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鉴定介导 αX I 结构域和 ICAM-1 相互作用的残基。

Characterization of the residues of αX I-domain and ICAM-1 mediating their interactions.

机构信息

Divisions of Science Education and Biology, Kangwon National University, Chuncheon, 200-701, Korea.

出版信息

Mol Cells. 2010 Sep;30(3):227-34. doi: 10.1007/s10059-010-0111-2. Epub 2010 Aug 23.

Abstract

Integrin αXβ2 performs a significant role in leukocyte functions including phagocytosis and migration, and binds to a variety of ligands, including fibrinogen, iC3b, and ICAM-1. A particular domain of the α subunit of the integrin - the αX I-domain - is a ligand binding site, and the interaction of the αX I-domain and ICAM-1 on the endothelium is an important step in leukocyte extravasation. In order to elucidate the structural aspects of this interaction, we defined the moieties of the αX and ICAM-1 relevant to their interaction in this study. It was determined that the ICAM-1 binding sites of the αX I-domain were located in the α3α4, βDα5, and βFα7 loops at the top surface of the I-domain. The residues Q(202), K(242), K(243), E(298) and D(299) on these loops were crucial for the recognition of ICAM-1. Among these residues, K(242) and K(243) on the βDα5 loop were found to be the most salient, thereby suggesting an ionic interaction between these proteins. Domain 3 of ICAM-1 was identified as a primary binding site for the αX I-domain. Two regions of domain 3 (D(229)QRLNPTV and E(254)DEGTQRL) perform critical functions in the binding of the αX I-domain. Especially, the residue E(254)DEG, is most important with regard to the αX I-domain.

摘要

整合素 αXβ2 在白细胞功能中发挥重要作用,包括吞噬作用和迁移作用,并与多种配体结合,包括纤维蛋白原、iC3b 和 ICAM-1。整合素的 α 亚基的一个特定结构域 - αX I 结构域 - 是一个配体结合位点,αX I 结构域与内皮细胞上的 ICAM-1 的相互作用是白细胞渗出的重要步骤。为了阐明这种相互作用的结构方面,我们在本研究中定义了与相互作用相关的 αX 和 ICAM-1 的部分。确定了 αX I 结构域的 ICAM-1 结合位点位于 I 结构域的顶部表面的 α3α4、βDα5 和 βFα7 环中。这些环上的残基 Q(202)、K(242)、K(243)、E(298)和 D(299)对于识别 ICAM-1 至关重要。在这些残基中,βDα5 环上的 K(242)和 K(243)被发现是最突出的,从而表明这两种蛋白质之间存在离子相互作用。ICAM-1 的结构域 3 被鉴定为与 αX I 结构域的主要结合位点。结构域 3 的两个区域(D(229)QRLNPTV 和 E(254)DEGTQRL)在 αX I 结构域的结合中发挥关键作用。特别是,残基 E(254)DEG 对于 αX I 结构域最为重要。

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