首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Adhesive receptor Mac-1 coordinates the activation of factor X on stimulated cells of monocytic and myeloid differentiation: an alternative initiation of the coagulation protease cascade.
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Adhesive receptor Mac-1 coordinates the activation of factor X on stimulated cells of monocytic and myeloid differentiation: an alternative initiation of the coagulation protease cascade.

机译:粘附受体Mac-1协调单核细胞和髓样分化刺激细胞上X因子的活化:凝血蛋白酶级联反应的另一种起始方式。

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摘要

Monocytes initiate coagulation through regulated surface expression of tissue factor and local assembly of a proteolytic enzymatic complex formed by tissue factor and factor VII/activated factor VII. We now show that, in the absence of these initiating molecules, monocytes and cell lines of monocytic/myeloid differentiation can alternatively initiate coagulation after exposure to ADP. The molecular basis for this procoagulant response consists of two distinct events. First, cell stimulation with ADP induces high-affinity binding of coagulation factor X to the surface-adhesive receptor Mac-1. Locally, Mac-1-concentrated factor X is then rapidly proteolytically cleaved to an active protease with size and activity characteristics of activated factor X, which supports the cell-associated formation of thrombin and the procoagulant response. We conclude that the monocytic/myeloid adhesive receptor Mac-1 has the unexpected, specifically inducible property to organize a molecular assembly culminating in rapid fibrin formation that is independently regulated from tissue factor and factor VII/activated factor VII.
机译:单核细胞通过调节的组织因子表面表达和由组织因子和因子VII /活化因子VII形成的蛋白水解酶复合物的局部组装来启动凝血。我们现在表明,在没有这些起始分子的情况下,单核细胞/骨髓分化的单核细胞和细胞系可以替代性地在暴露于ADP后启动凝血。这种促凝血反应的分子基础包括两个不同的事件。首先,用ADP刺激细胞会诱导凝血因子X与表面粘附受体Mac-1高亲和力结合。然后,将Mac-1浓缩因子X局部快速蛋白水解切割为具有活化因子X大小和活性特征的活性蛋白酶,该蛋白酶支持细胞相关凝血酶的形成和促凝血反应。我们得出的结论是,单核细胞/髓样粘附受体Mac-1具有意想不到的,特别可诱导的特性,可以组织分子组装,最终形成快速的血纤蛋白,而不受组织因子和因子VII /活化的因子VII的调节。

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