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Dual antiplatelet therapy and non-cardiac surgery: evolving issues and anesthetic implications

机译:双重抗血小板治疗和非心脏手术:不断发展的问题和麻醉学意义

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摘要

Dual antiplatelet therapy (DAPT) consisting of aspirin plus a P2Y12 inhibitor (clopidogrel, prasugrel, or ticagrelor) is imperative for the treatment of acute coronary syndrome, particularly during the re-endothelialization period after percutaneous coronary intervention (PCI). When patients undergo surgery during this period, the consequences of stent thrombosis are far more serious than those of bleeding complications, except in cases of intracranial surgery. The recommendations for perioperative DAPT have changed with emerging evidence regarding the improved efficacy of non-first-generation drug (everolimus, zotarolimus)-eluting stents (DES). The mandatory interval of 1 year for elective surgery after DES implantation was shortened to 6 months (3 months if surgery cannot be further delayed). After this period, it is generally recommended that the P2Y12 inhibitor be stopped for the amount of time necessary for platelet function recovery (clopidogrel 5–7 days, prasugrel 7–10 days, ticagrelor 3–5 days), and that aspirin be continued during the perioperative period. In emergent or urgent surgeries that cannot be delayed beyond the recommended period after PCI, proceeding to surgery with continued DAPT should be considered. For intracranial procedures or other selected surgeries in which increased bleeding risk may also be fatal, cessation of DAPT (possibly with continuation or minimized interruption [3–4 days] of aspirin) with bridge therapy using short-acting, reversible intravenous antiplatelet agents such as cangrelor (P2Y12 inhibitor) or glycoprotein IIb/IIIa inhibitors (tirofiban, eptifibatide) may be contemplated. Such a critical decision should be individually tailored based on consensus among the anesthesiologist, cardiologist, surgeon, and patient to minimize both ischemic and bleeding risks.
机译:由阿司匹林加P2Y12抑制剂(氯吡格雷,普拉格雷或替卡格雷)组成的双重抗血小板治疗(DAPT)对于急性冠脉综合征的治疗势在必行,特别是在经皮冠状动脉介入治疗(PCI)后重新内皮化期间。在此期间进行手术时,除颅内手术外,支架血栓形成的后果远比出血并发症严重。围手术期DAPT的建议已随着非第一代药物(依维莫司,佐他莫司)洗脱支架(DES)疗效提高的新证据而改变。 DES植入后的择期手术的强制性间隔为1年,缩短为6个月(如果不能进一步推迟手术,则为3个月)。在此期间之后,通常建议在恢复血小板功能所需的时间内停止使用P2Y12抑制剂(氯吡格雷5-7天,普拉格雷7-10天,替卡格雷3-5天),并在此期间继续服用阿司匹林围手术期。如果紧急或紧急手术不能延误至PCI术后建议的时间后,应考虑继续进行DAPT手术。对于颅内手术或其他可能增加出血风险可能致命的外科手术,使用短效,可逆的静脉抗血小板药物,例如桥联疗法,停止DAPT(可能持续或最小限度地中断阿司匹林[3-4天])。可以考虑坎格雷洛(P2Y12抑制剂)或糖蛋白IIb / IIIa抑制剂(替罗非班,依替巴肽)。应该根据麻醉医师,心脏病专家,外科医生和患者之间的共识,对此类关键决策进行个性化定制,以最大程度地减少缺血和出血风险。

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