Plasma concentrations and pharmacokinetics of idebenone and its metabolites following single and repeated doses in young patients with mitochondrial encephalomyopathy

被引:15
|
作者
Pisano, P
Durand, A
Autret, E
Desnuelle, C
Pinsard, N
Serratrice, G
Legout, V
Joubert, M
Blin, O
机构
[1] CHU TIMONE,CTR PHARMACOL CLIN & EVALUAT THERAPEUT,F-13385 MARSEILLE 5,FRANCE
[2] CHU TIMONE,LAB PHARMACOCINET & TOXICOCINET,F-13385 MARSEILLE 5,FRANCE
[3] HOP BRETONNEAU,PHARMACOL LAB,F-37044 TOURS,FRANCE
[4] HOP LOUIS PASTEUR,SERV NEUROL,LAB NEUROBIOL CELLULAIRE,F-06002 NICE,FRANCE
[5] CHU TIMONE ADULTES,CLIN MALAD SYST NERVEUX & APPAREIL LECOMOTEUR,F-13385 MARSEILLE 5,FRANCE
[6] CHU TIMONE ENFANTS,SERV NEUROL PEDIAT,F-13385 MARSEILLE 5,FRANCE
[7] LABS TAKEDA,F-92816 PUTEAUX,FRANCE
关键词
idebenone; mitochondrial encephalomyopathy; young patients; pharmacokinetics;
D O I
10.1007/s002280050179
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Objective: The pharmacokinetics and tolerance of idebenone after single or repeated doses have been studied in young patients with mitochondrial encephalomyopathy. Results: No significant adverse effects were noted. In 3 out of 7 patients idebenone induced overall stimulation and improvement in arousal. Plasma concentrations of idebenone and its main metabolites were determined and the pharmacokinetic parameters of idebenone after single and repeated doses were estimated. During the single dose study, the mean plasma concentrations of idebenone and its main metabolites and mean pharmacokinetic parameters were comparable to published results (C-max = 452.2 ng . ml(-1), t(max) = 2.3 h, AUC = 26 mu g . ml(-1). h, t(1/2 beta) = 16.5 h). During the repeated doses study, no significant difference was found between mean residual plasma concentrations of idebenone on Day 2 (47 ng . ml(-1)) and Day 5 (70.6 ng . ml(-1)), and mean t(1/2 beta) Of idebenone after the single and after repeated dose studies, i.e., there was no evidence of accumulation. Although idebenone did not appear to accumulate during this study, the coadministration of anticonvulsants, often prescribed during mitochondrial encephalomyopathy, can affect its pharmacokinetics.
引用
收藏
页码:167 / 169
页数:3
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