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通过载体蛋白驱动结晶获得的纤维蛋白原γ链整合素结合位点和因子XIIIa交联位点的结构

Structure of the fibrinogen gamma-chain integrin binding and factor XIIIa cross-linking sites obtained through carrier protein driven crystallization.

作者信息

Ware S, Donahue J P, Hawiger J, Anderson W F

机构信息

Department of Molecular Pharmacology and Biological Chemistry, Northwestern University Medical School, Chicago, Illinois 60611, USA.

出版信息

Protein Sci. 1999 Dec;8(12):2663-71. doi: 10.1110/ps.8.12.2663.

Abstract

The human fibrinogen gamma-chain C-terminal segment functions as the platelet integrin binding site as well as the Factor XIIIa cross-linking substrate and thus plays an important role in blood clot formation and stabilization. The three-dimensional structure of this segment has been determined using carrier protein driven crystallization. The C-terminal segment, gamma-(398-411), was attached to a linker sequence at the C-terminus of glutathione S-transferase and the structure of this fusion protein determined at 1.8 A resolution. Functional studies of the chimeric protein demonstrate that the fibrinogen sequence in the presence of the carrier protein retains its specific functions as ligand for platelet integrin alpha(IIb)beta3 (gpIIb/IIIa) and as a cross-linking substrate for Factor XIIIa. The structure obtained for the fibrinogen gamma-chain segment is not affected by crystal packing and can provide the missing links to the recently reported model of cross-linked fibrin.

摘要

人纤维蛋白原γ链C末端片段作为血小板整合素结合位点以及因子XIIIa交联底物发挥作用,因此在血凝块形成和稳定过程中起重要作用。该片段的三维结构已通过载体蛋白驱动结晶法确定。C末端片段γ-(398 - 411)连接到谷胱甘肽S-转移酶C末端的接头序列上,并以1.8埃分辨率确定了该融合蛋白的结构。对嵌合蛋白的功能研究表明,在载体蛋白存在下,纤维蛋白原序列保留了其作为血小板整合素α(IIb)β3(糖蛋白IIb/IIIa)配体以及因子XIIIa交联底物的特定功能。获得的纤维蛋白原γ链片段结构不受晶体堆积的影响,可为最近报道的交联纤维蛋白模型提供缺失的环节。

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