PHARMACOKINETICS AND METABOLISM OF DOFETILIDE IN MOUSE, RAT, DOG AND MAN

被引:54
|
作者
SMITH, DA [1 ]
RASMUSSEN, HS [1 ]
STOPHER, DA [1 ]
WALKER, DK [1 ]
机构
[1] PFIZER LTD,DEPT CLIN RES,SANDWICH CT13 9NJ,KENT,ENGLAND
关键词
D O I
10.3109/00498259209053133
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
1. Pharmacokinetics of dofetilide were studied in man, dog, rat and mouse after single i.v. and oral doses of dofetilide or C-14-dofetilide. 2. Dofetilide was absorbed completely in all species. Low metabolic clearance in man resulted in complete bioavailability following oral administration. Higher metabolic clearance in rodents, and to a lesser extent dogs, resulted in decreased bioavailability because of first-pass metabolism. 3. Following i.v. administration, the volume of distribution showed only moderate variation in all species (2.8-6.3 l/kg). High plasma clearance in rodents resulted in short half-life values (mouse 0.32, male rat 0.5 and female rat 1.2 h), whilst lower clearance in dog and man gave longer terminal elimination half-lives (4.6 and 7.6 h respectively). 4. After single i.v. doses of C-14-dofetilide, unchanged drug was the major component excreted in urine of all species with several metabolites also present. 5. Metabolites identified in urine from all species were formed by N-oxidation or N-dealkylation of the tertiary nitrogen atom of dofetilide. 6. After oral and i.v. administration of C-14-dofetilide to man, parent compound was the only detectable component present in plasma and represented 75% of plasma radioactivity. No single metabolite accounted for >5% of plasma radioactivity.
引用
收藏
页码:709 / 719
页数:11
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