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ICAM-2的晶体结构揭示了一个独特的整合素识别表面。

Crystal structure of ICAM-2 reveals a distinctive integrin recognition surface.

作者信息

Casasnovas J M, Springer T A, Liu J H, Harrison S C, Wang J H

机构信息

The Center for Blood Research, Harvard Medical School, Department of Pathology, Boston, Massachusetts 02115, USA.

出版信息

Nature. 1997 May 15;387(6630):312-5. doi: 10.1038/387312a0.

DOI:10.1038/387312a0
PMID:9153399
Abstract

Recognition by integrin proteins on the cell surface regulates the adhesive interactions between cells and their surroundings. The structure of the 'I' domain that is found in some but not all integrins, has been determined. However, the only integrin ligands for which structures are known, namely fibronectin and VCAM-1, are recognized by integrins that lack I domains. The intercellular adhesion molecules ICAM-1, 2 and 3 are, like VCAM-1, members of the immunoglobulin superfamily (IgSF), but they are recognized by an I domain-containing integrin, lymphocyte-function-associated antigen 1 (LFA-1, or CD11a/CD18). Here we present the crystal structure of the extracellular region of ICAM-2. The glutamic acid residue at position 37 is critical for LFA-1 binding and is proposed to coordinate the Mg2+ ion in the I domain; this Glu 37 is surrounded by a relatively flat recognition surface and lies in a beta-strand, whereas the critical aspartic acid residue in VCAM-1 and fibronectin lie in protruding loops. This finding suggests that there are differences in the architecture of recognition sites between integrins that contain or lack I domains. A bend between domains 1 and 2 of ICAM-2 and a tripod-like arrangement of N-linked glycans in the membrane-proximal region of domain 2 may be important for presenting the recognition surface to LFA-1. A model of ICAM-1 based on the ICAM-2 structure provides a framework for understanding its recognition by pathogens.

摘要

细胞表面整联蛋白的识别作用调控着细胞与其周围环境之间的黏附相互作用。已确定了某些(但并非全部)整联蛋白中存在的“I”结构域的结构。然而,目前已知结构的整联蛋白配体只有纤连蛋白和血管细胞黏附分子-1(VCAM-1),而它们是由缺乏I结构域的整联蛋白识别的。细胞间黏附分子ICAM-1、ICAM-2和ICAM-3与VCAM-1一样,都是免疫球蛋白超家族(IgSF)成员,但它们是由含I结构域的整联蛋白淋巴细胞功能相关抗原1(LFA-1,即CD11a/CD18)识别的。本文展示了ICAM-2胞外区域的晶体结构。第37位的谷氨酸残基对LFA-1结合至关重要,推测其在I结构域中与Mg2+离子配位;该Glu37被一个相对平坦的识别表面所环绕,位于一条β链中,而VCAM-1和纤连蛋白中的关键天冬氨酸残基则位于突出的环中。这一发现表明,含或不含I结构域的整联蛋白之间识别位点的结构存在差异。ICAM-2的结构域1和结构域2之间的弯曲以及结构域2膜近端区域中N-连接聚糖的三脚架样排列,可能对于将识别表面呈现给LFA-1很重要。基于ICAM-2结构构建的ICAM-1模型为理解病原体对其的识别提供了一个框架。

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