Treatment With Liraglutide-a Once-Daily GLP-1 Analog-Does Not Reduce the Bioavailability of Ethinyl Estradiol/Levonorgestrel Taken as an Oral Combination Contraceptive Drug
Liraglutide is a once-daily human GLP-1 analog for treatment of type 2 diabetes. Like other GLP-1 analogs, liraglutide delays gastric emptying, which could potentially affect absorption of concomitantly administered oral drugs. This study investigated the effect of liraglutide on the pharmacokinetics of the components of an oral contraceptive (ethinyl estradiol/levonorgestrel). Postmenopausal healthy women (n = 21) were included. A single dose of this contraceptive was administered. Blood samples for ethinyl estradiol/levonorgestrel measurements were drawn until 74 hours post dosing of the contraceptive during liraglutide and placebo treatments. The 90% confidence interval (CI) of the ratio of the area under the curve (AUC) (1.06; 90% CI, 0.99-1.13) for ethinyl estradiol (during liraglutide and placebo) was within defined limits, demonstrating equivalence. The 90% CI for the ratio of AUC for levonorgestrel was not fully contained within the limits (1.18; 90% CI, 1.04-1.34) (levonorgestrel AUC was 18% greater with liraglutide vs placebo). However, equivalence was demonstrated for levonorgestrel AUC(0-t) (1.15; 90% CI, 1.06-1.24). Equivalence was not demonstrated for maximum concentration (C-max); values for ethinyl estradiol and levonorgestrel C-max were 12% and 13% lower with liraglutide versus placebo, respectively. Both reached C-max similar to 1.5 hours later with liraglutide. No clinically relevant reduction in bioavailability of ethinyl estradiol/levonorgestrel occurred.
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Univ Copenhagen, Fac Life Sci, Dept Human Nutr, DK-1958 Frederiksberg C, DenmarkUniv Copenhagen, Fac Life Sci, Dept Human Nutr, DK-1958 Frederiksberg C, Denmark
Astrup, A.
Carraro, R.
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Univ Hosp La Princesa, Inst Invest Sanitaria Princesa, Dept Endocrinol, Madrid, SpainUniv Copenhagen, Fac Life Sci, Dept Human Nutr, DK-1958 Frederiksberg C, Denmark
Carraro, R.
Finer, N.
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UCL, Dept Med, London, EnglandUniv Copenhagen, Fac Life Sci, Dept Human Nutr, DK-1958 Frederiksberg C, Denmark
Finer, N.
Harper, A.
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Novo Nordisk AS, Clin Reporting, Soborg, DenmarkUniv Copenhagen, Fac Life Sci, Dept Human Nutr, DK-1958 Frederiksberg C, Denmark
Harper, A.
Kunesova, M.
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Inst Endocrinol, Obes Management Ctr, Prague, Czech RepublicUniv Copenhagen, Fac Life Sci, Dept Human Nutr, DK-1958 Frederiksberg C, Denmark
Kunesova, M.
Lean, M. E. J.
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Univ Glasgow, Glasgow Royal Infirm, Dept Human Nutr, Glasgow G31 2ER, Lanark, ScotlandUniv Copenhagen, Fac Life Sci, Dept Human Nutr, DK-1958 Frederiksberg C, Denmark
Lean, M. E. J.
Niskanen, L.
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Cent Hosp Cent Finland, Dept Med, Jyvaskyla, Finland
Univ Eastern Finland, Kuopio, FinlandUniv Copenhagen, Fac Life Sci, Dept Human Nutr, DK-1958 Frederiksberg C, Denmark
Niskanen, L.
Rasmussen, M. F.
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Novo Nordisk Inc, Med & Sci Dept, Princeton, NJ USAUniv Copenhagen, Fac Life Sci, Dept Human Nutr, DK-1958 Frederiksberg C, Denmark
Rasmussen, M. F.
Rissanen, A.
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Univ Helsinki, Cent Hosp, Dept Psychiat, Obes Res Unit, Helsinki, FinlandUniv Copenhagen, Fac Life Sci, Dept Human Nutr, DK-1958 Frederiksberg C, Denmark
Rissanen, A.
Rossner, S.
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Karolinska Univ Hosp, Obes Unit, Huddinge, SwedenUniv Copenhagen, Fac Life Sci, Dept Human Nutr, DK-1958 Frederiksberg C, Denmark
Rossner, S.
Savolainen, M. J.
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Univ Oulu, Inst Clin Med, Oulu, FinlandUniv Copenhagen, Fac Life Sci, Dept Human Nutr, DK-1958 Frederiksberg C, Denmark
Savolainen, M. J.
Van Gaal, L.
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Univ Antwerp Hosp, Dept Endocrinol Diabetol & Metab, Antwerp, BelgiumUniv Copenhagen, Fac Life Sci, Dept Human Nutr, DK-1958 Frederiksberg C, Denmark