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Hemostatic and signaling functions of transfused platelets.

机译:输血血小板的止血和信号传导功能。

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摘要

Metabolic studies have revealed a gradual impairment in platelet integrity during storage, a process termed the platelet storage lesion. Recent evidence shows that stored platelets also lose signaling responses to physiological agonists with impaired integrin activation, secretion, and aggregation of the cells. On the other hand, storage leads to a gain in platelet activation properties, such as release of microparticles and appearance of surface epitopes for their clearance by macrophages. New techniques for measuring flow-induced thrombus formation and platelet-dependent coagulation provide evidence that the hemostatic activity of platelets decreases during storage. Besides pharmacological inhibition, novel storage strategies, like metabolic suppression, should be considered to better preserve platelet functionality while limiting the expression of clearance markers. Understanding the changes that occur in association with the platelet storage lesion and the use of updated storage methods will help to generate platelets for transfusion with optimal hemostatic function and a long circulation time after transfusion.
机译:代谢研究表明,储存过程中血小板完整性逐渐受损,这一过程称为血小板储存病变。最近的证据表明,储存的血小板还会丧失对整合素激活,分泌和细胞聚集受损的生理激动剂的信号响应。另一方面,储存导致血小板活化性质的增加,例如微粒的释放和表面表位的出现,以被巨噬细胞清除。测量血流诱导的血栓形成和血小板依赖性凝血的新技术提供了证据,表明在储存过程中血小板的止血活性降低。除了药理学抑制作用外,还应考虑使用新的存储策略(例如代谢抑制)来更好地保存血小板功能,同时限制清除标记的表达。了解与血小板存储病变有关的变化以及使用更新的存储方法将有助于生成具有最佳止血功能且输血后循环时间长的血小板用于输血。

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