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血管性血友病因子与内皮细胞

von Willebrand factor and the endothelium.

作者信息

Wagner D D, Bonfanti R

机构信息

Center of Hemostasis and Thrombosis Research, New England Medical Center, Boston, Massachusetts.

出版信息

Mayo Clin Proc. 1991 Jun;66(6):621-7. doi: 10.1016/s0025-6196(12)60522-9.

Abstract

Endothelial cells are the principal source of plasma and basement membrane von Willebrand factor (vWF). To arrive at its biologically active multimeric form, vWF undergoes a series of intracellular processing steps. The protein is synthesized as a large precursor pro-vWF, which dimerizes in the endoplasmic reticulum through disulfide bonds located in the carboxyl-terminal portion of the subunit. Only dimers are transported to the Golgi apparatus. Expression of truncated pro-vWF subunits, which lack the last 20 kd, abolishes the requirement for dimerization and thereby allows the monomeric protein to be secreted. Another requirement for intracellular transport from the endoplasmic reticulum is N-linked glycosylation. Inhibition of N-linked glycosylation prevents exit of both the wild-type and the truncated vWF from the endoplasmic reticulum. In the acidic environment of the trans-Golgi and post-Golgi compartments, pro-vWF dimers multimerize by a second set of interchain disulfide bonds. The presence of the vWF propolypeptide and acidic pH conditions are necessary for the multimerization process. The largest vWF multimers are stored in endothelial cell-specific organelles called Weibel-Palade bodies. At the site of vascular injury and inflammation, physiologic secretagogues such as thrombin, fibrin, and histamine may cause release of these large, biologically potent vWF multimers from the Weibel-Palade bodies into the surrounding blood and subendothelium.

摘要

内皮细胞是血浆和基底膜血管性血友病因子(vWF)的主要来源。为了形成其具有生物活性的多聚体形式,vWF经历了一系列细胞内加工步骤。该蛋白作为一种大的前体蛋白原vWF被合成,它在内质网中通过位于亚基羧基末端部分的二硫键形成二聚体。只有二聚体被转运到高尔基体。缺乏最后20kd的截短型蛋白原vWF亚基的表达消除了二聚化的需求,从而使单体蛋白能够被分泌。从内质网进行细胞内运输的另一个要求是N-连接糖基化。抑制N-连接糖基化会阻止野生型和截短型vWF从内质网中排出。在反式高尔基体和高尔基体后区室的酸性环境中,蛋白原vWF二聚体通过另一组链间二硫键形成多聚体。vWF前肽的存在和酸性pH条件对于多聚化过程是必需的。最大的vWF多聚体储存在称为魏尔-帕拉德小体的内皮细胞特异性细胞器中。在血管损伤和炎症部位,诸如凝血酶、纤维蛋白和组胺等生理性促分泌剂可能导致这些大的、具有生物活性的vWF多聚体从魏尔-帕拉德小体释放到周围血液和内皮下。

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