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血小板糖蛋白 IIIa PlA 多态性与血小板活性增高在接受阿司匹林治疗的稳定型冠心病的突尼斯患者中的关系。

The GPIIIa PlA polymorphism and the platelet hyperactivity in Tunisian patients with stable coronary artery disease treated with aspirin.

机构信息

Haematology's Laboratory; Fattouma Bourguiba University Hospital, Monastir, Tunisia.

出版信息

Thromb Res. 2010 Jun;125(6):e265-8. doi: 10.1016/j.thromres.2010.01.011.

DOI:10.1016/j.thromres.2010.01.011
PMID:20138334
Abstract

BACKGROUND

Various genetic polymorphisms have been proposed to explain the persistent platelet hyperactivity (HPR) under aspirin treatment. PlA polymorphism of platelet GPIIIa receptor has been largely studied. However, its influence on platelet sensitivity to aspirin remains controversial.

OBJECTIVES

The aim of this prospective study is to investigate whether this PlA polymorphism is associated with a greater prevalence of HPR in stable coronary artery disease patients Material and Methods: 188 stable coronary artery disease patients were included. Platelet aspirin inhibitory effect was determined with PFA-100 using Collagen/Epinephrine closure time (CEPI-CT). A CEPI-CT<160sec was defining the HPR status. GPIIIa PlA polymorphism was established using polymerase chain reaction and classical restriction fragments length polymorphism.

RESULTS

The observed frequencies of different genotypes were not different from those predicted by the Hardy-Weinberg equilibrium: PlA1/lA1 (55.3%), PlA1/PlA2 (39.4%) and PlA2/PlA2 (5.3%). HPR patients with inadequate aspirin inhibition were significantly more often homozygous PlA1/A1 (65.4% vs. 47.7%, p=0.015). After multivariate analysis, PlA1/A1 genotype was the only independent risk factor for persistent HPR (OR: 2.07; 95% CI [1.14 to 3.76; p=0.016).

CONCLUSION

In CAD patients receiving daily low dose of aspirin, there is a significant and independent association between the expression of GPIIIa PlA1 allele and the occurrence of persistent HPR detected with PFA-100.

摘要

背景

各种遗传多态性被认为可以解释阿司匹林治疗下持续的血小板高反应性(HPR)。血小板糖蛋白 IIIa 受体的 PlA 多态性已被广泛研究。然而,其对血小板对阿司匹林敏感性的影响仍存在争议。

目的

本前瞻性研究旨在探讨血小板糖蛋白 IIIa 受体 PlA 多态性是否与稳定型冠状动脉疾病患者中 HPR 的发生率较高有关。

材料和方法

共纳入 188 例稳定型冠状动脉疾病患者。使用 PFA-100 通过胶原/肾上腺素封闭时间(CEPI-CT)测定血小板对阿司匹林的抑制作用。CEPI-CT<160sec 定义为 HPR 状态。使用聚合酶链反应和经典限制性片段长度多态性确定 GPIIIa PlA 多态性。

结果

观察到的不同基因型的频率与 Hardy-Weinberg 平衡预测的频率无差异:PlA1/lA1(55.3%)、PlA1/PlA2(39.4%)和 PlA2/PlA2(5.3%)。阿司匹林抑制不足的 HPR 患者 PlA1/A1 纯合子明显更多(65.4%比 47.7%,p=0.015)。多变量分析后,PlA1/A1 基因型是持续 HPR 的唯一独立危险因素(OR:2.07;95%CI[1.14 至 3.76;p=0.016])。

结论

在接受每日低剂量阿司匹林治疗的 CAD 患者中,GPIIIa PlA1 等位基因的表达与使用 PFA-100 检测到的持续 HPR 之间存在显著且独立的关联。

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