently outside of the minimal ephrin binding domain of EphA3, our findings provide experimental evidence for the essential contribution of three distinct protein-interaction interfaces to assemble functional EphA3 signaling complexes.

摘要

Eph受体酪氨酸激酶(Ephs)作为分子中继器,与细胞表面结合的ephrin配体相互作用,以指导迁移细胞的位置。结构研究表明,通过每种蛋白质相对位点上的两个不同接触表面,Eph和ephrin结合域组装成对称的圆形异四聚体。然而,Eph信号起始需要更高阶寡聚体的组装,这表明存在其他接触点。通过筛选EphA3结合受损的ephrin-A5突变体的随机文库,我们现在确定了对高亲和力EphA3信号复合物组装至关重要的ephrin-A5残基。除了从同源EphB2.ephrin-B2复合物的晶体结构预测的两个界面外,我们还在ephrin-A5的Eα螺旋、E-F环、下方的Hβ链以及附近的B-C环上鉴定出一组10个残基,这些残基定义了EphA3信号寡聚化和激活所需的一个独特的第三表面。与最近在EphA3最小ephrin结合域之外鉴定的相应第三表面区域一起,我们的研究结果为三个不同的蛋白质-相互作用界面在组装功能性EphA3信号复合物中的重要贡献提供了实验证据。

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