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人肽聚糖识别蛋白S(PGRP-S)在1.70埃分辨率下的晶体结构。

Crystal structure of human peptidoglycan recognition protein S (PGRP-S) at 1.70 A resolution.

作者信息

Guan Rongjin, Wang Qian, Sundberg Eric J, Mariuzza Roy A

机构信息

Center for Advanced Research in Biotechnology, W. M. Keck Laboratory for Structural Biology, University of Maryland Biotechnology Institute, Rockville, MD 20850, USA.

出版信息

J Mol Biol. 2005 Apr 8;347(4):683-91. doi: 10.1016/j.jmb.2005.01.070.

DOI:10.1016/j.jmb.2005.01.070
PMID:15769462
Abstract

Peptidoglycan recognition proteins (PGRPs) are pattern recognition receptors of the innate immune system that bind peptidoglycans (PGNs) of bacterial cell walls. These molecules, which are highly conserved from insects to mammals, contribute to host defense against infections by both Gram-positive and Gram-negative bacteria. Here, we present the crystal structure of human PGRP-S at 1.70A resolution. The overall structure of PGRP-S, which participates in intracellular killing of Gram-positive bacteria, is similar to that of other PGRPs, including Drosophila PGRP-LB and PGRP-SA and human PGRP-Ialpha. However, comparison with these PGRPs reveals important differences in both the PGN-binding site and a groove formed by the PGRP-specific segment on the opposite face of the molecule. This groove, which may constitute a binding site for effector or signaling proteins, is less hydrophobic and deeper in PGRP-S than in PGRP-IalphaC, whose PGRP-specific segments vary considerably in amino acid sequence. By docking a PGN ligand into the PGN-binding cleft of PGRP-S based on the known structure of a PGRP-Ialpha-PGN complex, we identified potential PGN-binding residues in PGRP-S. Differences in PGN-contacting residues and interactions suggest that, although PGRPs may engage PGNs in a similar mode, structural differences exist that likely regulate the affinity and fine specificity of PGN recognition.

摘要

肽聚糖识别蛋白(PGRPs)是先天性免疫系统的模式识别受体,可结合细菌细胞壁的肽聚糖(PGNs)。这些分子在从昆虫到哺乳动物的物种中高度保守,有助于宿主抵御革兰氏阳性菌和革兰氏阴性菌的感染。在此,我们展示了分辨率为1.70埃的人PGRP-S的晶体结构。参与细胞内杀灭革兰氏阳性菌的PGRP-S的整体结构与其他PGRPs相似,包括果蝇PGRP-LB和PGRP-SA以及人PGRP-Iα。然而,与这些PGRPs的比较揭示了PGN结合位点以及分子相对面上由PGRP特异性片段形成的凹槽存在重要差异。这个凹槽可能构成效应蛋白或信号蛋白的结合位点,与PGRP-IαC相比,PGRP-S中的凹槽疏水性更低且更深,PGRP-IαC的PGRP特异性片段在氨基酸序列上有很大差异。通过基于PGRP-Iα-PGN复合物的已知结构将PGN配体对接至PGRP-S的PGN结合裂隙中,我们确定了PGRP-S中潜在的PGN结合残基。PGN接触残基和相互作用的差异表明,尽管PGRPs可能以类似模式结合PGNs,但存在的结构差异可能会调节PGN识别的亲和力和精细特异性。

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