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纤维蛋白原BβN结构域的结构与功能

Structure and function of fibrinogen BβN-domains.

作者信息

Medved Leonid, Yakovlev Sergiy

机构信息

Center for Vascular and Inflammatory Diseases and Departments of Biochemistry and Molecular Biology, University of Maryland School of Medicine, Baltimore, MD, U.S.A.

出版信息

Ukr Biochem J. 2020 May-Jun;92(3):22-32. doi: 10.15407/ubj92.03.022.

Abstract

Two BβN-domains of fibrinogen are formed by the N-terminal portions of its two Bβ chains including amino acid residues Bβ1-65. Although their folding status is not well understood and the recombinant disulfide-linked (Bβ1-66) fragment corresponding to a pair of these domains was found to be unfolded, some data suggest that these domains may be folded in the parent molecule. In contrast, their major functional properties are well established. Removal of fibrinopeptides B (amino acid residues Bβ1-14) from these domains upon fibrinogen to fibrin conversion results in the exposure of multiple binding sites in fibrin βN-domains (residues β15-65). These sites provide interactions of the βN-domains with different proteins and cells and their participation in various physiological and pathological processes including fibrin assembly, fibrin-dependent angiogenesis, and fibrin-dependent leukocyte transmigration and thereby inflammation. The major goal of the present review is to summarize current view on the structure and function of these domains in fibrinogen and fibrin and their role in the above-mentioned processes.

摘要

纤维蛋白原的两个BβN结构域由其两条Bβ链的N端部分形成,包括氨基酸残基Bβ1-65。尽管它们的折叠状态尚未完全了解,并且发现与一对这些结构域相对应的重组二硫键连接的(Bβ1-66)片段是未折叠的,但一些数据表明这些结构域可能在亲本分子中折叠。相比之下,它们的主要功能特性已得到充分证实。在纤维蛋白原向纤维蛋白转化过程中,从这些结构域中去除纤维蛋白肽B(氨基酸残基Bβ1-14)会导致纤维蛋白βN结构域(残基β15-65)中多个结合位点的暴露。这些位点提供了βN结构域与不同蛋白质和细胞的相互作用,并参与各种生理和病理过程,包括纤维蛋白组装、纤维蛋白依赖性血管生成以及纤维蛋白依赖性白细胞迁移,进而引发炎症。本综述的主要目的是总结当前关于这些结构域在纤维蛋白原和纤维蛋白中的结构和功能及其在上述过程中作用的观点。

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