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A Study to Evaluate the Efficacy, Safety, and Tolerability of Brivaracetam as Monotherapy in Patients 2 to 25 Years of Age With Childhood Absence Epilepsy or Juvenile Absence Epilepsy

Phase 3
Recruiting
Conditions
Juvenile Absence Epilepsy
Childhood Absence Epilepsy
Interventions
Other: Placebo
Registration Number
NCT04666610
Lead Sponsor
UCB Biopharma SRL
Brief Summary

The purpose of the study is to test the efficacy, safety and tolerability of brivaracetam monotherapy in study participants 2 to 25 years of age inclusive with childhood absence epilepsy (CAE) or juvenile absence epilepsy (JAE).

Detailed Description

Not available

Recruitment & Eligibility

Status
RECRUITING
Sex
All
Target Recruitment
160
Inclusion Criteria

  • Study participant is 2 to 25 years of age inclusive, at the time of signing the informed consent. No study participants from 2 to <4 years of age will be included in Stage 1

  • Study participant is diagnosed with either childhood absence epilepsy (CAE) or juvenile absence epilepsy (JAE) as defined by the International League Against Epilepsy (ILAE) criteria

  • Study participants 2 to <4 years of age and participants who had onset of absence seizures at an age younger than 4 years must have a negative glucose transporter type 1 deficiency syndrome (GLUT1DS) genetic test

  • Study participant is untreated with antiepileptic drugs (AEDs) or pretreated for absence seizures with a maximum of 2 historical AEDs, but without AED treatment for a period of at least 5 half-lives of the AED before randomization into this study. The UCB study physician should be consulted if in doubt

  • Study participant has electroencephalogram (EEG) evidence of bilateral synchronous, symmetric generalized paroxysmal spike waves (2.5-6 hertz) with normal background activity and with at least 1 electrographically recorded seizure lasting 3 seconds or more on a 1-hour EEG with hyperventilation (HV) while awake at Visit 1 (V1), or on a historical EEG up to 12 weeks before enrollment

  • Study participant has a history of clinically evident absence seizures occurring on at least 3 days per week in the 2 weeks prior to enrollment

  • Study participant is without treatment with psychoactive drugs or on a stable dose for at least 2 weeks prior to randomization

  • Study participant has normal neurological examination, head size, development and cognition

  • Body weight is ≥9 kg

  • Male and female

    a) A sexually active male study participant must agree to use contraception during the treatment period and for at least 2 days, corresponding to the time needed to eliminate study treatment, after the last dose of study treatment and refrain from donating sperm during this period b) A female study participant is eligible to participate if she is not pregnant, not breastfeeding, and at least 1 of the following conditions applies: The study participant is premenarchial OR A woman of childbearing potential (WOCBP) who agrees to follow the contraceptive guidance during the treatment period and for at least 2 days after the last dose of study treatment, corresponding to the time needed to eliminate study treatment

  • Study participant provides consent/assent, and the study participant's parent/legal representative/caregiver provides signed informed consent for minor study participants, which includes compliance with the requirements and restrictions listed in the informed consent form (ICF) and in this protocol

Exclusion Criteria
  • Study participant has a history of nonfebrile seizures other than absence seizures (eg, generalized tonic-clonic seizures or myoclonic seizures)
  • Study participant has a history of absence status epilepticus
  • Study participant has a history or presence of paroxysmal nonepileptic seizures
  • Study participant has a clinically relevant electrocardiogram (ECG) abnormality in the opinion of the Principal Investigator
  • Study participant has hepatic impairment (Child Pugh Score A, B, or C) based on the Investigator's assessment
  • Study participant has a history of major psychiatric disease or any clinically significant medical condition that would preclude appropriate study participation
  • Study participant has active suicidal ideation prior to study entry as indicated by a positive response ("Yes") to either Question 4 or Question 5 of the Columbia-Suicide Severity Rating Scale (C-SSRS; for study participants 6 years or older) or clinical judgement (for study participants younger than 6 years). The study participant should be referred immediately to a Mental Healthcare Professional
  • Study participant has a lifetime history of suicide attempt (including an active attempt, interrupted attempt, or aborted attempt). The study participant should be immediately evaluated by a Mental Healthcare Professional to address safety concerns
  • Study participant with known fructose intolerance or hypersensitivity of any of the ingredients in brivaracetam oral solution
  • Study participant has end-stage kidney disease requiring dialysis
  • Concomitant use of rifampicin/rifampin; prior use must have been stopped at least 2 months before randomization
  • Concomitant use of strong CYP2C19 inhibitors like fluconazole, fluoxetine and fluvoxamine, prior use must have been stopped at least 1 week before randomization
  • Study participant has participated in another study of an investigational medicinal product (IMP; and/or an investigational device) within the previous 30 days prior to informed consent
  • Study participant has clinical or EEG findings not consistent with a diagnosis of childhood absence epilepsy (CAE) or juvenile absence epilepsy (JAE)

