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异源转染的CV-1细胞中含血管性血友病因子细胞器的生物发生

Biogenesis of von Willebrand factor-containing organelles in heterologous transfected CV-1 cells.

作者信息

Voorberg J, Fontijn R, Calafat J, Janssen H, van Mourik J A, Pannekoek H

机构信息

Department of Molecular Biology and Blood Coagulation, Central Laboratory, The Netherlands Red Cross Blood Transfusion Service, Amsterdam.

出版信息

EMBO J. 1993 Feb;12(2):749-58. doi: 10.1002/j.1460-2075.1993.tb05709.x.

Abstract

Von Willebrand factor (vWF) is a multimeric protein involved in the adhesion of platelets to an injured vessel wall. vWF is synthesized by the endothelial cell and the megakaryocyte as a precursor protein (pro-vWF) that consists of four repeated domains, denoted D1-D2-D'-D3-A1-A2-A3-D4-B1-B2-B3-C1-C2. Previously, we have defined the domains on the pro-vWF molecule involved in dimerization as well as the domains involved in multimer assembly of vWF dimers. In the endothelial cell, part of the vWF multimers is stored in specialized organelles, the Weibel-Palade bodies. By using immunoelectron microscopy, we demonstrate that upon expression of full-length vWF cDNA, vWF-containing organelles are encountered in monkey kidney CV-1 cells that are morphologically similar to the endothelial-specific Weibel-Palade bodies. Expression in CV-1 cells of a series of vWF cDNA deletion mutants, lacking one or more domains, revealed that only those vWF mutant proteins that are able to assemble into multimers are encountered in dense-cored vesicles. Our data show that this process is independent of a particular domain on vWF and indicate that a 'condensed', multimeric vWF is required for targeting to the Weibel-Palade body.

摘要

血管性血友病因子(vWF)是一种多聚体蛋白,参与血小板与受损血管壁的黏附。vWF由内皮细胞和巨核细胞合成为前体蛋白(前vWF),其由四个重复结构域组成,分别为D1-D2-D'-D3-A1-A2-A3-D4-B1-B2-B3-C1-C2。此前,我们已确定了前vWF分子中参与二聚化的结构域以及参与vWF二聚体多聚体组装的结构域。在内皮细胞中,部分vWF多聚体储存在特殊的细胞器——魏尔-帕拉德小体中。通过免疫电子显微镜技术,我们证明,在全长vWF cDNA表达后,在猴肾CV-1细胞中会出现含vWF的细胞器,其形态与内皮细胞特异性的魏尔-帕拉德小体相似。在CV-1细胞中表达一系列缺失一个或多个结构域的vWF cDNA缺失突变体,结果显示,只有那些能够组装成多聚体的vWF突变蛋白才会出现在致密核心囊泡中。我们的数据表明,这一过程独立于vWF上的特定结构域,并表明靶向魏尔-帕拉德小体需要“浓缩的”多聚体vWF。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7dfd/413262/cbdd3c1d26d8/emboj00074-0369-a.jpg

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