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Microparticles in vascular diseases.

机译:血管疾病中的微粒。

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摘要

Cellular microparticles (MP) are small membrane vesicles that are released from cells upon activation or apoptosis. They constitute a heterogeneous population of submicron elements differing in cellular origin, number, size, antigenic composition and functional properties. Circulating MP provide an additional procoagulant phospholipid surface enabling the assembly of the clotting enzyme complexes and thrombin generation. Their procoagulant properties rely on the exposure of phosphatidylserine and on the possible presence of tissue factor, the main initiator of blood coagulation. Microparticles constitute the main reservoir of blood-borne tissue factor. Derived from various cells, most notably platelets, erythrocytes, leucocytes and endothelial cells, circulating MP are detectable in the circulation of healthy subjects. Elevated levels are encountered in diseases with vascular involvement and hypercoagulability such as disseminated intravascular coagulation, diabetes, immune-mediated thrombosis, kidney diseases, acute coronary syndromes or systemic inflammatory disease, where they appear indicative of a poor clinical outcome. Converging evidence from experimental and clinical data underlines an involvement of procoagulant MP in the initiation/dissemination of procoagulant and inflammatory responses. In these clinical settings, the pharmacological modulation of MP level or activity provides challenging issues.
机译:细胞微粒(MP)是小的膜小泡,在激活或凋亡后会从细胞中释放出来。它们构成细胞来源,数量,大小,抗原组成和功能特性不同的亚微米元素异质群体。循环MP提供了一个额外的促凝血磷脂表面,使凝血酶复合物的组装和凝血酶的产生成为可能。它们的促凝特性取决于磷脂酰丝氨酸的暴露以及可能是血液凝结的主要引发剂的组织因子的存在。微粒构成血液传播的组织因子的主要储存库。源自各种细胞,最明显的是血小板,红细胞,白细胞和内皮细胞,在健康受试者的循环中可检测到循环MP。在具有血管受累和高凝性的疾病(例如弥散性血管内凝血,糖尿病,免疫介导的血栓形成,肾脏疾病,急性冠状动脉综合征或全身性炎症性疾病)中,其水平升高,它们似乎表明临床结果较差。来自实验和临床数据的越来越多的证据强调,促凝剂MP参与促凝剂和炎症反应的启动/传播。在这些临床环境中,MP水平或活性的药理学调节提供了具有挑战性的问题。

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