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Drug Monograph

Cenobamate (Xcopri)

cenobamate — tetrazole-derived carbamate antiseizure medication

Antiseizure Medication (ASM) · Oral · Schedule V (CV)
Pharmacokinetic Profile
Half-Life
50–60 h
Metabolism
UGT2B7, CYP2E1, CYP2A6, CYP2B6
Protein Binding
60% (albumin)
Bioavailability
≥88%
Volume of Distribution
40–50 L (apparent)
Clinical Information
Drug Class
Antiseizure Medication (ASM)
Available Doses
12.5, 25, 50, 100, 150, 200 mg tablets
Route
Oral (tablet, crushed/NG tube)
Renal Adjustment
Use with caution; not recommended in ESRD on dialysis
Hepatic Adjustment
Max 200 mg/day (mild–moderate); avoid in severe
Pregnancy
Potential fetal harm (animal data)
Lactation
Unknown in human milk; present in rat milk
Schedule / Legal Status
Schedule V (CV) Controlled Substance
Generic Available
No
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Focal-onset (partial-onset) seizuresAdults (≥18 years)Monotherapy or adjunctiveFDA Approved
Focal-onset seizures with or without secondary generalizationAdults with history of failure of ≥2 ASMsAdjunctive onlyEMA Approved

Cenobamate was approved by the FDA in November 2019 for focal-onset seizures in adults, initially as adjunctive therapy. Based on population pharmacokinetic analyses demonstrating similar exposure in monotherapy and adjunctive settings, the labeling does not restrict use to adjunctive therapy, effectively permitting monotherapy. The EMA approved cenobamate (marketed as Ontozry) in March 2021 with a narrower adjunctive-only indication in patients who have failed at least two prior antiseizure medications. Pediatric efficacy and safety have not been established; post-marketing studies in children aged 2–17 years are required by the FDA.

Off-Label Uses

Primary generalized tonic-clonic seizures: Limited case series and retrospective data suggest potential benefit, but no controlled trial evidence exists. Evidence quality: Very low.

Neuropathic pain: Preclinical data show analgesic activity in animal models; no published human clinical trials for this indication. Evidence quality: Very low.

Dose

Dosing

Adult Dosing — By Clinical Scenario

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
Focal epilepsy — new adjunctive therapy12.5 mg once daily200 mg once daily400 mg once dailyTitrate q2 weeks: 12.5 → 25 → 50 → 100 → 150 → 200 mg/day over 10 weeks
Do not exceed titration schedule due to DRESS risk
Focal epilepsy — monotherapy initiation12.5 mg once daily200 mg once daily400 mg once dailySame titration as adjunctive; withdraw prior ASMs gradually after target dose reached
Monotherapy PK exposure equivalent to adjunctive (FDA PI)
Drug-resistant focal epilepsy — higher-dose optimization12.5 mg once daily200–400 mg once daily400 mg once dailyAfter reaching 200 mg, increase by 50 mg q2 weeks if needed; higher seizure freedom rates observed at 400 mg
Reduce concomitant sodium channel blockers to improve tolerability
Hepatic impairment (Child-Pugh A or B)12.5 mg once dailyPer clinical response200 mg once dailyAUC increased 1.9-fold (mild) and 2.3-fold (moderate) vs healthy controls
Avoid in severe hepatic impairment (Child-Pugh C); AUC 4.2-fold higher
Renal impairment (CrCl 15–89 mL/min)12.5 mg once dailyPer clinical response400 mg once dailyAUC increased 1.4–1.5-fold in mild–moderate impairment; dose reduction may be considered
Not recommended in ESRD (CrCl <15 mL/min) on dialysis; dialysis clearance unknown
Clinical Pearl: Titration Timing and DRESS Risk

The slow biweekly titration schedule starting at 12.5 mg is mandatory, not merely recommended. In early-phase studies with rapid weekly titration, three cases of DRESS occurred including one fatality. The open-label C021 safety study (n = 1,339) using the recommended slow titration reported zero DRESS cases, validating this approach. Never exceed the titration schedule, even in treatment-urgent scenarios.

Administration Options (FDA Label Update, April 2024)

Cenobamate tablets may be taken whole, crushed and mixed with 25 mL water for oral suspension, or crushed and administered via nasogastric tube. Bioequivalence has been confirmed across all three routes. The crushed-tablet suspension should be consumed immediately and not stored.

