首页> 外文期刊>The Journal of biological chemistry >Structural Characterization of the EphA4-Ephrin-B2 Complex Reveals New Features Enabling Eph-Ephrin Binding Promiscuity*
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Structural Characterization of the EphA4-Ephrin-B2 Complex Reveals New Features Enabling Eph-Ephrin Binding Promiscuity*

机译:EphA4-Ephrin-B2复合体的结构表征揭示了启用Eph-Ephrin结合滥交的新功能*

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EphA and EphB receptors preferentially bind ephrin-A and ephrin-B ligands, respectively, but EphA4 is exceptional for its ability to bind all ephrins. Here, we report the crystal structure of the EphA4 ligand-binding domain in complex with ephrin-B2, which represents the first structure of an EphA-ephrin-B interclass complex. A loose fit of the ephrin-B2 G-H loop in the EphA4 ligand-binding channel is consistent with a relatively weak binding affinity. Additional surface contacts also exist between EphA4 residues Gln12 and Glu14 and ephrin-B2. Mutation of Gln12 and Glu14 does not cause significant structural changes in EphA4 or changes in its affinity for ephrin-A ligands. However, the EphA4 mutant has ~10-fold reduced affinity for ephrin-B ligands, indicating that the surface contacts are critical for interclass but not intraclass ephrin binding. Thus, EphA4 uses different strategies to bind ephrin-A or ephrin-B ligands and achieve binding promiscuity. NMR characterization also suggests that the contacts of Gln12 and Glu14 with ephrin-B2 induce dynamic changes throughout the whole EphA4 ligand-binding domain. Our findings shed light on the distinctive features that enable the remarkable ligand binding promiscuity of EphA4 and suggest that diverse strategies are needed to effectively disrupt different Eph-ephrin complexes.
机译:EphA和EphB受体分别优先结合ephrin-A和ephrin-B配体,但EphA4因其结合所有ephrin的能力而非常出色。在这里,我们报告与ephrin-B2配合物的EphA4配体结合域的晶体结构,它代表EphA-ephrin-B中间类配合物的第一个结构。 ephrin-B2 G-H环在EphA4配体结合通道中的松配合与相对较弱的结合亲和力一致。 EphA4残基Gln12和Glu14与ephrin-B2之间也存在其他表面接触。 Gln12和Glu14的突变不会引起EphA4的明显结构变化或对ephrin-A配体的亲和力变化。然而,EphA4突变体对ephrin-B配体的亲和力降低了约10倍,这表明表面接触对于类别间而不是类别内的ephrin结合至关重要。因此,EphA4使用不同的策略来结合ephrin-A或ephrin-B配体并实现结合滥交。 NMR表征还表明,Gln12和Glu14与ephrin-B2的接触在整个EphA4配体结合域中诱导了动态变化。我们的发现揭示了使EphA4具有显着的配体结合滥交性的独特特征,并表明需要多种策略来有效地破坏不同的Eph-ephrin复合物。

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