Study & Design

Study Type
INTERVENTIONAL
Study Design
PARALLEL
Arm && Interventions
GroupInterventionDescription
Placebo to 200 mg brivaracetamPlaceboPlacebo-Controlled (PC) and Active Treatment (AT) Period: Stage 1: Study participants randomized to 'placebo to BRV 200mg/day' (or equivalent dose) will receive placebo during the PC period followed by BRV 200mg/day (or equivalent dose) during the AT period.
Placebo to 100 mg brivaracetamPlaceboPlacebo-Controlled (PC) and Active Treatment (AT) Period: Stage 1: Study participants randomized to 'placebo to BRV 100mg/day' (or equivalent dose) will receive placebo during the PC period followed by BRV 100mg/day (or equivalent dose) during the AT period.
Placebo to BRV optimal dose (defined following Stage 1)PlaceboPlacebo-Controlled (PC) and Active Treatment (AT) Period: Stage 2: Study participants will be randomized in Stage 2 of the study to 'placebo to BRV optimal dose'. Study participants randomized to placebo to brivaracetam (BRV) optimal dose will receive placebo during the PC period followed by BRV optimal dose during the AT period.
Placebo received during RDWPlaceboRandomized Withdrawal (RDW) Period: Only study participants who are absence seizure-free based on the outcome of the 24h EEG of Visit 5 will enter the RDW Period. Study participants who are randomized to the placebo arm in the RDW Period will be tapered down to 0 mg and receive 0 mg for 2 weeks.
Brivaracetam 100 mgBrivaracetamPlacebo-Controlled (PC) and Active Treatment (AT) Period: Stage 1: Study participants randomized to BRV 100mg/day (or equivalent dose) will receive these doses during the 2-week PC period and subsequent 11-week AT period.
Brivaracetam 200 mgBrivaracetamPlacebo-Controlled (PC) and Active Treatment (AT) Period: Stage 1: Study participants randomized to brivaracetam (BRV) 200mg/day (or equivalent dose) will receive these doses during the 2-week PC period and subsequent 11-week AT period.
Placebo to 200 mg brivaracetamBrivaracetamPlacebo-Controlled (PC) and Active Treatment (AT) Period: Stage 1: Study participants randomized to 'placebo to BRV 200mg/day' (or equivalent dose) will receive placebo during the PC period followed by BRV 200mg/day (or equivalent dose) during the AT period.
Placebo to 100 mg brivaracetamBrivaracetamPlacebo-Controlled (PC) and Active Treatment (AT) Period: Stage 1: Study participants randomized to 'placebo to BRV 100mg/day' (or equivalent dose) will receive placebo during the PC period followed by BRV 100mg/day (or equivalent dose) during the AT period.
Optimal dose of BRV (defined following Stage 1)BrivaracetamPlacebo-Controlled (PC) and Active Treatment Period (AT): Stage 2: Study participants will be randomized in Stage 2 to receive a fixed dose of the optimal dose of brivaracetam (defined following Stage 1). Study participants randomized to the BRV optimal dose will receive this dose during the 2-week PC period and subsequent 11-week AT period.
Placebo to BRV optimal dose (defined following Stage 1)BrivaracetamPlacebo-Controlled (PC) and Active Treatment (AT) Period: Stage 2: Study participants will be randomized in Stage 2 of the study to 'placebo to BRV optimal dose'. Study participants randomized to placebo to brivaracetam (BRV) optimal dose will receive placebo during the PC period followed by BRV optimal dose during the AT period.
Placebo received during RDWBrivaracetamRandomized Withdrawal (RDW) Period: Only study participants who are absence seizure-free based on the outcome of the 24h EEG of Visit 5 will enter the RDW Period. Study participants who are randomized to the placebo arm in the RDW Period will be tapered down to 0 mg and receive 0 mg for 2 weeks.
Brivaracetam received during RDWBrivaracetamRandomized Withdrawal (RDW) Period: Only study participants who are absence seizure-free based on the outcome of the 24h EEG of Visit 5 will enter the RDW Period. Participants who are randomized to this arm will continue on the Brivaracetam dose they were receiving in the AT period.
Primary Outcome Measures
NameTimeMethod
Percentage of participants who met the criteria for absence seizure freedom within 4 days prior to or during the 24-hour ambulatory electroencephalogram (EEG) at Day 14Day 14

