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多潘立酮与酮康唑的药物动力学相互作用导致健康志愿者 QT 间期延长:一项随机、安慰剂对照、双盲、交叉研究。

Pharmacokinetic interaction between domperidone and ketoconazole leads to QT prolongation in healthy volunteers: a randomized, placebo-controlled, double-blind, crossover study.

机构信息

Hammersmith Medicines Research, Cumberland Avenue, London NW107ES, UK.

出版信息

Br J Clin Pharmacol. 2012 Mar;73(3):411-21. doi: 10.1111/j.1365-2125.2011.04093.x.

Abstract

AIMS

To assess the steady-state pharmacokinetic and QT(c) effects of domperidone and ketoconazole, given alone and together.

METHODS

A randomized, placebo-controlled, double-blind, crossover study was carried out. Healthy subjects (14 men, 10 women; age 18-39 years; mean weight 73.5kg, range 53.8-98.8kg; 23 Europid, 1 Afro-Caribbean) received orally, for 7 days each, placebo, domperidone 10mg, four doses daily, at 4h intervals, ketoconazole 200mg 12-hourly and domperidone and ketoconazole together. The washout period was 15 days. Pharmacokinetics and serial 12-lead ECGs were assessed on day 7, and serial ECGs on day -1 and at follow-up. Two subjects withdrew before the third treatment period, so data were available for 22-24 subjects. RESULTS Ketoconazole tripled domperidone concentrations at steady-state. Domperidone, ketoconazole and their combination significantly increased QT(c) F in men. Overall adjusted mean differences from placebo were 4.20 (95% CI 0.77, 7.63), 9.24 (95% CI 5.85, 12.63) and 15.90 (95% CI 12.47, 19.33) ms, respectively. In women, QT(c) F was not significantly different from placebo on either domperidone or ketoconazole alone, or in combination. However, QT(c) was positively correlated with plasma drug concentrations, in both men and women. ΔQT(c) F increased by about 2ms per 10ngml(-1) rise in domperidone concentration, and per 1µgml(-1) rise in ketoconazole concentration.

CONCLUSIONS

Ketoconazole tripled the plasma concentrations of domperidone. Domperidone and ketoconazole increased QT(c) F in men, whether given together or separately. The effect of domperidone alone was below the level of clinical importance. The negative result in women is unexplained.

摘要

目的

评估多潘立酮和酮康唑单独及联合应用时的稳态药代动力学和 QT(c) 效应。

方法

进行了一项随机、安慰剂对照、双盲、交叉研究。健康受试者(14 名男性,10 名女性;年龄 18-39 岁;平均体重 73.5kg,范围 53.8-98.8kg;23 名欧洲人,1 名非裔加勒比人)分别口服 7 天安慰剂、多潘立酮 10mg,每日 4 次,每 4 小时 1 次、酮康唑 200mg,每 12 小时 1 次以及多潘立酮和酮康唑联合应用。洗脱期为 15 天。第 7 天评估药代动力学和连续 12 导联心电图,第-1 天和随访时评估连续心电图。在第三个治疗期之前,有 2 名受试者退出,因此有 22-24 名受试者的数据可用。

结果

酮康唑使多潘立酮的稳态浓度增加了 3 倍。多潘立酮、酮康唑及其联合应用显著增加了男性的 QT(c)F。与安慰剂相比,总体调整后的平均差异分别为 4.20(95%CI 0.77,7.63)、9.24(95%CI 5.85,12.63)和 15.90(95%CI 12.47,19.33)ms。在女性中,单独使用多潘立酮或酮康唑,或联合使用时,QT(c)F 与安慰剂相比均无显著差异。然而,QT(c)与血浆药物浓度呈正相关,在男性和女性中均如此。多潘立酮浓度每升高 10ngml(-1),QT(c)F 增加约 2ms,酮康唑浓度每升高 1µgml(-1),QT(c)F 增加约 2ms。

结论

酮康唑使多潘立酮的血浆浓度增加了 3 倍。多潘立酮和酮康唑增加了男性的 QT(c)F,无论是联合应用还是单独应用。多潘立酮的单独作用低于临床重要性水平。女性的阴性结果尚无法解释。

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