Sabarinath Sreedharan N, Asthana Omkar P, Puri Sunil K, Srivastava Kumkum, Madhusudanan Kunnath P, Gupta Ram C
Pharmacokinetics and Metabolism Division, Central Drug Research Institute, Lucknow, India.
Clin Pharmacokinet. 2005;44(11):1191-203. doi: 10.2165/00003088-200544110-00006.
To evaluate the pharmacokinetics of alpha- and beta-diastereomers of arteether in healthy male volunteers.
The study was a single-centre clinical pharmacokinetic trial in healthy male subjects. A group comprising 13 subjects aged 25-50 years received a single intramuscular 150 mg individual dose of the arteether formulation containing alpha- and beta-isomers in a 30:70 ratio. Serial blood samples collected over a period of 0-192 hours were analysed by high-performance liquid chromatography-electrospray ionisation/tandem mass spectrometry and the plasma concentrations were subjected to compartmental and noncompartmental analyses. Pharmacodynamic parameters such as area under the inhibitory curve, ratio of area under the concentration-time curve to minimum inhibitory concentration (AUC/MIC), maximum plasma concentration to MIC (Cmax/MIC) and time that plasma concentration exceeds the MIC (T>MIC) were calculated in vitro in four strains of Plasmodium falciparum to evaluate the in vivo effectiveness of the proposed dosage regimen.
There were no adverse effects observed during the study. The extent of metabolism of arteether to dihydroartemisinin (DHA) was low (approximately 5%) so as to be therapeutically nonsignificant. The pharmacokinetic profiles of the arteether diastereomers were different, and the maximum plasma concentrations of alpha- and beta-isomers were reached at 4.77+/-1.21 hours and 6.96+/-1.62 hours, respectively, after which they showed biphasic decline with apparent terminal elimination half-lives of 13.24+/-1.08 hours and 30.17+/-2.44 hours, respectively. The plasma and renal clearances, as well as whole blood to plasma partition ratios of the isomers, were comparable, while the apparent volume of distribution during terminal phase of the beta-isomer was approximately 3-fold higher than that of the alpha-isomer. In vitro erythrocyte culture experiments with four strains of P. falciparum showed similar MICs for both isomers of arteether. The highest observed MIC of 8 microg/L was selected for estimating the pharmacokinetic and pharmacodynamic parameters, which showed excellent correlation with published data on the clinical efficacy of arteether.
The pharmacokinetics of arteether isomers demonstrated stereoselectivity, which was reflected mainly in the volume of distribution and the terminal elimination half-life. The alpha- and beta-isomers of arteether appeared to compliment each other pharmacokinetically, with the alpha-isomer providing comparatively rapid and higher plasma concentrations resulting in immediate reduction in percentage parasitaemia, while the beta-isomer, with its longer terminal elimination half-life, mean residence time and sustained plasma concentrations, maintained the activity for longer periods. The extent of metabolic conversion of arteether to DHA was minimal, so as to have any therapeutic or toxic significance.
评估蒿乙醚α和β非对映体在健康男性志愿者体内的药代动力学。
本研究为在健康男性受试者中开展的单中心临床药代动力学试验。一组13名年龄在25至50岁之间的受试者接受了单次肌肉注射150mg蒿乙醚制剂,该制剂中α和β异构体的比例为30:70。在0至192小时内采集的系列血样通过高效液相色谱-电喷雾电离/串联质谱进行分析,并对血浆浓度进行房室和非房室分析。在四株恶性疟原虫体外计算药效学参数,如抑制曲线下面积、浓度-时间曲线下面积与最低抑菌浓度之比(AUC/MIC)、最大血浆浓度与MIC之比(Cmax/MIC)以及血浆浓度超过MIC的时间(T>MIC),以评估所提议给药方案的体内有效性。
研究期间未观察到不良反应。蒿乙醚代谢为双氢青蒿素(DHA)的程度较低(约5%),因此在治疗上无显著意义。蒿乙醚非对映体的药代动力学特征不同,α和β异构体的最大血浆浓度分别在4.77±1.21小时和6.96±1.62小时达到,之后呈双相下降,表观终末消除半衰期分别为13.24±1.08小时和30.17±2.44小时。异构体的血浆清除率、肾清除率以及全血与血浆的分配比相当,而β异构体终末相的表观分布容积比α异构体高约3倍。对四株恶性疟原虫进行的体外红细胞培养实验显示,蒿乙醚两种异构体的最低抑菌浓度相似。选择观察到的最高最低抑菌浓度8μg/L来估算药代动力学和药效学参数,结果显示与已发表的蒿乙醚临床疗效数据具有良好的相关性。
蒿乙醚异构体的药代动力学表现出立体选择性,主要体现在分布容积和终末消除半衰期上。蒿乙醚的α和β异构体在药代动力学上似乎相互补充,α异构体可提供相对较快且较高的血浆浓度,从而使疟原虫血症百分比立即降低,而β异构体因其较长的终末消除半衰期、平均驻留时间和持续的血浆浓度而能维持较长时间的活性。蒿乙醚代谢转化为DHA的程度极小,因此无任何治疗或毒性意义。
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