Cross-species comparisons of the pharmacokinetics of ibudilast

被引:22
|
作者
Sanftner, L. M. [1 ]
Gibbons, J. A. [2 ]
Gross, M. I. [1 ]
Suzuki, B. M. [1 ]
Gaeta, F. C. A. [3 ]
Johnson, K. W. [1 ]
机构
[1] Avigen Inc, Res & Dev, Alameda, CA 94502 USA
[2] Jacqueline Gibbons Consulting, Piedmont, CA USA
[3] Gaeta Consulting, Mountain View, CA USA
关键词
Ibudilast; tolerability; pharmacokinetics; metabolism; animals; PHOSPHODIESTERASE INHIBITOR; DRUG-METABOLISM; RAT; LIVER; HEPATOCYTES; EXPRESSION; INDUCTION; CELLS; GLIA; CYTOCHROME-P-450;
D O I
10.3109/00498250903254340
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
1. To enable clinical development of ibudilast for new indications, its pharmacokinetics were characterized in mice, rats, rabbits, dogs, cynomolgus monkeys, and minipigs. Animal pharmacokinetics were compared with a separate study in healthy volunteers. 2. Following oral dosing, the dose-normalized area under the curve (AUC) (DN-AUC(24h)) in humans is 896 ((ng.h ml(-1))/(mg kg(-1))), and in animals ranges from 0.3 to 87. The variability among species cannot be explained by intrinsic clearance, which in intravenous dosing experiments shows only moderate interspecies variation (13-41 l h(-1) m(-2)). A portal vein rat pharmacokinetics model suggested that differences in first-pass gut clearance may explain some of the interspecies variation in oral bioavailability. Ibudilast shows auto-induction of metabolism in some animals, but not in humans. Plasma protein binding in humans and some animals is greater than or equal to 95%. The primary metabolite 6,7-dihyrdodiol-ibudilast is measurable and has been quantitated in plasma from animals and humans. Finally, biodistribution studies show that ibudilast distributes rapidly, extensively, and reversibly to the central nervous system.
引用
收藏
页码:964 / 977
页数:14
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