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首页> 外文期刊>Platelets >Clopidogrel resistance in North Indian patients of coronary artery disease and lack of its association with platelet ADP receptors P2Y1 and P2Y12 gene polymorphisms
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Clopidogrel resistance in North Indian patients of coronary artery disease and lack of its association with platelet ADP receptors P2Y1 and P2Y12 gene polymorphisms

机译:印度北部冠心病患者的氯吡格雷抵抗及其与血小板ADP受体P2Y1和P2Y12基因多态性的缺乏相关性

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摘要

Aspirin and Clopidogrel are used in prophylaxis of patients undergoing percutaneous coronary intervention and long-term prevention of cardiovascular and cerebrovascular events. Clopidogrel resistance has been attributed to P2Y1 and P2Y12 adenosine diphosphate (ADP) receptor polymorphisms. This study enrolled 100 patients of coronary artery disease (CAD) who were on the maintenance dose of clopidogrel (75 mg OD) with or without aspirin. In addition, 10 received loading dose (300 mg) prior to percutaneous coronary intervention. Relevant clinical and drug history were elicited. ADP-induced platelet aggregation study and PCR-RFLP for P2Y1 (1622A > G) and P2Y12 (i-T744C) polymorphisms were performed. Two groups of controls were used for defining cut-off for platelet aggregation response. Follow-up data, wherever available was recorded. The most common pattern of aggregation response was disaggregation, either complete (46.4%) or partial (53.6%). A frequency of 13% clopidogrel non-responders and 19% semi-responders was found. All the cases were H1/H1 haplotype for P2Y12 gene polymorphism and 28 (29.2%) patients carried P2Y1 1622A > G (21(21.9%) AG and 7(7.3%) GG) gene polymorphism, the frequency being greater in clopidogrel responders compared to semion-responders but difference was not statistically significant. There was no statistically significant difference between responders and semion-responders in terms of the history of risk factor for CAD, concurrent atorvastatin use or past history of an acute vascular event. On follow up, the two patients who developed myocardial infarction/acute coronary syndromes (MI/ACS) were clopidogrel semi- and non-responder, respectively. Variability in clopidogrel response with 13% non-responders and 19% semi-responders was seen in this study with adverse outcome (MI/ACS) on follow up seen in two patients. Hence, poor response to clopidogrel may be related to increased likelihood of adverse long-term coronary event that may benefit from additional or alternative anti-platelet therapy. Clopidogrel resistance was not associated with ADP receptor P2Y1 and P2Y12 gene polymorphisms. Hence, it is postulated that clopidogrel resistance in CAD patients is multifactorial and not caused by single-gene polymorphisms.
机译:阿司匹林和氯吡格雷用于预防经皮冠状动脉介入治疗的患者以及长期预防心脑血管事件。氯吡格雷耐药性归因于P2Y1和P2Y12腺苷二磷酸(ADP)受体多态性。这项研究招募了100名冠状动脉疾病(CAD)患者,他们接受维持剂量的氯吡格雷(75 mg OD)或不使用阿司匹林。此外,在经皮冠状动脉介入治疗之前,有10位接受了负荷剂量(300 mg)。得出相关的临床和药物史。进行了ADP诱导的血小板聚集研究和P2Y1(1622A> G)和P2Y12(i-T744C)多态性的PCR-RFLP。两组对照用于定义血小板聚集反应的临界值。记录了任何可能的跟踪数据。最常见的聚集响应模式是完全(46.4%)或部分(53.6%)的分解。发现频率为13%的氯吡格雷无反应者和19%的半反应者。所有病例均为P2Y12基因多态性的H1 / H1单倍型,其中28位(29.2%)患者携带P2Y1 1622A> G(21(21.9%)AG和7(7.3%)GG)基因多态性,与氯吡格雷反应者相比,发生频率更高为半/无反应者,但差异无统计学意义。就CAD的危险因素史,同时使用阿托伐他汀或过去发生过急性血管事件的历史而言,反应者和半/无反应者之间在统计学上无显着差异。随访时,两名发生心肌梗塞/急性冠状动脉综合征(MI / ACS)的患者分别为氯吡格雷半应答和无应答。在这项研究中观察到氯吡格雷反应率为13%的无反应者和19%的半反应者的变异性,其中两名患者的随访结果为不良结果(MI / ACS)。因此,对氯吡格雷的不良反应可能与不良长期冠状动脉事件的可能性增加有关,这可能受益于其他或替代的抗血小板治疗。氯吡格雷抵抗与ADP受体P2Y1和P2Y12基因多态性无关。因此,推测CAD患者的氯吡格雷抵抗是多因素的,而不是由单基因多态性引起的。

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