Madani Soraya, Barilla Denise, Cramer Jeffrey, Wang Yibin, Paul Carle
Clinical Pharmacology, Novartis Pharmaceuticals Corporation, East Hanover, New Jersey 07936-1080, USA.
J Clin Pharmacol. 2002 Nov;42(11):1211-8. doi: 10.1177/009127002762491299.
Terbinafine-CYP2D6 inhibition was evaluated by assessing 48-hour concentration-time profiles of the tricyclic antidepressant desipramine in 12 healthy volunteers identified as extensive cytochrome P450 2D6 (CYP2D6) metabolizers by genotyping and phenotyping. Pharmacokinetics was evaluated at baseline (50 mg oral desipramine given alone), steady state (after 250 mg oral terbinafine for 21 days), and 2 and 4 weeks after terbinafine discontinuation. Pharmacodynamics was evaluated before and 2 hours after each desipramine administration, using Mini-Mental Status Examination (MMSE) and EGG. Terbinafine administration inhibited CYP2D6 metabolism, as indicated by the significant increase in desipramine C(max) (19 ng/ml vs. 36 ng/ml) and AUC0-infinity (482 ng.h/ml vs. 2383 ng.h/ml) and decrease in AUC0-24 and C(max) of the CYP2D6-mediated metabolite, 2-hydroxydesipramine. In addition, the C(max) and AGUC0-infinity of desipramine and metabolite were still elevated 4 weeks after terbinafine discontinuation. Caution should be exercised when coprescribing terbinafine and drugs metabolized by CYP2D6, particularly those with a narrow therapeutic index.
通过评估12名经基因分型和表型分析确定为细胞色素P450 2D6(CYP2D6)广泛代谢者的健康志愿者体内三环类抗抑郁药地昔帕明的48小时浓度-时间曲线,来评价特比萘芬对CYP2D6的抑制作用。在基线(单独口服50 mg地昔帕明)、稳态(口服250 mg特比萘芬21天后)以及停用特比萘芬后2周和4周时评估药代动力学。在每次服用地昔帕明之前和之后2小时,使用简易精神状态检查表(MMSE)和脑电图(EEG)评估药效学。服用特比萘芬抑制了CYP2D6代谢,这表现为地昔帕明的Cmax(19 ng/ml对36 ng/ml)和AUC0-∞(482 ng·h/ml对2383 ng·h/ml)显著增加,以及CYP2D6介导的代谢产物2-羟基地昔帕明的AUC0-24和Cmax降低。此外,停用特比萘芬4周后,地昔帕明及其代谢产物的Cmax和AUC0-∞仍然升高。当同时开具特比萘芬和经CYP2D6代谢的药物时应谨慎,尤其是那些治疗指数较窄的药物。