PK

Pharmacology

Mechanism of Action

Cenobamate is a tetrazole-derived carbamate with a dual mechanism of antiseizure activity. It preferentially inhibits the persistent component of voltage-gated sodium currents, which is the fraction responsible for sustained repetitive neuronal firing during seizures. Unlike many traditional sodium channel blockers that primarily target transient sodium currents, cenobamate’s selectivity for persistent currents may account for its differentiated efficacy profile. Additionally, cenobamate acts as a positive allosteric modulator of GABAA receptors at a binding site distinct from the benzodiazepine site. This dual action on both excitatory sodium channels and inhibitory GABAergic transmission may contribute to the unusually high seizure freedom rates observed in clinical trials compared with other third-generation antiseizure medications.

ADME Profile

ParameterValueClinical Implication
Absorption≥88% oral bioavailability; Tmax 1–4 h (intact tablet), 0.5 h (crushed)High and reliable absorption; food has no clinically significant effect; take with or without food at any time of day
DistributionVd/F ≈ 40–50 L; 60% protein-bound (albumin); concentration-independentModerate distribution volume; displacement interactions unlikely given concentration-independent binding
MetabolismExtensive; glucuronidation (UGT2B7, UGT2B4) + oxidation (CYP2E1, CYP2A6, CYP2B6, minor CYP2C19, CYP3A4/5); parent drug >98% of plasma radioactivityInhibits CYP2C19, induces CYP3A4 and CYP2B6; important for drug interactions with phenytoin, oral contraceptives, and CYP3A substrates
Eliminationt½ 50–60 h; CL/F 0.45–0.63 L/h; 87.8% urine, 5.2% feces; only 6.8% excreted as unchanged drugLong half-life supports once-daily dosing; steady-state reached in ~2 weeks; dose-dependent clearance (non-linear pharmacokinetics)
SE

Side Effects

Adverse reaction data are from pooled analysis of two pivotal placebo-controlled trials (Study C013 and Study C017; n = 442 cenobamate, n = 216 placebo). Most adverse effects are dose-dependent and CNS-related. Incidence figures represent the pooled rate across the 200 mg dose group unless specified; dose-stratified data (100 mg/200 mg/400 mg vs placebo) are shown where clinically relevant.

