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血小板生物学和功能:新概念和临床视角。

Platelet biology and functions: new concepts and clinical perspectives.

机构信息

Department of Biochemistry, Cardiovascular Research Institute Maastricht (CARIM), Maastricht University, Maastricht, The Netherlands.

出版信息

Nat Rev Cardiol. 2019 Mar;16(3):166-179. doi: 10.1038/s41569-018-0110-0.


DOI:10.1038/s41569-018-0110-0
PMID:30429532
Abstract

Platelets - blood cells continuously produced from megakaryocytes mainly in the bone marrow - are implicated not only in haemostasis and arterial thrombosis, but also in other physiological and pathophysiological processes. This Review describes current evidence for the heterogeneity in platelet structure, age, and activation properties, with consequences for a diversity of platelet functions. Signalling processes of platelet populations involved in thrombus formation with ongoing coagulation are well understood. Genetic approaches have provided information on multiple genes related to normal haemostasis, such as those encoding receptors and signalling or secretory proteins, that determine platelet count and/or responsiveness. As highly responsive and secretory cells, platelets can alter the environment through the release of growth factors, chemokines, coagulant factors, RNA species, and extracellular vesicles. Conversely, platelets will also adapt to their environment. In disease states, platelets can be positively primed to reach a pre-activated condition. At the inflamed vessel wall, platelets interact with leukocytes and the coagulation system, interactions mediating thromboinflammation. With current antiplatelet therapies invariably causing bleeding as an undesired adverse effect, novel therapies can be more beneficial if directed against specific platelet responses, populations, interactions, or priming conditions. On the basis of these novel concepts and processes, we discuss several initiatives to target platelets therapeutically.

摘要

血小板是由骨髓中的巨核细胞不断产生的血细胞,不仅参与止血和动脉血栓形成,还参与其他生理和病理生理过程。这篇综述描述了目前关于血小板结构、年龄和激活特性的异质性的证据,这对血小板功能的多样性有影响。与持续凝血相关的血栓形成中血小板群体的信号转导过程已得到充分理解。遗传方法提供了有关与正常止血相关的多种基因的信息,如编码受体和信号或分泌蛋白的基因,这些基因决定了血小板的数量和/或反应性。作为高度反应性和分泌性细胞,血小板可以通过释放生长因子、趋化因子、凝血因子、RNA 种类和细胞外囊泡来改变环境。相反,血小板也会适应其环境。在疾病状态下,血小板可以被正向预激活到预先激活的状态。在炎症血管壁上,血小板与白细胞和凝血系统相互作用,这些相互作用介导血栓炎症。由于目前的抗血小板治疗不可避免地导致出血作为一种不良的不良反应,针对特定的血小板反应、群体、相互作用或预激活条件的新型治疗方法可能更有益。基于这些新的概念和过程,我们讨论了几种靶向血小板治疗的策略。

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[7]
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[8]
Impaired Secondary Platelet Response in Chronic Kidney Disease as a Consequence of Prior Platelet Activation.

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