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双氯芬酸、双硫仑、伊曲康唑、葡萄柚汁及红霉素对奎尼丁药代动力学的影响。

Effect of diclofenac, disulfiram, itraconazole, grapefruit juice and erythromycin on the pharmacokinetics of quinidine.

作者信息

Damkier P, Hansen L L, Brosen K

机构信息

Institute of Public Health, Clinical Phamacology, University of Southern Denmark, Odense, Denmark.

出版信息

Br J Clin Pharmacol. 1999 Dec;48(6):829-38. doi: 10.1046/j.1365-2125.1999.00099.x.

Abstract

AIMS

In vitro studies suggest that the oxidation of quinidine to 3-hydroxyquinidine is a specific marker reaction for CYP3A4 activity. To assess the possible use of this reaction as an in vivo marker of CYP3A4 activity, we studied the involvement of cytochromes CYP2C9, CYP2E1 and CYP3A4 in the in vivo oxidative metabolism of quinidine.

METHODS

An open study of 30 healthy young male volunteers was performed. The pharmacokinetics of a 200 mg single oral dose of quinidine was studied before and during daily administration of 100 mg diclofenac, a CYP2C9 substrate (n=6); 200 mg disulfiram, an inhibitor of CYP2E1 (n=6); 100 mg itraconazole, an inhibitor of CYP3A4 (n=6); 250 ml single strength grapefruit juice twice daily, an inhibitor of CYP3A4 (n=6); 250 mg of erythromycin 4 times daily, an inhibitor of CYP3A4 (n=6). Probes of other enzyme activities, caffeine (CYP1A2), sparteine (CYP2D6), mephenytoin (CYP2C19), tolbutamide (CYP2C9) and cortisol (CYP3A4) were also studied.

RESULTS

Concomitant administration of diclofenac reduced the partial clearance of quinidine by N-oxidation by 27%, while no effect was found for other pharmacokinetic parameters of quinidine. Concomitant administration of disulfiram did not alter any of the pharmacokinetic parameters of quinidine. Concomitant administration of itraconazole reduced quinidine total clearance, partial clearance by 3-hydroxylation and partial clearance by N-oxidation by 61, 84 and 73%, respectively. The renal clearance was reduced by 60% and the elimination half-life increased by 35%. Concomitant administration of grapefruit juice reduced the total clearance of quinidine and its partial clearance by 3-hydroxylation and N-oxidation by 15, 19 and 27%, respectively. The elimination half-life of quinidine was increased by 19%. The caffeine metabolic index was reduced by 25%. Concomitant administration of erythromycin reduced the total clearance of quinidine and its partial clearance by 3-hydroxylation and N-oxidation by 34, 50 and 33%, respectively. Cmax was increased by 39%.

CONCLUSIONS

The results confirm an important role for CYP3A4 in the oxidation of quinidine in vivo, and this applies particularly to the formation of 3-hydroxyquinidine. While a minor contribution of CYP2C9 to the N-oxidation of quinidine is possible, a major involvement of the CYP2C9 or CYP2E1 enzymes in the oxidation of quinidine in vivo is unlikely.

摘要

目的

体外研究表明,奎尼丁氧化为3 - 羟基奎尼丁是CYP3A4活性的特异性标记反应。为评估该反应作为CYP3A4活性体内标记的可能性,我们研究了细胞色素CYP2C9、CYP2E1和CYP3A4在奎尼丁体内氧化代谢中的作用。

方法

对30名健康年轻男性志愿者进行了一项开放性研究。在每日服用100 mg双氯芬酸(一种CYP2C9底物,n = 6)、200 mg双硫仑(一种CYP2E1抑制剂,n = 6)、100 mg伊曲康唑(一种CYP3A4抑制剂,n = 6)、每日两次250 ml单浓度葡萄柚汁(一种CYP3A4抑制剂,n = 6)、每日4次250 mg红霉素(一种CYP3A4抑制剂,n = 6)之前及期间,研究了200 mg单剂量口服奎尼丁的药代动力学。还研究了其他酶活性的探针,咖啡因(CYP1A2)、司巴丁(CYP2D6)、美芬妥英(CYP2C19)、甲苯磺丁脲(CYP2C9)和皮质醇(CYP3A4)。

结果

同时服用双氯芬酸使奎尼丁经N - 氧化的部分清除率降低了27%,而奎尼丁的其他药代动力学参数未受影响。同时服用双硫仑未改变奎尼丁的任何药代动力学参数。同时服用伊曲康唑使奎尼丁的总清除率、经3 - 羟基化的部分清除率和经N - 氧化的部分清除率分别降低了61%、84%和73%。肾清除率降低了60%,消除半衰期延长了35%。同时服用葡萄柚汁使奎尼丁的总清除率及其经3 - 羟基化和N - 氧化的部分清除率分别降低了15%、19%和27%。奎尼丁的消除半衰期延长了19%。咖啡因代谢指数降低了25%。同时服用红霉素使奎尼丁的总清除率及其经3 - 羟基化和N - 氧化的部分清除率分别降低了34%、50%和33%。Cmax升高了39%。

结论

结果证实CYP3A4在奎尼丁体内氧化中起重要作用,这尤其适用于3 - 羟基奎尼丁的形成。虽然CYP2C9对奎尼丁的N - 氧化可能有较小贡献,但CYP2C9或CYP2E1酶在奎尼丁体内氧化中起主要作用的可能性不大。

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