≥10% Very Common
Adverse EffectIncidence (100 / 200 / 400 mg)Clinical Note
Somnolence19% / 22% / 37% vs 11% placeboDose-dependent; typically improves over 2–4 weeks; additive with CNS depressants and alcohol
Dizziness18% / 22% / 33% vs 15% placeboDose-dependent; advise patients to avoid driving until effect is known
Fatigue12% / 14% / 24% vs 7% placeboPart of a broader fatigue-related cluster including asthenia, malaise, hypersomnia, and lethargy
Diplopia6% / 7% / 15% vs 2% placeboMay indicate excessive sodium channel blockade when co-prescribed with carbamazepine or lacosamide
Headache10% / 12% / 10% vs 9% placeboNot clearly dose-dependent; generally mild and self-limiting
1–10% Common
Adverse EffectIncidence (200 mg group)Clinical Note
Nausea6% vs 3% placeboUsually transient; not dose-limiting in most patients
Balance disorder5% vs 1% placeboPart of the gait/coordination disturbance cluster; dose-dependent (9% at 400 mg)
Nystagmus7% vs 0% placeboClinical sign of CNS toxicity; consider dose reduction or concomitant ASM adjustment
Constipation4% vs 0% placeboMore common at higher doses (8% at 400 mg)
Vomiting4% vs 0% placeboDose-dependent; 5% at 400 mg
Gait disturbance3% vs 1% placeboStrongly dose-dependent (8% at 400 mg); may improve with concomitant ASM dose reduction
Ataxia3% vs 2% placeboRises to 6% at 400 mg; one of the most common reasons for discontinuation
Dysarthria1% vs 0% placeboReaches 7% at 400 mg; reversible with dose adjustment
Confusional state2% vs 0% placeboPart of cognitive dysfunction cluster; 3% at 400 mg
Decreased appetite1% vs 1% placebo5% at 400 mg; may contribute to weight loss
Tremor3% vs 1% placeboPredominantly at 200 mg dose
Serious Serious Adverse Effects (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
DRESS / Multiorgan HypersensitivityRare (0 cases with slow titration in C021; 3 cases with rapid titration in early studies)Typically within first 1–8 weeks (during titration)Immediate discontinuation; do not rechallenge; one fatal case reported with rapid titration. Monitor for fever, rash, lymphadenopathy, organ involvement
QT ShorteningDose-dependent: 31% had >20 ms shortening at 200 mg, 66% at 500 mgDose-dependent; present at steady stateContraindicated in familial short QT syndrome; use caution with other QT-shortening drugs; QTc <300 ms not observed in studies
Suicidal Behavior and IdeationAED class effect (~0.43% vs 0.24% placebo)As early as 1 week after initiationMonitor for depression, suicidal ideation, mood changes; counsel patients and caregivers; suicidal ideation reported in 2% (100 mg) and 1% (200 mg) vs 0% placebo
Hepatic FailureVery rare (postmarketing reports)VariableMonitor hepatic function; ALT >3x ULN observed in up to 2.7% at 400 mg in Study C017; discontinue if hepatic failure suspected
Psychosis (Hallucinations, Delusions)Very rare (postmarketing reports)VariableEvaluate for organic and drug-related causes; dose reduction or discontinuation; psychiatric consultation as needed
Severe Neurological Impairment (ataxia, gait disturbance)Serious in ~2% of treated patients vs 0% placeboDose-dependent; typically during titration or at higher dosesDose reduction; consider reducing concomitant sodium channel blockers; advise against driving and hazardous activities
Discontinuation Discontinuation Rates
Adults — 200 mg/day
9% vs 4% placebo
Top reasons: Dizziness, somnolence, ataxia
Adults — 400 mg/day
21% vs 4% placebo
Top reasons: Ataxia, dizziness, somnolence, diplopia, nystagmus, vertigo
Reason for DiscontinuationIncidence (≥1% in any group, > placebo)Context
AtaxiaMost common reason at 400 mgStrongly dose-dependent; often reduces with concomitant ASM adjustment
Dizziness≥1% across dose groupsCommon early in treatment; usually attenuates
Somnolence≥1% across dose groupsCNS class effect; additive with benzodiazepines and other sedatives
Diplopia≥1% (predominantly at 400 mg)May indicate pharmacodynamic interaction with sodium channel blockers
Nystagmus≥1% (predominantly at 400 mg)Clinical marker of CNS saturation; warrants dose adjustment
Managing CNS Side Effects

The most impactful strategy for improving tolerability at higher cenobamate doses is to reduce concomitant antiseizure medication doses, particularly other sodium channel blockers (carbamazepine, lacosamide, oxcarbazepine). In the C021 open-label safety study, 50% of patients remaining on cenobamate for more than one year were able to reduce their concomitant ASM burden. A proactive approach to dose adjustments of background therapy can significantly improve the therapeutic index of cenobamate.

Int

Drug Interactions

Cenobamate has a complex interaction profile: it inhibits CYP2C19, induces CYP3A4 and CYP2B6, and has bidirectional interactions with several antiseizure medications. Cenobamate itself is metabolized primarily via UGT2B7 and multiple CYP isoenzymes; its own plasma levels are reduced by approximately 27–28% when co-administered with phenytoin but are not significantly affected by valproate, phenobarbital, or carbamazepine.

