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弹性蛋白肽 VGVAPG 与人弹性蛋白结合蛋白的相互作用。

Interaction between the elastin peptide VGVAPG and human elastin binding protein.

机构信息

Laboratoire de Signalisation et Récepteurs Matriciels, FRE CNRS 3184, Université de Reims Champagne Ardenne, UFR Sciences Exactes et Naturelles, Moulin de la Housse, BP 1039, 51687 Reims Cedex 2, France.

出版信息

J Biol Chem. 2013 Jan 11;288(2):1317-28. doi: 10.1074/jbc.M112.419929. Epub 2012 Nov 19.

Abstract

The elastin binding protein (EBP), a spliced variant of lysosomal β-galactosidase, is the primary receptor of elastin peptides that have been linked to emphysema, aneurysm and cancer progression. The sequences recognized by EBP share the XGXXPG consensus pattern found in numerous matrix proteins, notably in elastin where the VGVAPG motif is repeated. To delineate the elastin binding site of human EBP, we built a homology model of this protein and docked VGVAPG on its surface. Analysis of this model suggested that Gln-97 and Asp-98 were required for interaction with VGVAPG because they contribute to the definition of a pocket thought to represent the elastin binding site of EBP. Additionally, we proposed that Leu-103, Arg-107, and Glu-137 were essential residues because they could interact with VGVAPG itself. Site-directed mutagenesis experiments at these key positions validated our model. This work therefore provides the first structural data concerning the interaction of the VGVAPG with its cognate receptor. The present structural data should now allow the development of EBP-specific antagonists.

摘要

弹性蛋白结合蛋白(EBP)是溶酶体β-半乳糖苷酶的剪接变体,是与肺气肿、动脉瘤和癌症进展相关的弹性肽的主要受体。EBP 识别的序列具有在许多基质蛋白中发现的 XGXXPG 共识模式,特别是在弹性蛋白中,VGVAPG 基序重复出现。为了描绘人 EBP 的弹性蛋白结合位点,我们构建了该蛋白的同源模型,并在其表面对接 VGVAPG。该模型的分析表明,由于 Gln-97 和 Asp-98 有助于定义一个口袋,该口袋被认为代表 EBP 的弹性蛋白结合位点,因此它们与 VGVAPG 的相互作用是必需的。此外,我们提出 Leu-103、Arg-107 和 Glu-137 是必需残基,因为它们可以与 VGVAPG 本身相互作用。在这些关键位置进行的定点突变实验验证了我们的模型。因此,这项工作首次提供了关于 VGVAPG 与其同源受体相互作用的结构数据。目前的结构数据现在应该允许开发 EBP 特异性拮抗剂。

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