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Polyphosphate nanoparticles on the platelet surface trigger contact system activation

机译:在血小板表面触发器接触系统激活的多磷酸纳米粒子

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摘要

Polyphosphate is an inorganic polymer that can potentiate several interactions in the blood coagulation system. Blood platelets contain polyphosphate, and the secretion of platelet-derived polyphosphate has been associated with increased thrombus formation and activation of coagulation factor XII. However, the small polymer size of secreted platelet polyphosphate limits its capacity to activate factor XII in vitro. Thus, the mechanism by which platelet polyphosphate contributes to thrombus formation remains unclear. Using live-cell imaging, confocal and electron microscopy, we show that activated platelets retain polyphosphate on their cell surface. The apparent polymer size of membrane-associated polyphosphate largely exceeds that of secreted polyphosphate. Ultracentrifugation fractionation experiments revealed that membrane-associated platelet polyphosphate is condensed into insoluble spherical nanoparticles with divalent metal ions. In contrast to soluble polyphosphate, membrane-associated polyphosphate nanoparticles potently activate factor XII. Our findings identify membrane-associated polyphosphate in a nanoparticle state on the surface of activated platelets. We propose that these polyphosphate nanoparticles mechanistically link the procoagulant activity of platelets with the activation of coagulation factor XII.
机译:多磷酸盐是一种无机聚合物,可使血液凝固系统中的几种相互作用。血小血小板含有多磷酸盐,并且血小板衍生的多磷酸盐的分泌与血栓形成和凝血因子XII的激活有关。然而,分泌的血小板多磷酸盐的小聚合物尺寸限制了其在体外激活因子XII的能力。因此,血小板多磷酸磷酸含有血栓形成的机制仍不清楚。使用直接细胞成像,共焦和电子显微镜,我们表明活性血小板在其细胞表面保持多磷酸盐。膜相关多磷酸盐的表观聚合物尺寸在很大程度上超过分泌的多磷酸盐。超速离心分馏实验表明,膜相关的血小磷酸盐用二价金属离子缩合到不溶性球形纳米颗粒中。与可溶性多磷酸盐,膜相关多磷酸纳米粒子尤其激活因子XII。我们的研究结果鉴定了在活性血小板表面上的纳米颗粒状态下的膜相关的多磷酸磷酸。我们提出这些多磷酸纳米粒子将血小板的血小杂化活性与凝固因子XII的激活机械化。

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