Major Phenytoin
MechanismCenobamate inhibits CYP2C19, which metabolizes phenytoin; phenytoin also induces cenobamate clearance (~27%)
EffectPhenytoin Cmax and AUC increased by ~70% and ~84% respectively at cenobamate 200 mg/day
ManagementGradually decrease phenytoin by up to 50% as cenobamate is titrated; monitor phenytoin levels closely
FDA PI
Major Oral Contraceptives
MechanismCenobamate induces CYP3A4, which metabolizes ethinyl estradiol and progestins
EffectReduced plasma concentrations and potential contraceptive failure
ManagementUse additional or alternative non-hormonal contraception (copper IUD, barrier methods)
FDA PI
Major CYP3A4 Substrates (e.g., Midazolam)
MechanismCenobamate induces CYP3A4
EffectMidazolam AUC decreased by 72% and Cmax by 61% at cenobamate 200 mg/day
ManagementIncrease CYP3A substrate doses as needed; applies to immunosuppressants, some statins, and many other drugs
FDA PI
Moderate Clobazam (Desmethylclobazam)
MechanismCenobamate inhibits CYP2C19, increasing levels of the active metabolite desmethylclobazam
EffectIncreased desmethylclobazam exposure; increased sedation and CNS depression risk
ManagementReduce clobazam dose as clinically appropriate when adding cenobamate; monitor for excessive sedation
FDA PI
Moderate Phenobarbital
MechanismCenobamate increases phenobarbital concentrations (mechanism not fully characterized)
EffectPhenobarbital Cmax and AUC increased by ~34% and ~37% respectively
ManagementConsider reducing phenobarbital dose; monitor for signs of toxicity (excessive sedation, ataxia)
FDA PI
Moderate Lamotrigine
MechanismCenobamate reduces lamotrigine concentrations (likely via induction of glucuronidation)
EffectLamotrigine levels expected to decrease by 21–52% across the 100–400 mg cenobamate dose range
ManagementMay need to increase lamotrigine dose; monitor levels and seizure control; risk of breakthrough seizures
FDA PI
Moderate Carbamazepine
MechanismCenobamate induces CYP3A4 and CYP2B6
EffectCarbamazepine Cmax and AUC each decreased by ~23%
ManagementIncrease carbamazepine dose as needed based on clinical response and levels; also reduce carbamazepine for additive CNS effects
FDA PI
Moderate CYP2C19 Substrates (e.g., Omeprazole)
MechanismCenobamate inhibits CYP2C19
EffectOmeprazole AUC increased by 107% and Cmax by 83%
ManagementConsider dose reduction of CYP2C19 substrates; also relevant for clopidogrel (reduced active metabolite formation)
FDA PI
Minor CYP2B6 Substrates (e.g., Bupropion)
MechanismCenobamate induces CYP2B6
EffectBupropion AUC decreased by 39% and Cmax by 23%
ManagementMay need to increase bupropion dose; monitor antidepressant and seizure threshold effects
FDA PI
Minor CNS Depressants / Alcohol
MechanismPharmacodynamic additive CNS depression
EffectIncreased risk of somnolence, sedation, respiratory depression
ManagementCounsel patients about additive sedation; no PK interaction with alcohol confirmed
FDA PI
Clinical Pearl: Drugs Unaffected by Cenobamate

Several important co-prescribed drugs are not significantly affected by cenobamate. Population pharmacokinetic analyses confirmed no clinically meaningful interaction with valproic acid, levetiracetam (only 4–13% decrease), lacosamide, or warfarin (CYP2C9 substrate). This simplifies polytherapy decisions for patients already stabilized on these agents.

Mon

Monitoring

  • DRESS Surveillance Every visit during first 8 weeks of titration
    Routine     Monitor for fever, rash, lymphadenopathy, facial swelling, or laboratory signs of organ involvement (eosinophilia, elevated transaminases). Early manifestations may present without rash. Highest risk during titration.
  • Hepatic Function Baseline, then periodically
    Routine     Check ALT, AST at baseline. ALT >3x ULN occurred in up to 2.7% of patients at 400 mg. Repeat if symptoms suggest hepatotoxicity (jaundice, fatigue, nausea). Postmarketing hepatic failure cases reported.
  • Serum Potassium Baseline, then periodically during titration
    Routine     Dose-related elevations >5 mEq/L observed in 8–17% of cenobamate-treated patients in trials (vs 5.6–7% placebo). Maximum values of 5.9 mEq/L reported. Check in patients on ACE inhibitors, potassium-sparing diuretics, or with renal impairment.
  • Concomitant ASM Levels Before and during cenobamate titration
    Routine     Phenytoin levels (up to 84% increase), phenobarbital levels (up to 37% increase), and lamotrigine levels (21–52% decrease) should be checked. Adjust concomitant doses proactively to prevent toxicity or breakthrough seizures.
  • Mood and Suicidality Every visit, ongoing
    Routine     AED class warning: screen for depression, anxiety, irritability, suicidal ideation, and behavioral changes. Risk observed as early as one week after initiation and persists throughout treatment.
  • ECG (QT Interval) Baseline if cardiac risk factors present
    Trigger-based     Dose-dependent QT shortening (mean –11 ms at 200 mg, –18 ms at 500 mg). Consider baseline ECG in patients with cardiac disease, family history of sudden death, or co-prescribed QT-shortening drugs. QTc below 300 ms has not been observed.
  • Neurological Assessment Each dose escalation and as needed
    Trigger-based     Assess for ataxia, gait disturbance, nystagmus, dysarthria, and cognitive changes. Dose-dependent neurological adverse reactions were the most common reason for discontinuation. May necessitate reducing concomitant ASMs.
CI

