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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >New Insights Into the spatiotemporal localization of prothrombinase in vivo
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New Insights Into the spatiotemporal localization of prothrombinase in vivo

机译:凝血酶原在体内时空定位的新见解

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摘要

The membrane-dependent interaction of factor Xa (FXa) with factor Va (FVa) forms prothrombinase and drives thrombin formation essential for hemostasis. Activated platelets are considered to provide the primary biological surface to support prothrombinase function. However, the question of how other eel! types may cooperate within the biological milieu to affect hemostatic plug formation remains unaddressed. We used confocal fluorescence microscopy to image the distribution of site-specific fluorescent derivatives of FVa and FXa after laser injury in the mouse cremaster arteriole. These proteins bound to the injury site extend beyond the platelet mass to the surrounding endotheiium. Although bound FVa and FXa may have been present on the platelet core at the nidus of the injury, bound proteins were not evident on platelets adherent even a small distance from the injury site. Manipulations to drastically reduce adherent platelets yielded a surprisingly modest decrease in bound FXa and FVa with little impact on fibrin formation. Thus, platelets adherent to the site of vascular injury do not play the presumed preeminent role in supporting prothrombinase assembly and thrombin formation. Rather, the damaged/ activated endotheiium and possibly other blood cells play an unexpectedly important role in providing a procoagulant membrane surface in vivo.
机译:Xa因子(FXa)与Va因子(FVa)的膜依赖性相互作用形成凝血酶原酶并驱动凝血酶形成,这对于止血至关重要。活化的血小板被认为提供了支持凝血酶原功能的主要生物表面。但是,其他鳗鱼的问题!类型可能在生物学环境中协同作用以影响止血栓的形成,但仍未解决。我们使用共聚焦荧光显微镜对小鼠提睾小动脉激光损伤后FVa和FXa的位点特异性荧光衍生物的分布进行成像。结合到损伤部位的这些蛋白质延伸超过血小板块,到达周围的内皮。尽管结合的FVa和FXa可能已经存在于损伤部位的血小板核上,但是即使离损伤部位只有很小的距离,结合蛋白在粘附的血小板上也不明显。大幅减少粘附血小板的操作使结合的FXa和FVa出乎意料地适度降低,而对血纤蛋白的形成影响很小。因此,粘附在血管损伤部位的血小板在支持凝血酶原酶组装和凝血酶形成中不发挥推测的重要作用。而是,受损/激活的内皮和可能的其他血细胞在体内提供促凝血膜表面方面起着意想不到的重要作用。

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