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Sla1p同源结构域1的结构及其与NPFxD内吞内化基序的相互作用。

Structure of Sla1p homology domain 1 and interaction with the NPFxD endocytic internalization motif.

作者信息

Mahadev Ravi K, Di Pietro Santiago M, Olson John M, Piao Hai Lan, Payne Gregory S, Overduin Michael

机构信息

CR-UK Institute for Cancer Studies, School of Medicine, University of Birmingham, Birmingham, UK.

出版信息

EMBO J. 2007 Apr 4;26(7):1963-71. doi: 10.1038/sj.emboj.7601646. Epub 2007 Mar 15.

Abstract

Adaptor proteins play important endocytic roles including recognition of internalization signals in transmembrane cargo. Sla1p serves as the adaptor for uptake of transmembrane proteins containing the NPFxD internalization signal, and is essential for normal functioning of the actin cytoskeleton during endocytosis. The Sla1p homology domain 1 (SHD1) within Sla1p is responsible for recognition of the NPFxD signal. This study presents the NMR structure of the NPFxD-bound state of SHD1 and a model for the protein-ligand complex. The alpha+beta structure of the protein reveals an SH3-like topology with a solvent-exposed hydrophobic ligand binding site. NMR chemical shift perturbations and effects of structure-based mutations on ligand binding in vitro define residues that are key for NPFxD binding. Mutations that abolish ligand recognition in vitro also abolish NPFxD-mediated receptor internalization in vivo. Thus, SHD1 is a novel functional domain based on SH3-like topology, which employs a unique binding site to recognize the NPFxD endocytic internalization signal. Its distant relationship with the SH3 fold endows this superfamily with a new role in endocytosis.

摘要

衔接蛋白发挥着重要的内吞作用,包括识别跨膜货物中的内化信号。Sla1p作为含有NPFxD内化信号的跨膜蛋白摄取的衔接蛋白,对于内吞过程中肌动蛋白细胞骨架的正常功能至关重要。Sla1p中的Sla1p同源结构域1(SHD1)负责识别NPFxD信号。本研究展示了SHD1与NPFxD结合状态的核磁共振结构以及蛋白质-配体复合物的模型。该蛋白质的α+β结构显示出类似SH3的拓扑结构,带有一个溶剂暴露的疏水配体结合位点。核磁共振化学位移扰动以及基于结构的突变对体外配体结合的影响确定了对NPFxD结合至关重要的残基。在体外消除配体识别的突变在体内也消除了NPFxD介导的受体内化。因此,SHD1是基于类似SH3拓扑结构的新型功能结构域,它利用独特的结合位点识别NPFxD内吞内化信号。它与SH3折叠的远亲关系赋予了这个超家族在内吞作用中的新角色。

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