Do Cenobamate Pharmacokinetics Change with Co-Administered Antiseizure Medications? An Exploratory Analysis of Responder Patients with Focal Drug-Resistant Epilepsy
Bruno Charlier, Viviana Izzo, Giovanni Assenza, Anna Chiara Balsamo, Flavia Cirillo, Albino Coglianese, Carlo Di Bonaventura, Mariana Fernandes, Antonio Gambardella, Emanuele Cerulli Irelli, Claudio Liguori, Sandra Rufolo, Ilaria Sammarra, Amelia Filippelli

TL;DR
This study explores how cenobamate's drug levels in the body are affected by other seizure medications and patient factors like sex in people with drug-resistant epilepsy.
Contribution
The study provides new insights into cenobamate's variable pharmacokinetics influenced by sex and co-administered antiseizure medications.
Findings
Female patients were more likely to be in the high-exposure cenobamate group.
Lacosamide increased and topiramate decreased cenobamate exposure.
Cenobamate's dose-concentration relationship was nonlinear with high variability at higher doses.
Abstract
Background: Cenobamate (CNB) is an anti-seizure medication (ASM) approved for the treatment of drug-resistant focal epilepsy in adults. Notwithstanding significant proof of efficacy, real-world pharmacokinetics (PK) data are lacking, particularly regarding sex-based variations and the effect of concomitant ASMs. This exploratory study aimed to investigate the PK profile of CNB in responder adults with drug-resistant focal epilepsy and assess potential relationship with concomitant ASMs and clinical variables. Methods: We enrolled 17 patients receiving add-on CNB. The concentration-to-dose ratio (C/D), incremental slope (ΔC/ΔD), and dose-to-concentration AUC were calculated. Enrolled individuals were stratified into three exposure clusters (low, medium, and high). Univariate ANOVA was used to explore associations between PK parameters, clinical variables and concomitant ASMs. Results:…
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Taxonomy
TopicsEpilepsy research and treatment · Pharmacological Effects and Toxicity Studies · Pharmacogenetics and Drug Metabolism
