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首页> 外文期刊>The American Journal of Cardiology >Relation of body mass index to high on-treatment platelet reactivity and of failed clopidogrel dose adjustment according to platelet reactivity monitoring in patients undergoing percutaneous coronary intervention.
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Relation of body mass index to high on-treatment platelet reactivity and of failed clopidogrel dose adjustment according to platelet reactivity monitoring in patients undergoing percutaneous coronary intervention.

机译:根据经皮冠状动脉介入治疗患者的血小板反应性监测,体重指数与治疗中高血小板反应性和氯吡格雷剂量调整失败的关系。

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摘要

High on-treatment platelet reactivity (HTPR) after a clopidogrel loading dose predicts the risk of thrombotic events after percutaneous coronary intervention. We have demonstrated that HTPR could be overcome in most cases using dose adjustment according to PR monitoring resulting in an improved clinical outcome. However, this strategy failed in nearly 10% of patients with HTPR. Cytochrome P450 (CYP) 2C19 polymorphism was a major determinant of the response to clopidogrel and could be responsible for a failure of dose adjustment. We aimed to determine the clinical and genetical predictors of a failure of the dose-adjustment strategy. Seventy-three patients undergoing percutaneous coronary intervention were included in this prospective multicenter study. A vasodilator phosphoprotein index >or=50% after a 600-mg loading dose of clopidogrel defined HTPR. Dose adjustment was performed according to PR monitoring to reach a vasodilator phosphoprotein index <50%. Genetic polymorphism of CYP2C19 was determined by direct sequencing. Clinical predictors of HTPR were body mass index (BMI; p = 0.01), diabetes mellitus (p = 0.03), and acute coronary syndrome (p = 0.02). The mutant 2 allele of CYP2C19 681A > G loss of function polymorphism was also significantly associated with HTPR (p = 0.04). The rate of successful dose adjustment was similar in carriers of the CYP2C19 2 allele and carriers of the wild-type allele. The only independent predictor of a failed dose adjustment was a high BMI (p = 0.01). In conclusion, high BMI, acute coronary syndrome, diabetes mellitus, and CYP2C19 2 are associated with HTPR after a 600-mg loading dose of clopidogrel. Dose adjustment overcomes HTPR in carriers of the CYP2C19 2 allele. BMI is the only independent predictor of failed dose adjustment. Thus, drug underdosage seems to be the main determinant of HTPR.
机译:氯吡格雷负荷剂量后高治疗血小板反应性(HTPR)预测经皮冠状动脉介入治疗后发生血栓形成事件的风险。我们已经证明,根据PR监测,通过调整剂量在大多数情况下可以克服HTPR,从而改善临床结果。但是,这种策略在将近10%的HTPR患者中无效。细胞色素P450(CYP)2C19多态性是对氯吡格雷反应的主要决定因素,可能是剂量调整失败的原因。我们旨在确定剂量调整策略失败的临床和遗传预测因素。该前瞻性多中心研究纳入了73名接受经皮冠状动脉介入治疗的患者。 600毫克氯吡格雷负荷剂量定义的HTPR后,血管舒张剂磷蛋白指数≥50%。根据PR监测进行剂量调整,以使血管舒张剂磷蛋白指数<50%。通过直接测序确定CYP2C19的遗传多态性。 HTPR的临床预测指标是体重指数(BMI; p = 0.01),糖尿病(p = 0.03)和急性冠脉综合征(p = 0.02)。 CYP2C19 681A> G功能丧失多态性的突变2等位基因也与HTPR显着相关(p = 0.04)。 CYP2C19 2等位基因携带者和野生型等位基因携带者的剂量调整成功率相似。剂量调整失败的唯一独立预测因素是BMI高(p = 0.01)。总之,在服用600 mg氯吡格雷后,高BMI,急性冠状动脉综合征,糖尿病和CYP2C19 2与HTPR相关。剂量调整克服了CYP2C19 2等位基因携带者中的HTPR。 BMI是剂量调整失败的唯一独立预测因子。因此,药物剂量不足似乎是HTPR的主要决定因素。

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