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药物-药物相互作用会减少具有药理活性的代谢物的形成:这是临床实践中一个尚未被充分认识的问题。

Drug-drug interactions that reduce the formation of pharmacologically active metabolites: a poorly understood problem in clinical practice.

机构信息

Karolinska Institutet, Department of Clinical Science and Education at Södersjukhuset, Division of Clinical Pharmacology, Karolinska University Hospital, Stockholm, Sweden.

出版信息

J Intern Med. 2010 Dec;268(6):540-8. doi: 10.1111/j.1365-2796.2010.02303.x.

Abstract

Drug-drug interactions can lead to reduced efficacy of medical treatment. Therapeutic failure may for instance result from combined treatment with an inhibitor of the specific pathway that is responsible for the generation of pharmacologically active drug metabolites. This problem may be overlooked in clinical practice. Several examples of drugs will be discussed -clopidogrel, losartan, tamoxifen and codeine - to illustrate differences in the potential impact on drug treatment in clinical practice. We conclude that the combined use of cytochrome P450-blocking serotonin reuptake inhibitors and tamoxifen or codeine should be avoided, whereas the situation is much more complex regarding the use of proton pump inhibitors together with clopidogrel, and the evidence regarding cytochrome P450 inhibitor-dependent activation of losartan is inconclusive.

摘要

药物-药物相互作用可导致医疗效果降低。例如,联合使用特定途径的抑制剂(该途径负责生成具有药理活性的药物代谢物)可能导致治疗失败。在临床实践中,这一问题可能被忽视。我们将讨论几种药物的例子——氯吡格雷、洛沙坦、他莫昔芬和可待因——以说明其在临床实践中对药物治疗的潜在影响的差异。我们的结论是,应避免同时使用细胞色素 P450 阻断性 5-羟色胺再摄取抑制剂与他莫昔芬或可待因,而质子泵抑制剂与氯吡格雷联合使用的情况则要复杂得多,且关于洛沙坦依赖细胞色素 P450 抑制剂激活的证据尚无定论。

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