This phase!, open-label study investigated the effects of steady-state brivaracetam administration on steady-state pharmacokinetics of carbamazepine, and steady-state carbamazepine administration on single-dose and steady-state pharmacokinetics of brivaracetam, in 14 healthy participants who received brivaracetam 200 mg single doses on days 1 and 22, and 200 mg twice daily (bid) on days 24-35; and were titrated to carbamazepine 300 mg bid on days 4-35. Brivaracetam did not significantly alter carbamazepine area under the plasma concentration time curve (AUC) over a dosing interval, but resulted in a 2.6-fold increase in carbamazepine-epoxide. Carbamazepine decreased brivaracetam AUC by 29%, while hydroxy-brivaracetam metabolite was increased by 17%. Urinary 6 beta-hydroxycortisol/cortisol ratio was unchanged by brivaracetam, but was increased 3-fold by carbamazepine. In vitro hydrolysis of carbamazepine-epoxide in human hepatocytes was inhibited by brivaracetam, with an IC50 of 8.2 mu M. Brivaracetam 200 mg bid was predicted to increase carbamazepine-epoxide by 2.3-fold, in close agreement with the observed value. In conclusion, brivaracetam did not modify carbamazepine exposure but increased carbamazepine-epoxide. Carbamazepine modestly decreased brivaracetam exposure and increased oxidative metabolism. (C) 2015 Elsevier B.V. All rights reserved.
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DecisionLine Clin Res Corp, Toronto, ON, Canada
Altreos Res Partners Inc, Toronto, ON, CanadaDecisionLine Clin Res Corp, Toronto, ON, Canada
Schoedel, Kerri A.
Stockis, Armel
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UCB Pharma, Braine Lalleud, BelgiumDecisionLine Clin Res Corp, Toronto, ON, Canada
Stockis, Armel
Sellers, Edward M.
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DecisionLine Clin Res Corp, Toronto, ON, Canada
DL Global Partners Inc, Toronto, ON, Canada
Univ Toronto, Pharmacol & Toxicol Med & Psychiat, Toronto, ON, CanadaDecisionLine Clin Res Corp, Toronto, ON, Canada