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首页> 外文期刊>The American heart journal >In-hospital switching of oral P2Y12 inhibitor treatment in patients with acute coronary syndrome undergoing percutaneous coronary intervention: Prevalence, predictors and short-term outcome
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In-hospital switching of oral P2Y12 inhibitor treatment in patients with acute coronary syndrome undergoing percutaneous coronary intervention: Prevalence, predictors and short-term outcome

机译:接受经皮冠状动脉介入治疗的急性冠状动脉综合征患者的院内口服P2Y12抑制剂治疗的发生率,预测因素和短期结果

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Background P2Y12 inhibitor switching has appeared in clinical practice as a consequence of prasugrel and ticagrelor availability, apart from clopidogrel, for use in patients with acute coronary syndrome (ACS) undergoing percutaneous coronary intervention (PCI). Methods In the context of the GReek AntiPlatelet REgistry (GRAPE) we assessed the prevalence, predictive factors and short-term outcome of in-hospital P2Y12 inhibitor switching in 1794 ACS patients undergoing PCI. Results Switching occurred in 636 (35.5%) patients of which in the form of clopidogrel to a novel agent, novel agent to clopidogrel and between prasugrel and ticagrelor in 574 (90.4%), 34 (5.3%) and 27 (4.3%) patients, respectively. Presentation to non PCI-capable hospital, bivalirudin use, age ≥75 years (inverse predictor), and regional trends emerged as predictive factors of switching to a novel agent. At combined in-hospital and one-month follow-up, propensity matched pairs analysis showed no differences in major adverse cardiovascular (MACE) or bleeding events between switching from clopidogrel to a novel agent vs novel agent constant administration. More Bleeding Academic Research Consortium type 1, type 2 and any type events and fewer MACE were seen when switching from clopidogrel to a novel agent vs only clopidogrel administration (23.7%, 3.8%, 30.6%, 1.2% vs 8.9%, 1.2%, 12.0%, 3.8% with P <.001, P =.03, P <.001 and P =.03 respectively). Conclusions In a real-life experience with contemporary antiplatelet treatment in ACS patients undergoing PCI, in-hospital switching represents common clinical practice. Clinical factors and regional practice differences seem to affect this strategy's choice, while switching to a novel agent may be associated with higher risk of bleeding.
机译:背景技术除氯吡格雷外,由于普拉格雷和替卡格雷的可用性,P2Y12抑制剂的转换在临床实践中已出现,除氯吡格雷外,还用于接受经皮冠状动脉介入治疗(PCI)的急性冠脉综合征(ACS)患者。方法在GReek AntiPlatelet REgistry(GRAPE)的背景下,我们评估了1794例接受PCI的ACS患者中院内P2Y12抑制剂转换的发生率,预测因素和短期结果。结果636(35.5%)的患者发生了转换,其中574(90.4%),34(5.3%)和27(4.3%)的患者以氯吡格雷,新药,氯吡格雷和普拉格雷与替卡格雷之间的切换。 , 分别。在没有PCI能力的医院就诊,使用比伐卢定,年龄≥75岁(逆向预测因素)和区域趋势已成为切换为新型药物的预测因素。在院内和一个月的联合随访中,倾向配对分析显示,从氯吡格雷转用新药与持续用药之间,主要不良心血管(MACE)或出血事件无差异。从氯吡格雷换用新药时,与仅使用氯吡格雷相比,出血性学术研究联合会的1型,2型和任何类型事件发生率更高,而MACE则更少(23.7%,3.8%,30.6%,1.2%和8.9%,1.2%,分别为12.0%,3.8%(P <.001,P = .03,P <.001和P = .03)。结论在对接受PCI的ACS患者进行当代抗血小板治疗的真实经验中,医院内切换代表了常见的临床实践。临床因素和地区实践差异似乎会影响该策略的选择,而换用新药可能会增加出血风险。

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