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Review
. 2020 Jul:163:106327.
doi: 10.1016/j.eplepsyres.2020.106327. Epub 2020 Apr 9.

A review of the drug-drug interactions of the antiepileptic drug brivaracetam

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Free article
Review

A review of the drug-drug interactions of the antiepileptic drug brivaracetam

Brian D Moseley et al. Epilepsy Res. 2020 Jul.
Free article

Abstract

Brivaracetam is an antiepileptic drug (AED) indicated for the treatment of focal seizures, with improved safety and tolerability vs first-generation AEDs. Brivaracetam binds with high affinity to synaptic vesicle protein 2A in the brain, which confers its antiseizure activity. Brivaracetam is rapidly absorbed and extensively biotransformed, and exhibits linear and dose-proportional pharmacokinetics at therapeutic doses. Brivaracetam does not interact with most metabolizing enzymes and drug transporters, and therefore does not interfere with drugs that use these metabolic routes. The favorable pharmacokinetic profile of brivaracetam and lack of clinically relevant drug-drug interactions with commonly prescribed AEDs or oral contraceptives allows administration without dose adjustment, and avoids potential untoward events from decreased efficacy of an AED or oral contraceptive due to a drug-drug interaction. Few agents have been reported to affect the pharmacokinetics of brivaracetam. The strong enzyme-inducing AEDs carbamazepine, phenytoin and phenobarbital/primidone have been shown to moderately lower brivaracetam plasma concentrations, with no adjustment of brivaracetam dose needed. Dose adjustment should be considered when brivaracetam is coadministered with the more potent CYP inducer, rifampin. Additionally, caution should be used when adding or ending treatment with the strong enzyme inducer, St. John's wort. In summary, brivaracetam (50-200 mg/day) has a favorable pharmacokinetic profile and is associated with few clinically relevant drug-drug interactions.

Keywords: Antiepileptic drug; Brivaracetam; Drug-drug interaction; Pharmacokinetics; SV2A.

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Conflict of interest statement

Declaration of Competing Interest BD Moseley has served as an advisory board member/consultant for Eisai and UCB Pharma and as a speaker for Eisai, LivaNova and UCB Pharma; and has received research support from GW Pharma, LivaNova, Nonin Medical, Inc, Sunovion and Xenon Pharmaceuticals. H Chanteux, JM Nicolas and C Laloyaux are employees of UCB Pharma. B Gidal has served as a consultant/speaker for Aquestive Therapeutics, Eisai, Greenwich Biosciences, Sunovion; and has received research support from UCB Pharma. A Stockis is an employee of UCB Pharma.

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