Molden Espen, Skovlund Eva, Braathen Pia
School of Pharmacy, University of Oslo, Oslo, Norway.
Drug Saf. 2008;31(7):587-96. doi: 10.2165/00002018-200831070-00004.
Co-administration of cytochrome P450 (CYP) 3A4 inhibitors with simvastatin or atorvastatin is associated with increased risk of developing myopathy or rhabdomyolysis.
To detect co-prescriptions of CYP3A4 inhibitors with simvastatin or atorvastatin in community pharmacies and assess the risk-preventive actions taken by the prescribing physicians who were alerted about the co-prescription by the pharmacist.
This naturalistic study was performed during four separate 6-week periods in 2004 and 2005, and involved 110 Norwegian community pharmacists (25-30 in each period). Co-prescription of the selected CYP3A4 inhibitors diltiazem, verapamil, clarithromycin, erythromycin, fluconazole, itraconazole and ketoconazole with either simvastatin or atorvastatin was detected with the aid of a simple computer programme. In instances where the pharmacist alerted the prescribing physician about the co-prescription, information on possible strategies to minimize the risk associated with the interaction was also provided. Odds ratios (ORs) were estimated to describe the associations between prescription variables and frequencies of physician information and prescription change, respectively.
In total, 245 co-prescriptions of CYP3A4 inhibitors with simvastatin (134 events) or atorvastatin (111) were detected. Diltiazem (86 events), verapamil (72), erythromycin (48) and clarithromycin (29) were the most commonly co-prescribed CYP3A4 inhibitors. Physicians were informed in 168 out of 245 cases (68.6%). The prescription was subsequently changed in 100 out of 168 cases (59.5%). Another 50 physicians (29.8%) responded that they would consult the patient and monitor potential adverse effects, while only 18 physicians (10.7%) replied that they had already managed the interactions or considered the issue as irrelevant. The adjusted OR for the informing of the physician was 1.89 (95% CI 0.98, 3.63) in patients receiving a daily HMG-CoA reductase inhibitor ('statin') dose of >or=40 mg compared with patients receiving a statin dose of <40 mg/day. The adjusted OR for prescription change was 4.98 (95% CI 2.36, 10.52) if co-prescription was detected prior to the initiation of concurrent use compared with if it was detected during concurrent use.
Nine out of ten physicians changed prescriptions or monitored potential adverse effects when informed by community pharmacists about the risk associated with co-prescription of CYP3A4 inhibitors with simvastatin or atorvastatin. This suggests that an important risk factor for myotoxicity due to these statins could be minimized through interdisciplinary co-operation.
细胞色素P450(CYP)3A4抑制剂与辛伐他汀或阿托伐他汀联合使用会增加发生肌病或横纹肌溶解的风险。
检测社区药房中CYP3A4抑制剂与辛伐他汀或阿托伐他汀的联合处方情况,并评估被药剂师告知联合处方风险的开处方医生所采取的风险预防措施。
这项观察性研究在2004年和2005年的四个不同的6周期间进行,涉及110名挪威社区药剂师(每个期间25 - 30名)。借助一个简单的计算机程序检测所选的CYP3A4抑制剂(地尔硫卓、维拉帕米、克拉霉素、红霉素、氟康唑、伊曲康唑和酮康唑)与辛伐他汀或阿托伐他汀的联合处方情况。在药剂师就联合处方向开处方医生发出警示的情况下,还会提供关于将与相互作用相关的风险降至最低的可能策略的信息。分别估算优势比(OR)以描述处方变量与医生获取信息及处方变更频率之间的关联。
总共检测到245例CYP3A4抑制剂与辛伐他汀(134例)或阿托伐他汀(111例)的联合处方。地尔硫卓(86例)、维拉帕米(72例)、红霉素(48例)和克拉霉素(29例)是最常联合处方的CYP3A4抑制剂。245例中有168例(68.6%)告知了医生。随后在168例中有100例(59.5%)更改了处方。另外50名医生(29.8%)回复称他们会咨询患者并监测潜在不良反应,而只有18名医生(10.7%)回复称他们已经处理了相互作用问题或认为该问题不相关。与接受每日HMG - CoA还原酶抑制剂(“他汀类药物”)剂量<40mg的患者相比,接受每日剂量≥40mg的患者中,告知医生的校正OR为1.89(95%CI 0.98,3.63)。与在同时使用期间检测到联合处方相比,如果在开始同时使用之前检测到联合处方,处方更改的校正OR为4.98(95%CI 2.36,10.52)。
当社区药剂师告知CYP3A4抑制剂与辛伐他汀或阿托伐他汀联合处方相关风险时,十分之九的医生更改了处方或监测了潜在不良反应。这表明通过跨学科合作可将这些他汀类药物导致肌毒性的一个重要风险因素降至最低。
