首页> 外文期刊>Thrombosis Research: An International Journal on Vascular Obstruction, Hemorrhage and Hemostasis >The stratification of platelet reactivity and activation in patients with stable coronary artery disease on aspirin therapy.
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The stratification of platelet reactivity and activation in patients with stable coronary artery disease on aspirin therapy.

机译:阿司匹林治疗稳定型冠心病患者的血小板反应性和活化分层。

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摘要

Heightened platelet reactivity may affect the occurrence of ischemic events in patients with coronary artery disease on aspirin therapy. However, a definition to stratify platelet reactivity in this group of patients has not been previously reported. We studied platelet reactivity and activation by measuring platelet aggregation and the expression of p-selectin, total GP IIb/IIIa and active GP IIb/IIIa (n=96). Patients were divided into quartiles by each of the markers; correlations were made between the markers; and a definition of heightened platelet reactivity was proposed. Marked variability in activation and reactivity were observed despite aspirin therapy. BACKGROUND: Heightened platelet reactivity and activation may affect the occurrence of ischemic events in patients with coronary artery disease on aspirin therapy. However, a definition to stratify platelet reactivity has not been previously reported. METHODS AND RESULTS: Platelet aggregation (5 and 20 micromol/l ADP), total GP IIb/IIIa, activeGP IIb/IIIa and the expression of maximally stimulated p-selectin were measured in patients about to undergo elective coronary stenting (n=96). All patients had received aspirin (325 mg). There was marked variability in platelet reactivity and activation as measured by all markers. The highest quartile was defined by 77+/-1% and 98+/-1% aggregation by 5 and 20 micromol/l ADP, respectively; 65+/-2% p-selectin positivity; 508+/-15 MFI for total GP IIb/IIIa; and 23.0+/-1.8 MFI for active GP IIb/IIIa. CONCLUSIONS: There is a wide range in platelet reactivity and activation as measured by multiple markers in stable coronary disease patients on aspirin therapy. From these indices, we can define those patients at the extremes of reactivity and activation and thus, the greatest potential risk of thrombosis and bleeding. These indices will serve as a guide to future studies investigating the relationships of platelet reactivity, activation, drug-induced inhibition and clinical outcomes.
机译:服用阿司匹林治疗的冠心病患者血小板反应性升高可能会影响缺血事件的发生。但是,先前尚未报道在该组患者中分层血小板反应性的定义。我们通过测量血小板聚集和p-选择素,总GP IIb / IIIa和活性GP IIb / IIIa(n = 96)的表达来研究血小板反应性和活化。通过每个标记将患者分为四分位数;标记之间存在相关性;并提出了提高血小板反应性的定义。尽管进行了阿司匹林治疗,但仍观察到活化和反应性明显变化。背景:阿司匹林治疗后冠状动脉疾病患者血小板反应性和活化的增强可能会影响缺血事件的发生。但是,先前尚未报道过分层血小板反应性的定义。方法和结果:在即将进行选择性冠状动脉支架置入术的患者中(n = 96)测量了血小板聚集(5和20微摩尔/升ADP),总GP IIb / IIIa,activeGP IIb / IIIa和最大刺激的p选择素的表达。所有患者均接受了阿司匹林(325毫克)。如通过所有标记物所测量的,血小板反应性和活化存在明显的可变性。最高四分位数分别由5和20 micromol / l ADP的77 +/- 1%和98 +/- 1%的聚集定义; p-选择素阳性率为65 +/- 2%;总GP IIb / IIIa的508 +/- 15 MFI;有源GP IIb / IIIa的23.0 +/- 1.8 MFI。结论:通过多种标记物在稳定的冠心病患者中接受阿司匹林治疗后,血小板反应性和激活范围广泛。从这些指标,我们可以将那些患者定义为处于反应性和激活性极端状态,从而将血栓形成和出血的最大潜在风险定义为那些患者。这些指数将作为今后研究血小板反应性,活化,药物诱导的抑制作用和临床结果之间关系的指南。

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