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Inhibition of dihydropyrimidine dehydrogenase by 5‐propynyluracil, a metabolite of the anti‐varicella zoster virus agent netivudine

 

作者: Richard Peck,   Rebecca Wiggs,   Julia Callaghan,   Ray Wootton,   Peter Crome,   Ian Fraser,   Lloyd Frick,   John Posner,  

 

期刊: Clinical Pharmacology&Therapeutics  (WILEY Available online 1996)
卷期: Volume 59, issue 1  

页码: 22-31

 

ISSN:0009-9236

 

年代: 1996

 

DOI:10.1016/S0009-9236(96)90020-X

 

数据来源: WILEY

 

摘要:

ObjectiveTo study the effects of the anti‐herpetic drug netivudine on dihydropyrimidine dehydrogenase activity in elderly volunteers and to relate them to concentrations of netivudine and its metabolite 5‐propynyluracil.MethodsThree groups of eight elderly volunteers received 400 or 800 mg netivudine or placebo once daily for 8 days. Plasma netivudine, 5‐propynyluracil, and uracil, an indirect measure of dihydropyrimidine dehydrogenase activity, were assayed before the first dose and on days 2, 3, 5, 7, and 8. Full plasma profiles of netivudine and 5‐propynyluracil were determined after the last dose.ResultsPlasma uracil was unquantifiable in all subjects before the first dose and at all time points in the placebo group. In recipients of netivudine it reached a plateau between days 3 and 5, with mean values of 23.2 and 23.5 μmol/L on day 8 in the subjects who received 400 and 800 mg. Plasma netivudine concentrations were approximately dose proportional, but 5‐propynyluracil concentrations were similar in both groups. The half‐maximal rise in plasma uracil occurred after a cumulative 5‐propynyluracil exposure of 120 μmol/L · hr; such exposures will be achieved even after doses as low as 50 to 100 mg daily.ConclusionsNetivudine dosing produces complete inhibition of plasma dihydropyrimidine dehydrogenase. Coadministration with the antimetabolite 5‐fluorouracil will require a substantial reduction in 5‐fluorouracil dose to avoid toxicity but may also improve the therapeutic index of 5‐fluorouracil.Clinical Pharmacology&Therapeuti

 

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