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利福平对微猪中长春瑞滨药代动力学的影响。

The effect of rifampin on the pharmacokinetics of vinorelbine in the micropig.

作者信息

Leveque Dominique, Wisniewski Sandra, Renault Corinne, Peter Jean Daniel, Le Corre Pascal, Monteil Henri, Jehl François

机构信息

Hôpital de Hautepierre, Institut de Bactériologie, Laboratoire d'antibiologie, 67000 Strasbourg, France.

出版信息

Anticancer Res. 2003 May-Jun;23(3B):2741-4.

Abstract

BACKGROUND

Vinorelbine has been shown to be metabolised by CYP3A4 in vitro. To evaluate the impact of CYP3A in the disposition of vinorelbine in vivo, we compared the kinetics of the alkaloid given intravenously alone and combined with rifampin, a potent CYP3A inducer, in the micropig.

ANIMALS AND METHODS

Four healthy Yucatan micropigs, about 20 kg, received a first infusion of vinorelbine (0.5 mg/kg). During the next week they were injected rifampin (600 mg daily) and a second vinorelbine infusion (0.5 mg/kg) on the 7th day of rifampin dosing. Serum concentrations of vinorelbine and rifampin were measured by high performance liquid chromatography.

RESULTS

The mean peak concentrations of vinorelbine were 274.2 ng/ml (Standard Deviation or SD: 90) and 458 ng/ml (SD: 448), the mean areas under the serum concentration-time curve were 8,344 ng.min.ml-1 (SD: 2,604) and 14,093 ng/ml.min-1 (SD: 10,000) and the total clearances were 1.146 l/min (SD: 0.333) and 1.003 l/min (SD: 0.714) when the Catharanthus alkaloid was given alone or was combined with rifampin, respectively.

CONCLUSION

We did not observe an increase in vinorelbine elimination by rifampin related to a CYP3A induction in an animal model physiologically close to humans. Although the number of animals was small, these results suggest that CYP3A metabolism constitutes a minor pathway of elimination of intravenous vinorelbine in the micropig.

摘要

背景

体外研究表明长春瑞滨可被CYP3A4代谢。为评估CYP3A在长春瑞滨体内处置过程中的影响,我们比较了在小型猪体内单独静脉注射长春瑞滨以及联合使用强效CYP3A诱导剂利福平后长春瑞滨的动力学情况。

动物与方法

四只体重约20千克的健康尤卡坦小型猪接受首次长春瑞滨静脉输注(0.5毫克/千克)。在接下来的一周内,它们每天注射利福平(600毫克),并在利福平给药的第7天接受第二次长春瑞滨静脉输注(0.5毫克/千克)。采用高效液相色谱法测定血清中长春瑞滨和利福平的浓度。

结果

单独给予长春瑞滨或联合利福平给药时,长春瑞滨的平均峰浓度分别为274.2纳克/毫升(标准差或SD:90)和458纳克/毫升(SD:448),血清浓度-时间曲线下的平均面积分别为8344纳克·分钟·毫升⁻¹(SD:2604)和14093纳克/毫升·分钟⁻¹(SD:10000),总清除率分别为1.146升/分钟(SD:0.333)和1.003升/分钟(SD:0.714)。

结论

在生理上与人类接近的动物模型中,我们未观察到利福平因诱导CYP3A而使长春瑞滨的清除增加。尽管动物数量较少,但这些结果表明,在小型猪体内,CYP3A代谢是静脉注射长春瑞滨清除的次要途径。

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