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首页> 外文期刊>Pharmacogenetics and genomics >The functional G143E variant of carboxylesterase 1 is associated with increased clopidogrel active metabolite levels and greater clopidogrel response
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The functional G143E variant of carboxylesterase 1 is associated with increased clopidogrel active metabolite levels and greater clopidogrel response

机译:羧酸酯酶1的功能性G143E变体与氯吡格雷活性代谢物水平增加和氯吡格雷反应性更高相关

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INTRODUCTION: Carboxylesterase 1 (CES1) is the primary enzyme responsible for converting clopidogrel into biologically inactive carboxylic acid metabolites. METHODS: We genotyped a functional variant in CES1, G143E, in participants of the Pharmacogenomics of Anti-Platelet Intervention (PAPI) study (n=566) and in 350 patients with coronary heart disease treated with clopidogrel, and carried out an association analysis of bioactive metabolite levels, on-clopidogrel ADP-stimulated platelet aggregation, and cardiovascular outcomes. RESULTS: The levels of clopidogrel active metabolite were significantly greater in CES1 143E-allele carriers (P=0.001). Consistent with these findings, individuals who carried the CES1 143E-allele showed a better clopidogrel response as measured by ADP-stimulated platelet aggregation in both participants of the PAPI study (P=0.003) and clopidogrel-treated coronary heart disease patients (P=0.03). No association was found between this single nucleotide polymorphism and baseline measures of platelet aggregation in either cohort. CONCLUSION: Taken together, these findings suggest, for the first time, that genetic variation in CES1 may be an important determinant of the efficacy of clopidogrel.
机译:简介:羧基酯酶1(CES1)是负责将氯吡格雷转化为具有生物活性的羧酸代谢产物的主要酶。方法:我们在抗血小板干预药物基因组学(PAPI)研究的参与者(n = 566)和350例接受氯吡格雷治疗的冠心病患者中对CES1,G143E中的功能变体进行了基因分型,并进行了相关分析生物活性代谢物水平,氯吡格雷ADP刺激的血小板聚集和心血管预后。结果:在CES1 143E等位基因携带者中,氯吡格雷活性代谢产物的水平显着更高(P = 0.001)。与这些发现一致,在PAPI研究的参与者(P = 0.003)和氯吡格雷治疗的冠心病患者(P = 0.03)中,携带CES1 143E等位基因的个体表现出更好的氯吡格雷反应(通过ADP刺激的血小板聚集测定) )。在任何一个队列中,这种单核苷酸多态性与血小板聚集的基线测量值之间均未发现关联。结论:总而言之,这些发现首次表明,CES1的遗传变异可能是氯吡格雷疗效的重要决定因素。

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