Contraindications & Cautions

Absolute Contraindications

  • Hypersensitivity to cenobamate or any inactive ingredient in the formulation (contains lactose monohydrate)
  • Familial Short QT Syndrome — cenobamate causes dose-dependent QT shortening; this condition carries a baseline risk of sudden death and ventricular fibrillation, particularly when QTc falls below 300 ms

Relative Contraindications (Specialist Input Recommended)

  • History of DRESS or severe cutaneous hypersensitivity to other ASMs — cross-reactivity is not established, but heightened vigilance during titration is warranted. Document risk-benefit discussion.
  • Severe hepatic impairment (Child-Pugh C) — cenobamate AUC is 4.2-fold higher; use is not recommended by the manufacturer but may be considered in exceptional circumstances with specialist oversight and dose modification.
  • End-stage renal disease on dialysis (CrCl <15 mL/min) — no data on dialysis clearance; use not recommended.
  • Pregnancy — animal studies demonstrate embryofetal toxicity and neurobehavioral impairment in offspring at clinically relevant exposures. Weigh seizure control benefits against potential fetal risk. Encourage enrollment in NAAED Pregnancy Registry (1-888-233-2334).

Use with Caution

  • Mild to moderate hepatic impairment — reduce maximum dose to 200 mg/day; AUC elevated 1.9–2.3-fold
  • Mild to severe renal impairment (CrCl 15–89 mL/min) — AUC elevated 1.4–1.5-fold in mild-moderate impairment; severe RI (CrCl <30) did not show significant AUC change, but caution and dose reduction may still be considered per PI
  • Elderly patients — start at low end of dosing range due to higher likelihood of decreased hepatic, renal, or cardiac function
  • Concomitant QT-shortening drugs — potential synergistic QT shortening effect
  • Patients with depression or history of suicidal behavior — AED class warning applies; monitor closely
  • Concomitant phenytoin therapy — near-doubling of phenytoin levels mandates proactive dose reduction to avoid toxicity
  • Substance use history — cenobamate is a Schedule V controlled substance with demonstrated abuse potential at supratherapeutic doses (400 mg); may cause physical dependence and withdrawal syndrome upon abrupt discontinuation
FDA Class-Wide Regulatory Warning Suicidal Behavior and Ideation — All Antiepileptic Drugs

Antiepileptic drugs, including cenobamate, increase the risk of suicidal thoughts or behavior. Pooled analysis of 199 placebo-controlled trials of 11 AEDs showed approximately twice the risk of suicidal thinking or behavior (adjusted relative risk 1.8; 95% CI: 1.2–2.7) in AED-treated patients compared to placebo. The increased risk was observed as early as one week after starting treatment and persisted throughout the assessed treatment duration. Monitor all patients for emergence or worsening of depression, suicidal thoughts, or unusual changes in behavior.

Pt

Patient Counselling

Purpose of Therapy

Cenobamate is a once-daily antiseizure medication prescribed to reduce the frequency of focal (partial-onset) seizures. It works through two complementary pathways: stabilizing overactive electrical signals in the brain and enhancing the brain’s natural inhibitory system. It may be used alone or alongside other seizure medications. Clinical studies have shown that cenobamate can achieve meaningful seizure reduction in patients who have not responded adequately to other treatments, with some patients achieving complete seizure freedom.

How to Take

Take cenobamate once daily, with or without food, at approximately the same time each day. The dose will be started very low (12.5 mg) and increased gradually every two weeks over approximately 10 weeks. This slow increase is essential for safety and should not be rushed. Tablets may be swallowed whole or crushed and mixed with water if swallowing is difficult. If a dose is missed, take it as soon as remembered unless it is close to the next scheduled dose. Never stop cenobamate abruptly without medical guidance, as sudden withdrawal can trigger seizures.

