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细胞色素P450 3A4代谢的他汀类药物对600毫克负荷剂量氯吡格雷抗血小板作用及择期冠状动脉支架置入患者临床结局的影响。

Impact of cytochrome P450 3A4-metabolized statins on the antiplatelet effect of a 600-mg loading dose clopidogrel and on clinical outcome in patients undergoing elective coronary stent placement.

作者信息

Trenk Dietmar, Hochholzer Willibald, Frundi Devine, Stratz Christian, Valina Christian M, Bestehorn Hans-Peter, Büttner Heinz Joachim, Neumann Franz-Josef

机构信息

Herz-Zentrum Bad Krozingen, Suedring 15, 79189 Bad Krozingen, Germany.

出版信息

Thromb Haemost. 2008 Jan;99(1):174-81. doi: 10.1160/TH07-08-0503.

DOI:10.1160/TH07-08-0503
PMID:18217151
Abstract

Early studies suggested interactions between statins and clopidogrel. Based on the outcome and platelet data, there is now huge evidence of no interactions between statins and 75 to 300 mg clopidogrel; however, data with 600-mg loading are lacking. In a pre-specified analysis of the EXCELSIOR cohort, we investigated the interaction between statins, especially cytochrome P4503A4-metabolized atorvastatin and simvastatin, and the antiplatelet effects of a 600-mg loading dose of clopidogrel. We analyzed 1,395 patients scheduled for coronary angiography (CA). Patients received clopidogrel 600 mg at least two hours before CA and 75 mg daily thereafter in case of percutaneous coronary intervention (PCI). Statin medication on admission was continued unaltered until discharge. Platelet function was assessed by optical aggregometry and flow cytometry of adenosine diphosphate (ADP)-stimulated surface expression of CD62P, CD63 and PAC-1 before clopidogrel and immediately before CA. Residual platelet aggregation (RPA) after addition of ADP 5 muM was similar irrespective of statin treatment at baseline (p = 0.968). RPA at CA was 46.2 +/- 16.8% in patients without statin (n = 682), 45.5 +/- 17.0% in patients with atorvastatin (n = 255), 45.8 +/- 16.3% with simvastatin (n = 335), 47.3 +/- 14.9% with fluvastatin (n = 42) and 45.9 +/- 16.2% with pravastatin (n = 81; p = 0.962). Consistent results were obtained by flow cytometry. In patients with PCI (n = 553), the one-year incidence of death, myocardial infarction and target lesion reintervention did not differ between cohorts stratified according to statin co-medication (p = 0.645). Thus, peri-interventional atorvastatin and simvastatin had no effect on the antiplatelet activity of a loading dose of clopidogrel 600 mg and did not affect clinical outcome after PCI.

摘要

早期研究提示他汀类药物与氯吡格雷之间存在相互作用。基于研究结果和血小板数据,目前有大量证据表明他汀类药物与75至300毫克氯吡格雷之间不存在相互作用;然而,缺乏600毫克负荷剂量的数据。在EXCELSIOR队列的一项预先设定的分析中,我们研究了他汀类药物,尤其是细胞色素P4503A4代谢的阿托伐他汀和辛伐他汀,与600毫克负荷剂量氯吡格雷的抗血小板作用之间的相互作用。我们分析了1395例计划进行冠状动脉造影(CA)的患者。患者在CA前至少两小时接受600毫克氯吡格雷,此后若进行经皮冠状动脉介入治疗(PCI),则每日服用75毫克。入院时的他汀类药物治疗持续不变直至出院。在服用氯吡格雷前和CA前即刻,通过光学聚集法和流式细胞术检测二磷酸腺苷(ADP)刺激的CD62P、CD63和PAC-1表面表达,评估血小板功能。添加5μM ADP后的残余血小板聚集(RPA)在基线时与他汀类药物治疗无关(p = 0.968)。在未服用他汀类药物的患者(n = 682)中,CA时的RPA为46.2±16.8%,服用阿托伐他汀的患者(n = 255)中为45.5±17.0%,服用辛伐他汀的患者(n = 335)中为45.8±16.3%,服用氟伐他汀的患者(n = 42)中为47.3±14.9%,服用普伐他汀的患者(n = 81)中为45.9±16.2%(p = 0.962)。流式细胞术得到了一致的结果。在接受PCI的患者(n = 553)中,根据他汀类药物联合用药分层的各队列之间,死亡、心肌梗死和靶病变再次干预的一年发生率无差异(p = 0.645)。因此,围介入期阿托伐他汀和辛伐他汀对600毫克负荷剂量氯吡格雷的抗血小板活性无影响,且不影响PCI后的临床结局。

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