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首页> 外文期刊>Therapeutic Drug Monitoring >Therapeutic Drug Monitoring of Clobazam and Its Metabolite-Impact of Age and Comedication on Pharmacokinetic Variability
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Therapeutic Drug Monitoring of Clobazam and Its Metabolite-Impact of Age and Comedication on Pharmacokinetic Variability

机译:Clobazam的治疗药物监测及其年龄和喜剧的代谢产物对药代动力学变异性的影响

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Background:Clobazam (CLB) has been used as an antiepileptic drug for several decades. There is still insufficient data regarding its pharmacokinetic variability in clinical practice. The purpose of this study was to investigate pharmacokinetic variability of CLB with emphasis on the impact of age and comedication in patients with epilepsy.Methods:Serum concentration measurements of CLB and its metabolite N-desmethylclobazam (NCLB), as well as demographic and clinical data were retrieved from the routine therapeutic drug monitoring service at the National Center for Epilepsy, Norway, 2009-2013. NCLB/CLB and total (CLB + NCLB), CLB and NCLB concentration/dose (C/D) ratios were calculated.Results:550 patients (296 women/254 men), average age 27 years (range 1-86), were included. The interindividual pharmacokinetic variability was extensive, as illustrated by a 100-fold variability in serum concentration compared with dose (total C/D ratio 0.03-3.29 mu molL(-1)mg(-1)). The CLB C/D ratio was 36% lower in young children (2-9 years) than in adults (18-64 years), reflecting a higher clearance. In patients receiving phenytoin, felbamate, stiripentol, oxcarbazepine or eslicarbazepine acetate, valproate, phenobarbital, zonisamide or carbamazepine one or more of the calculated ratios were significantly different from that in patients receiving no or neutral comedications. The mean values for the different groups were in the order of 20%-230% of C/D ratios in the neutral group and 200%-950% of the NCLB/CLB ratio.Conclusions:The pharmacokinetic variability of CLB and its metabolite NCLB in clinical practice is extensive, and is influenced by drug-drug interactions, age, and pharmacogenetics. Therapeutic drug monitoring of CLB and NCLB is therefore valuable in patient management.
机译:背景:氯丙嗪(CLB)一直被用作抗癫痫药。关于其在临床实践中的药代动力学变异性仍然没有足够的数据。这项研究的目的是研究CLB的药代动力学变异性,重点是年龄和喜剧对癫痫患者的影响。方法:CLB及其代谢产物N-去甲基环丙胺(NCLB)的血清浓度测量以及人口统计学和临床​​数据于2009-2013年从挪威国家癫痫中心的常规治疗药物监测服务中检索到。计算NCLB / CLB以及总(CLB + NCLB),CLB和NCLB浓度/剂量(C / D)之比。结果:550例患者(296名女性/ 254名男性)平均年龄27岁(范围1-86),包括在内。个体间的药代动力学差异很大,如血清浓度与剂量(总C / D比为0.03-3.29μmolL(-1)mg(-1))相比,差异为100倍。幼儿(2-9岁)的CLB C / D比成人(18-64岁)低36%,这表明清除率更高。在接受苯妥英钠,非苯甲酸酯,替瑞替多,奥卡西平或醋酸依卡西平,醋酸丙戊酸盐,苯巴比妥,唑尼沙胺或卡马西平的患者中,一种或多种计算出的比例与未接受或中性接受药物的患者相比有显着差异。不同组的平均值约为中性组C / D比的20%-230%和NCLB / CLB比的200%-950%。结论:CLB及其代谢产物NCLB的药代动力学变异性在临床实践中,药物治疗广泛,并受药物相互作用,年龄和药物遗传学的影响。因此,CLB和NCLB的治疗药物监测在患者管理中很有价值。

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