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Antimicrob. Agents Chemother., Nov 1997, 2480-2483, Vol 41, No. 11
DR Van Harken, JC Pei, J Wagner and IM Pike
This nonrandomized, two-period crossover study was performed to assess
whether concomitant administration of megestrol acetate influences the
steady-state pharmacokinetics of zidovudine and its inactive 5'-O-
glucuronide metabolite. Twelve HIV-positive, asymptomatic male volunteers
received a 100-mg oral capsule dose of zidovudine at least 30 min before
meals five times a day at 0700, 1100, 1500, 1900, and 2300 h on study days
1 to 3 and a single 100-mg dose at 0700 h on day 4. On days 5 to 17, 800 mg
of megestrol acetate, as a 40-mg/ml aqueous suspension, was administered
orally immediately before the 0700 h dose of zidovudine. On days 5 to 16,
zidovudine was also administered at 1100, 1500, 1900, and 2300 h. Serial
blood samples were collected for 12 h after the single 100-mg dose of
zidovudine on days 4 and 17; trough samples were also obtained just before
the 0700 h dose on days 2 to 4 and 15 to 17. Levels of zidovudine and its
glucuronide in plasma were assayed by a validated radioimmunoassay.
Statistical analysis of trough plasma level data indicated that
steady-state levels of zidovudine and its glucuronide in plasma had been
attained when pharmacokinetic assessments were made on days 4 and 17. When
megestrol acetate and zidovudine were coadministered for 13 days,
differences of - 14, -6.5, and -4.6% in mean zidovudine peak concentration
and areas under the curve at 0 to 4 and 0 to 12 h, respectively, +22.5% in
mean trough concentration, +2.6% in mean plasma half-life, and no change in
median time to peak were observed compared to conditions when zidovudine
was administered alone; for zidovudine 5'-O-glucuronide the respective
differences were -9, -7.3, -4.4, +2.3, and +10% and no change. None of the
differences were statistically significant (P > 0.05). Concomitant
therapy with megestrol acetate, at the dose employed to treat anorexia,
cachexia, or an unexplained, significant weight loss in AIDS patients, did
not alter the steady-state pharmacokinetics of zidovudine or its
5'-O-glucuronide metabolite.
Copyright © 1997 by the American Society for Microbiology. All rights reserved.
Pharmacokinetic interaction of megestrol acetate with zidovudine in human immunodeficiency virus-infected patients
Division of Oncology and Immunology, Bristol-Myers Squibb Company, Plainsboro, New Jersey 08536, USA. donald_vanharken@ccmail.bms.com
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