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Eps15-斯顿宁2复合物的结构为EH结构域配体特异性提供了分子解释。

Structure of the Eps15-stonin2 complex provides a molecular explanation for EH-domain ligand specificity.

作者信息

Rumpf Julia, Simon Bernd, Jung Nadja, Maritzen Tanja, Haucke Volker, Sattler Michael, Groemping Yvonne

机构信息

Department of Biomolecular Mechanisms, Max-Planck-Institute for Medical Research, Heidelberg, Germany.

出版信息

EMBO J. 2008 Feb 6;27(3):558-69. doi: 10.1038/sj.emboj.7601980. Epub 2008 Jan 17.

Abstract

Eps15 homology (EH) domain-containing proteins play a key regulatory role in intracellular membrane trafficking and cell signalling. EH domains serve as interaction platforms for short peptide motifs comprising the residues NPF within natively unstructured regions of accessory proteins. The EH-NPF interactions described thus far are of very low affinity and specificity. Here, we identify the presynaptic endocytic sorting adaptor stonin2 as a high-affinity ligand for the second EH domain (EH2) of the clathrin accessory protein Eps15. Calorimetric data indicate that both NPF motifs within stonin2 interact with EH2 simultaneously and with sub-micromolar affinity. The solution structure of this complex reveals that the first NPF motif binds to the conserved site on the EH domain, whereas the second motif inserts into a novel hydrophobic pocket. Our data show how combination of two EH-attachment sites provides a means for modulating specificity and allows discrimination from a large pool of potential binding partners containing NPF motifs.

摘要

含Eps15同源(EH)结构域的蛋白质在细胞内膜运输和细胞信号传导中发挥关键调节作用。EH结构域作为辅助蛋白天然无结构区域内包含NPF残基的短肽基序的相互作用平台。迄今为止描述的EH-NPF相互作用具有非常低的亲和力和特异性。在这里,我们确定突触前内吞分选衔接蛋白stonin2是网格蛋白辅助蛋白Eps15的第二个EH结构域(EH2)的高亲和力配体。量热数据表明,stonin2中的两个NPF基序同时与EH2相互作用,亲和力为亚微摩尔级。该复合物的溶液结构表明,第一个NPF基序与EH结构域上的保守位点结合,而第二个基序插入一个新的疏水口袋。我们的数据展示了两个EH附着位点的组合如何提供一种调节特异性的方式,并允许从大量含有NPF基序的潜在结合伴侣中进行区分。

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