Drowsiness and Dizziness
Tell patient Feeling sleepy or dizzy is common, especially during the titration period and at higher doses. These effects usually lessen over 2–4 weeks as the body adjusts. Avoid driving, operating machinery, or performing hazardous tasks until you know how cenobamate affects you. Alcohol and other sedating medications can worsen these effects.
Call prescriber If drowsiness or dizziness remains severe after 4 weeks at a stable dose, if you experience balance problems or unsteadiness that affects daily activities, or if you fall because of these symptoms.
Skin Rash and Allergic Reactions (DRESS)
Tell patient A serious but rare allergic reaction called DRESS can occur, usually during the first few weeks of treatment. This is why your dose is increased very slowly. The risk has not been seen when using the recommended slow titration schedule. Early signs include fever, rash, swollen glands, or facial swelling. Not all cases begin with a rash.
Call prescriber Immediately if you develop any unexplained fever, skin rash (even mild), swollen lymph nodes, sore throat, mouth sores, yellowing of skin or eyes, unusual bruising, or severe fatigue during treatment. Do not wait for symptoms to worsen.
Mood Changes and Suicidal Thoughts
Tell patient Like all seizure medications, cenobamate may rarely be associated with mood changes including depression, anxiety, irritability, or thoughts of self-harm. These effects can occur at any point during treatment. Family members and caregivers should be aware of these potential changes.
Call prescriber Immediately if you or those close to you notice new or worsening depression, anxiety, agitation, panic attacks, difficulty sleeping, unusual mood or behavior changes, or any thoughts of suicide or self-harm.
Contraception
Tell patient Cenobamate can make hormonal birth control pills less effective by increasing the speed at which the body breaks them down. This applies to combined oral contraceptives, the mini-pill, and potentially hormonal patches and rings. Use an additional or alternative non-hormonal method of contraception (such as a copper IUD or barrier methods) while taking cenobamate.
Call prescriber If you become pregnant or plan to become pregnant. You may be eligible to enroll in the NAAED Pregnancy Registry (1-888-233-2334) to help collect safety information about antiseizure medications during pregnancy.
Do Not Stop Suddenly
Tell patient Never stop taking cenobamate abruptly. Sudden discontinuation can trigger more frequent seizures or status epilepticus, a dangerous condition where seizures do not stop. If treatment needs to end, your doctor will gradually reduce the dose over at least two weeks. Cenobamate is a controlled substance (Schedule V) and can cause withdrawal symptoms (insomnia, low mood, tremor) if stopped suddenly.
Call prescriber If you are unable to take cenobamate for any reason (illness, running out of supply, hospitalization). Your doctor can arrange a safe discontinuation plan or ensure continuity.
Vision Changes
Tell patient Double vision (diplopia) and blurred vision can occur, particularly at higher doses or when cenobamate is combined with other sodium channel blocking seizure medications. These effects are generally dose-related and may improve with dose adjustment.
Call prescriber If you develop double vision, blurred vision, or difficulty focusing that persists or worsens, especially if it interferes with daily activities or safety.
Ref

