A post-approval observational study to evaluate the safety and tolerability of perampanel as an add-on therapy in adolescent, adult, and elderly patients with epilepsy

A post-approval observational study to evaluate the safety and tolerability of perampanel as an add-on therapy in adolescent, adult, and elderly patients with epilepsy

•Observational study of perampanel (mean dose: 4.6 mg/day) in 493 patients with epilepsy.•Treatment-emergent adverse events (TEAEs) were consistent with the known safety profile of perampanel.•Frequencies of most clinically important TEAEs were lower than in clinical studies.•Frequency of depression...

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Bibliographic Details
Published in:Epilepsy & behavior Vol. 126; p. 108483
Main Authors: Maguire, Melissa, Ben-Menachem, Elinor, Patten, Anna, Malhotra, Manoj, Ngo, Leock Y.
Format: Journal Article
Language:English
Published: United States Elsevier Inc 01-01-2022
Subjects:
adjunctive perampanel
Adolescent
Adult
adverse events
Aged
ampa-receptor antagonist
Anti-seizure medication
Anticonvulsants - adverse effects
Behavioral Sciences
Child
Cohort Studies
depression
Double-Blind Method
Drug Therapy, Combination
Epilepsy
Epilepsy - chemically induced
Epilepsy - drug therapy
experience
Female
hospital anxiety
Humans
Neurosciences
Neurosciences & Neurology
Neurovetenskaper
Nitriles
Observational
open-label
partial-onset seizures
Perampanel
Post-approval safety study
Psychiatry
Psykiatri
Pyridones - adverse effects
randomized phase-iii
Real-world treatment
risk-factors
Treatment Outcome
RCT
AMPA
Observational
AE
SAS
Epilepsy
HADS
CGI-C
EOT
FOS
Real-world treatment
FBTCS
SD
TEAE
Post-approval safety study
Perampanel
EIASM
ASM
GTCS
Anti-seizure medication
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Summary:•Observational study of perampanel (mean dose: 4.6 mg/day) in 493 patients with epilepsy.•Treatment-emergent adverse events (TEAEs) were consistent with the known safety profile of perampanel.•Frequencies of most clinically important TEAEs were lower than in clinical studies.•Frequency of depression events was slightly lower than observed in clinical studies.•Based on clinician assessment, disease severity was improved in 44.6% of patients. Perampanel is a once-daily oral anti-seizure medication for focal-onset seizures, with or without focal to bilateral tonic-clonic seizures (FBTCS), and generalized tonic-clonic seizures. Study 402 (NCT02033902) collected safety information on clinically important treatment-emergent adverse events (TEAEs) from real-world clinical practice in patients aged ≥12 years with refractory epilepsy who were receiving perampanel as an add-on therapy. Study 402 was a multicenter, observational, 52-week cohort study conducted in Austria, Belgium, Czech Republic, Denmark, France, Israel, Sweden, and the United Kingdom. Safety data were gathered prospectively from patients at clinic visits. The primary endpoint was the incidence of clinically important TEAEs defined as dizziness; blurred vision; somnolence; aggression; balance disorders (including ataxia and falls); weight gain; suicidality; drug abuse, misuse, dependence, and withdrawal; skin photosensitivity; and unintended pregnancy while taking levonorgestrel-containing contraceptives. Off-label use of perampanel and outcomes associated with any suspected drug–drug interaction were also monitored and recorded. Secondary endpoints included the Hospital Anxiety and Depression Scale (HADS) and Clinical Global Impression of Change. Of 483 patients in the Safety Analysis Set, mean (standard deviation [SD]) age was 38.3 (15.1) years, 48.4% were female, mean (SD) time since diagnosis was 23 (14.8) years, 56.5% had focal impaired awareness seizures, and 48.7% had FBTCS. Overall, 243 (49.3%) patients treated with perampanel completed the study and 227 (46.0%) patients discontinued. The most common primary reason for discontinuation was adverse events (n = 130 [26.4%]). A total of 301 (62.3%) patients reported at least one TEAE, of which 45 (15.0%) patients had severe TEAEs and 256 (85.0%) patients had TEAEs judged as mild to moderate in severity. Overall, 51 (10.6%) patients had serious TEAEs, including two deaths that were judged as not related to perampanel, and 136 (28.2%) patients experienced a TEAE that led to treatment discontinuation. Clinically important TEAEs were reported by 153 (31.7%) patients, with the most common being dizziness (13.9%), balance disorders (5.6%), aggression (5.4%), and weight gain (5.4%). In general, the frequencies of clinically important TEAEs were lower in this study compared with previous interventional clinical studies, except for the incidence of suicidality (2.1% vs 1.0%) and aggression (5.4% vs 5.1%). Mean total HADS scores were similar at the end of the study compared with baseline; at the end of treatment, most (>60%) patients had no shift in HADS score category; ∼15% of patients moved to a worse category vs baseline and ∼20% of patients moved to an improved category vs baseline for both anxiety and depression. Based on investigator assessment, disease severity was improved in 185/415 (44.6%) patients. A subanalysis in elderly patients aged ≥65 years showed similar results to the overall population. The data from this observational study are consistent with the known safety profile of perampanel derived from previous interventional phase II and III clinical studies. No unusual or unexpected TEAEs were observed in this real-world clinical practice setting.
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ISSN:1525-5050
1525-5069
1525-5069
DOI:10.1016/j.yebeh.2021.108483