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Effects of prior administration of amodiaquine on the disposition of halofantrine in healthy volunteers.

机译:预先服用阿莫地喹对健康志愿者中氟替汀的影响。

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The prevalence of multidrug-resistant malaria parasites brings about the switch from an antimalarial drug with poor therapeutic outcome to an effective alternative, resulting in overlap in the plasma drug levels. In this study, the influence of prior administration of amodiaquine on the pharmacokinetics and electrocardiographic effect of halofantrine (HF) was investigated in healthy volunteers. Ten healthy male subjects were each given single oral doses of 500 mg HF alone or with 600 mg of amodiaquine hydrochloride (AQ) administered 24 hours before the HF dose in a crossover fashion. Blood samples, collected at predetermined time intervals, were analyzed for HF and its major metabolite, desbutylhalofantrine (HFM) using a validated high-performance liquid chromatography method. Electrocardiogram for each volunteer was taken at predetermined time points. Results showed that prior administration of amodiaquine resulted in no significant changes (P > 0.05) in any of the pharmacokinetic parameters of HF. For example, the parameter values for HF alone and with AQ were: Cmax 144 +/- 53 versus 164 +/- 58 microg/L; T1/2beta 142 +/- 23 versus 139 +/- 28 hours; Cl/F 37.3 +/- 13.9 versus 32.3 +/- 11.4 L/h; and metabolic ratio 1.2 +/- 0.5 vs 1.1 +/- 0.6 Similarly, the disposition of HFM was not significantly altered (P > 0.05) after an earlier exposure to amodiaquine. In addition, the presence of AQ was linked with a further lengthening of the QT interval compared with the effect of HF alone. This study suggests that prior administration of AQ does not result in a significant alteration of the pharmacokinetics of HF but may be associated with an increased risk of QT prolongation. It may be necessary to exercise caution in the use of HF for malaria treatment in persons who have recently received AQ.
机译:多药耐药性疟原虫的流行使治疗效果差的抗疟药转向了有效的替代药物,导致血浆药物水平重叠。在这项研究中,在健康志愿者中研究了事先服用阿莫地喹对氟替林(HF)的药代动力学和心电图作用的影响。十名健康的男性受试者每人口服一次剂量为500 mg HF或600 mg氨二喹盐酸盐(AQ)以交叉方式在HF剂量前24小时服用。使用经过验证的高效液相色谱法,以预定的时间间隔采集的血液样本中的HF及其主要代谢物desbutylhalofantrine(HFM)进行了分析。在预定时间点为每个志愿者采集心电图。结果表明,预先服用阿莫地喹不会导致HF的任何药代动力学参数发生显着变化(P> 0.05)。例如,单独使用HF和使用AQ的HF的参数值为:Cmax 144 +/- 53与164 +/- 58 microg / L; T1 / 2beta 142 +/- 23与139 +/- 28小时; Cl / F 37.3 +/- 13.9与32.3 +/- 11.4 L / h;代谢率1.2 +/- 0.5 vs 1.1 +/- 0.6类似地,早期暴露于阿莫地喹后,HFM的分布没有明显改变(P> 0.05)。此外,与单独使用HF相比,AQ的存在与QT间隔的进一步延长有关。这项研究表明,事先给予AQ不会导致HF的药代动力学显着改变,但可能与QT延长的风险增加有关。对于刚接受AQ的人,在使用HF进行疟疾治疗时可能要谨慎行事。

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