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Proton pump inhibitor and clopidogrel interaction: fact or fiction?

机译:质子泵抑制剂与氯吡格雷的相互作用:事实还是虚构?

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摘要

Current consensus recommendations state that patients prescribed clopidogrel plus aspirin should receive a proton pump inhibitor (PPI) to reduce gastrointestinal bleeding. Clopidogrel is converted to its active metabolite by cytochrome P450 (CYP) enzymes. Clopidogrel users with decreased CYP2C19 function have less inhibition of platelet aggregation and increased cardiovascular (CV) events. As PPI metabolism also involves CYP2C19, it was hypothesized that competition by PPIs might interfere with clopidogrel's action. Omeprazole, but not other PPIs, worsens surrogate markers of clopidogrel efficacy. Some (but not all) observational studies show that clopidogrel users prescribed PPIs have increased risks of CV events (hazard/odds ratios=1.25-1.5). When effect sizes are small to moderate (relative risks<1.5-2.0), however, it is only possible to conclude whether statistical associations are valid in randomized trials. A randomized trial of omeprazole vs. placebo in clopidogrel users showed no difference in CV events (hazard ratio=1.02,0.70-1.51). Thus, current evidence does not justify a conclusion that PPIs are associated with CV events among clopidogrel users, let alone a judgment of causality. Nonetheless, positive results from some observational studies and biological plausibility have led some health-care providers to accept that PPIs reduce clopidogrel's efficacy. The US Food and Drug Administration (FDA) recommends that "concomitant use of drugs that inhibit CYP2C19 (e.g., omeprazole) should be discouraged." As the presence of PPIs and clopidogrel in plasma is short lived, separation by 12-20 h should in theory prevent competitive inhibition of CYP metabolism and minimize any potential, though unproven, clinical interaction. PPI may be given before breakfast and clopidogrel at bedtime, or PPI may be taken before dinner and clopidogrel at lunchtime.
机译:当前的共识性建议指出,处方氯吡格雷加阿司匹林的患者应接受质子泵抑制剂(PPI)以减少胃肠道出血。氯吡格雷通过细胞色素P450(CYP)酶转化为其活性代谢物。 CYP2C19功能降低的氯吡格雷使用者对血小板聚集的抑制作用较小,而心血管(CV)事件则增加。由于PPI代谢也涉及CYP2C19,因此有假设认为PPI的竞争可能会干扰氯吡格雷的作用。奥美拉唑(而非其他PPI)会使氯吡格雷功效的替代指标恶化。一些(但不是全部)观察性研究表明,氯吡格雷使用者开具PPI会增加CV事件的风险(危险/奇数比= 1.25-1.5)。但是,当效应大小较小至中度(相对风险<1.5-2.0)时,只能得出结论,统计关联在随机试验中是否有效。氯吡格雷使用者中奥美拉唑和安慰剂的随机试验显示心血管事件无差异(危险比= 1.02,0.70-1.51)。因此,目前的证据并不能证明氯吡格雷使用者中PPI与CV事件有关,更不用说因果关系了。但是,一些观察性研究的积极结果和生物学上的合理性使一些医疗保健提供者接受了PPI降低氯吡格雷的功效。美国食品药品监督管理局(FDA)建议“应避免同时使用抑制CYP2C19的药物(例如奥美拉唑)”。由于血浆中PPI和氯吡格雷的存在时间很短,因此理论上应在12-20小时内进行分离,以防止竞争性抑制CYP代谢,并最大限度地减少任何潜在的(尽管未经证实)临床相互作用。 PPI可以在早餐前服用氯吡格雷,就寝前服用,或者PPI可以在晚餐前服用氯吡格雷,午饭前服用。

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