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与VLA-2相关的血小板表面胶原结合复合物的分离与鉴定。

Isolation and characterization of a platelet surface collagen binding complex related to VLA-2.

作者信息

Santoro S A, Rajpara S M, Staatz W D, Woods V L

机构信息

Division of Laboratory Medicine, Washington University School of Medicine, St. Louis, Missouri 63110.

出版信息

Biochem Biophys Res Commun. 1988 May 31;153(1):217-23. doi: 10.1016/s0006-291x(88)81211-7.

Abstract

A heterodimeric, Mg++-dependent, collagen binding protein has been isolated from platelet membranes. Electrophoretic properties and monoclonal antibody reactivity indicate that the heavy chain of the complex is platelet membrane glycoprotein Ia and that the light chain is glycoprotein IIa. Furthermore, the receptor appears to be identical with the recently defined VLA-2 complex found on activated T-lymphocytes, platelets and other cells. When incorporated into liposomes, the purified complex mediates the Mg++-dependent adhesion of the liposomes to collagen substrates. These observations suggest that the VLA-2 complex mediates cellular adhesion to collagen in platelets and possibly in other cells.

摘要

一种异源二聚体、依赖Mg++的胶原结合蛋白已从血小板膜中分离出来。电泳特性和单克隆抗体反应性表明,该复合物的重链是血小板膜糖蛋白Ia,轻链是糖蛋白IIa。此外,该受体似乎与最近在活化的T淋巴细胞、血小板和其他细胞上发现的VLA-2复合物相同。当掺入脂质体中时,纯化的复合物介导脂质体对胶原底物的Mg++依赖性黏附。这些观察结果表明,VLA-2复合物介导血小板以及可能其他细胞与胶原的细胞黏附。

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