Sources

Regulatory (PI / SmPC)
  1. XCOPRI (cenobamate) tablets, for oral use, CV. Full Prescribing Information. SK Life Science, Inc. Revised 04/2024. FDA Label Primary regulatory source for all dosing, pharmacokinetic, safety, and interaction data in this monograph.
  2. Ontozry (cenobamate) Summary of Product Characteristics. Angelini Pharma S.p.A. EMA Approved March 2021. EMA EPAR European regulatory source; provides the narrower adjunctive-only indication for drug-resistant focal epilepsy.
Key Clinical Trials
  1. Chung SS, French JA, Kowalski J, et al. Randomized phase 2 study of adjunctive cenobamate in patients with uncontrolled focal seizures. Neurology. 2020;94(22):e2311–e2322. doi:10.1212/WNL.0000000000009530 Study C013: pivotal phase 2 RCT demonstrating 55.6% median seizure reduction and 28.3% seizure freedom rate at 200 mg/day.
  2. Krauss GL, Klein P, Brandt C, et al. Safety and efficacy of adjunctive cenobamate (YKP3089) in patients with uncontrolled focal seizures: a multicentre, double-blind, randomised, placebo-controlled, dose-response trial. Lancet Neurol. 2020;19(1):38–48. doi:10.1016/S1474-4422(19)30399-0 Study C017: pivotal phase 3 dose-response RCT across 100, 200, and 400 mg/day demonstrating 21% seizure freedom at 400 mg.
  3. Sperling MR, Klein P, Aboumatar S, et al. Cenobamate (YKP3089) as adjunctive treatment for uncontrolled focal seizures in a large, multicenter, open-label safety study. Epilepsia. 2020;61(6):1099–1108. doi:10.1111/epi.16529 Study C021: open-label safety study (n=1,339) validating the slow titration schedule; zero DRESS cases with recommended protocol.
  4. Klein P, Aboumatar S, Bhatt A, et al. Long-term efficacy and safety of adjunctive cenobamate in patients with uncontrolled focal seizures: open-label extension of a randomized clinical study. Epilepsia. 2022;63(9):2262–2275. doi:10.1111/epi.17338 C017 OLE: sustained efficacy over 48 months with 76.4% showing ≥50% seizure reduction and >15% achieving seizure freedom.
Guidelines
  1. Lattanzi S, Trinka E, Zaccara G, et al. Third-generation antiseizure medications for adjunctive treatment of focal-onset seizures in adults: a systematic review and network meta-analysis. Drugs. 2022;82(2):199–218. doi:10.1007/s40265-021-01661-4 Network meta-analysis showing cenobamate with statistically superior 50% responder rate compared to brivaracetam, lacosamide, perampanel, and eslicarbazepine.
  2. Steinhoff BJ, Sanchez-Alvarez JC, Grunig K, et al. Practical guidance for the management of adults receiving adjunctive cenobamate for the treatment of focal epilepsy—expert opinion. Epilepsy Behav. 2021;124:108318. doi:10.1016/j.yebeh.2021.108318 Expert consensus on practical cenobamate management including ASM co-medication adjustments and titration strategies.
Mechanistic / Basic Science
  1. Roberti R, De Caro C, Iannone LF, et al. Pharmacology of cenobamate: mechanism of action, pharmacokinetics, drug–drug interactions, and tolerability. CNS Drugs. 2021;35(6):609–618. doi:10.1007/s40263-021-00819-8 Comprehensive pharmacology review detailing the dual sodium channel and GABAA receptor mechanism of action.
  2. Zaccara G, Lattanzi S, Leo A, Russo E. Critical appraisal of cenobamate as adjunctive treatment of focal seizures in adults. Neuropsychiatr Dis Treat. 2021;17:3567–3578. doi:10.2147/NDT.S299288 Review addressing pharmacodynamic selectivity for persistent sodium currents and clinical implications of the non-benzodiazepine GABAA site.
Pharmacokinetics / Special Populations
  1. Buckley CT, Bhatt A, Engasser JK, et al. Pharmacokinetics of cenobamate: results from single and multiple oral ascending-dose studies in healthy subjects. Clin Pharmacol Drug Dev. 2020;9(7):849–857. doi:10.1002/cpdd.801 Characterizes single- and multiple-dose PK including dose-proportional Cmax, non-linear AUC, and long terminal half-life across doses.
  2. Vashi M, Engasser JK, Gidal B. Pharmacokinetics of cenobamate as monotherapy compared with adjunctive therapy. Epilepsy Res. 2023;196:107208. doi:10.1016/j.eplepsyres.2023.107208 Population PK analysis confirming equivalent cenobamate exposure in monotherapy versus adjunctive therapy, supporting monotherapy labeling.
  3. Vashi M, Engasser JK, Ren Y, et al. Relative bioavailability of cenobamate administered as a crushed tablet, either orally or via nasogastric tube, versus an intact whole tablet. J Clin Pharmacol. 2024;64(10):1262–1270. doi:10.1002/jcph.2439 Bioequivalence study supporting the 2024 label update for crushed tablet and nasogastric tube administration.
  4. Beltrán-Corbellini Á, Toledano R, Gil-Nagel A, et al. Real-world safety and effectiveness of cenobamate in patients with focal onset seizures: outcomes from an Expanded Access Program. Epilepsia. 2023;64(9):2460–2472. doi:10.1111/epi.17701 Largest real-world cohort (n=170) confirming 63% responder rate and 13.3% seizure freedom in highly refractory epilepsy patients.