Adjunctive cenobamate in highly active and ultra-refractory focal epilepsy: A "real-world" retrospective study

Javier Peña-Ceballos; Patrick B Moloney; Tudor Munteanu; Michael Doyle; Niamh Colleran; Brenda Liggan; Annette Breen; Sinead Murphy; Hany El-Naggar; Peter Widdess-Walsh; Norman Delanty

doi:10.1111/epi.17549

Adjunctive cenobamate in highly active and ultra-refractory focal epilepsy: A "real-world" retrospective study

Epilepsia. 2023 May;64(5):1225-1235. doi: 10.1111/epi.17549. Epub 2023 Feb 27.

Authors

Javier Peña-Ceballos¹, Patrick B Moloney^{1

2

3}, Tudor Munteanu¹, Michael Doyle^{1

2

3}, Niamh Colleran¹, Brenda Liggan¹, Annette Breen¹, Sinead Murphy¹, Hany El-Naggar¹, Peter Widdess-Walsh¹, Norman Delanty^{1

2

3}

Affiliations

¹ Department of Neurology, Beaumont Hospital, Dublin, Ireland.
² School of Pharmacy and Biomolecular Sciences, Royal College of Surgeons in Ireland, Dublin, Ireland.
³ FutureNeuro, the Science Foundation Ireland Research Centre for Chronic and Rare Neurological Diseases, Dublin, Ireland.

PMID: 36790345
DOI: 10.1111/epi.17549

Abstract

Objective: Recent clinical trials have shown that cenobamate substantially improves seizure control in focal-onset drug-resistant epilepsy (DRE). However, little is known about cenobamate's performance in highly active (≥20 seizures/month) and ultra-refractory focal epilepsy (≥6 failed epilepsy treatments, including antiseizure medications [ASMs], epilepsy surgery, and vagus nerve stimulation). Here, we studied cenobamate's efficacy and tolerability in a "real-world" severe DRE cohort.

Methods: We conducted a single-center retrospective analysis of consecutive adults treated with cenobamate between October 2020 and September 2022. All patients received cenobamate through an Early Access Program. Cenobamate retention, seizure outcomes, treatment-emergent adverse events, and adjustments to concomitant ASMs were analyzed.

Results: Fifty-seven patients received cenobamate for at least 3 months (median duration, 11 months). The median cenobamate dose was 250 mg/day (range 75-350 mg). Baseline demographics were consistent with highly active (median seizure frequency, 60/month) and ultra-refractory epilepsy (median previously failed ASMs, nine). Most (87.8%) had prior epilepsy surgery and/or vagus nerve stimulation. Six patients stopped cenobamate due to lack of efficacy and/or adverse events. One patient died from factors unrelated to cenobamate. Among patients who continued cenobamate, three achieved seizure freedom (5.3% of cohort), 24 had a 75%-99% reduction in seizures (42.1% of cohort), and 16 had a 50%-74% reduction (28.1% of cohort). Cenobamate led to abolition of focal to bilateral tonic-clonic seizures in 55.6% (20/36) of patients. Among treatment responders, 67.4% (29/43) were treated with cenobamate doses of ≥250 mg/day. Three-fourths of patients reported at least one side-effect, most commonly fatigue and somnolence. Adverse events most commonly emerged at cenobamate doses of ≥250 mg/day. Side-effects were partially manageable by reducing the overall ASM burden, most often clobazam, eslicarbazepine, and perampanel.

Significance: Patients with highly active and ultra-refractory focal epilepsy experienced meaningful seizure outcomes on cenobamate. Emergence of adverse events at doses above 250 mg/day may limit the potential for further improvements in seizure control at higher cenobamate doses.

Keywords: cenobamate; drug-resistant epilepsy; focal epilepsy; highly active epilepsy.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adult
Drug Resistant Epilepsy* / drug therapy
Drug-Related Side Effects and Adverse Reactions*
Epilepsies, Partial* / drug therapy
Humans
Retrospective Studies
Seizures

Substances

Cenobamate