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Drug Metabolism Research (M.C., V.K.S., M.J.H., P.E.F., P.E.S,
J.J.V.) and
Structural, Analytical and Medicinal Chemistry
(D.A.K.), Pharmacia & Upjohn, Inc.
Delavirdine mesylate (U-90152T) is a highly specific nonnucleoside
HIV-1 reverse transcriptase inhibitor currently under development for
the treatment of AIDS. The metabolism of delavirdine was investigated in male and female cynomolgus monkeys after oral administration of
[14C-carboxamide]delavirdine mesylate at
single doses of 80 mg/kg and multiple doses of 160 to 300 mg/kg/day.
Desalkyl delavirdine was the major metabolite in circulation. In urine,
desalkyl delavirdine accounted for nearly half of the radioactivity,
with despyridinyl delavirdine and conjugates of desalkyl delavirdine
accounting for most of the remaining radioactivity. Bile was mostly
composed of desalkyl delavirdine and 6
-O-glucuronide
delavirdine, with parent drug, 4-O-glucuronide delavirdine,
and conjugates of desalkyl delavirdine as significant components. In
addition, several minor metabolites were observed in urine and bile of
delavirdine treated monkeys. The metabolism of delavirdine in the
monkey was extensive and involved N-desalkylation,
hydroxylation at the C-4 and C-6 positions of the pyridine ring,
hydroxylation at the C-4 position of the indole ring, pyridine
ring-cleavage, N-glucuronidation of the indole ring, and
amide bond cleavage as determined by MS and/or one-dimensional and
two-dimensional NMR spectroscopies. Phase II biotransformations
included glucuronidation, sulfation, and
-N-acetylglucosaminidation. The identification of the
N-linked -N-acetylglucosamine and
4-O-glucuronide metabolites of delavirdine represents novel
biotransformation pathways.
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