THE METABOLISM OF [C-14] RIMANTADINE HYDROCHLORIDE IN RATS AND DOGS

被引:0
|
作者
LOH, AC [1 ]
SZUNA, AJ [1 ]
WILLIAMS, TH [1 ]
SASSO, GJ [1 ]
LEINWEBER, FJ [1 ]
机构
[1] HOFFMANN LA ROCHE INC,DEPT DRUG METAB,340 KINGSLAND ST,NUTLEY,NJ 07110
来源
DRUG METABOLISM AND DISPOSITION | 1991年 / 19卷 / 02期
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中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Metabolism and route of excretion of [C-14]rimantadine hydrochloride was studied in male rats after single po (60 mg/kg) and iv doses (15 mg/kg) and in male dogs (5 or 10 mg/kg po and 5 mg/kg iv). Total C-14 excretion in urine (po and iv) in both species reached 81-87% of the dose in 96 hr. Rimantadine was excreted in rats free (1.0% po, 1.7% iv) and conjugated (0.8% of the dose, po and iv, both in 24 hr) and in dogs, free (2.6% po, 3.0% iv) and conjugated (6.4% po, 7.7% iv, both in 48 hr). In both species, rimantadine metabolism is essentially independent of the route of administration. In rats and dogs, m-hydroxyrimantadine (mostly unconjugated) was the major metabolite, 22% (po) and 24% (iv), and 27% (po) and 21% (iv), respectively. Rats, but not dogs, excreted trans-p-hydroxyrimantadine (23.5% and 25.2%, po and iv, free plus conjugated). An oxidative pathway in dogs produced the m- and p-hydroxylated analogs with a hydroxyl in place of the amino group (3.7% and 5.7% of the dose, both conjugated). A p-hydroxylated compound with a nitro group in place of the amino group may have originated from an N-hydroxy metabolite by spontaneous oxidation during isolation. Comparison of total C-14 excretion, in rats (81%, po; 82%, iv) and dogs (81%, po; 84%, iv) after po and iv administration after 96 hr indicates good absorption of rimantadine.
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页码:381 / 387
页数:7
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