A 24-hour ambulatory electroencephalogram (EEG) will be performed at day 14. The awake hours from the EEG will be analyzed for absence seizures. Every 24-hour EEG will include hyperventilation as a standard provocation test at the beginning of the EEG. Patient will be regarded as not meeting the criteria for absence seizure freedom if they received benzodiazepine in the 4 days prior to the EEG or during the EEG.

Secondary Outcome Measures
NameTimeMethod
Percentage of participants who met the criteria for absence seizure freedom during the randomized withdrawal (RDW) period as determined by electroencephalogram (EEG)From Week 13 to Week 17

Study participants (or their care givers) who believe they are experiencing a recurrence of absence seizures will contact the clinical site for a 1-hour EEG (with hyperventilation (HV)). If no absence seizure is observed during this 1hr EEG (locally read), the study participant will receive a 24-hour ambulatory EEG. If an absence seizure is observed during either EEG, the study participant will be considered as not Absence seizure free and leave the study. If no absence seizures are determined by 1/24hr ambulatory EEG the participant will conduct a 24-hour EEG at week 17. Patient will be regarded as not meeting the criteria for absence seizure freedom if they received benzodiazepine in the 4 days prior to the EEG or during the EEG.

The awake hours from the EEG will be analyzed for absence seizures. Every 24-hour EEG will include HV as a standard provocation test at the beginning of the EEG.

Percent change from Baseline to Day 14 in number of absence seizures on 24-hour ambulatory electroencephalogram (EEG)From Baseline to Day 14

A 24-hour ambulatory electroencephalogram (EEG) will be performed at baseline and day 14. The awake hours from the EEG will be analyzed for absence seizures. Every 24-hour EEG will include hyperventilation as a standard provocation test at the beginning of the EEG.

This endpoint is the difference between the number of seizures at baseline and Day 14.

Percentage of participants who met the criteria for absence seizure freedom based on diary during the 4 days prior to the visit at Day 14Day 14

During the study subjects will keep a diary to record daily seizure activity from Visit 1 until end of the randomized withdrawal (RDW) Period. Each seizure type experienced will be recorded. The last 4 study days prior to Day 14 EEG are used for this endpoint.

Patient will be regarded as not meeting the criteria for absence seizure freedom if they received benzodiazepine in the 4 days prior to the EEG or during the EEG.

Percentage of participants who met the criteria for absence seizure freedom on 24-hour ambulatory electroencephalogram (EEG) at Week 12Week 12

A 24-hour ambulatory electroencephalogram (EEG) will be performed at day 14. The awake hours from the EEG will be analyzed for absence seizures. Every 24-hour EEG will include hyperventilation as a standard provocation test at the beginning of the EEG. Patient will be regarded as not meeting the criteria for absence seizure freedom if they received benzodiazepine in the 4 days prior to the EEG or during the EEG.

Percentage of participants who met the criteria for absence seizure freedom based on diary during the 4 days prior to the visit at Week 12Week 12

During the study subjects will keep a diary to record daily seizure activity from Visit 1 until end of the randomized withdrawal (RDW) Period. Each seizure type experienced will be recorded. The last 4 study days prior to Week 12 EEG are used for this endpoint. Patient will be regarded as not meeting the criteria for absence seizure freedom if they received benzodiazepine in the 4 days prior to the EEG or during the EEG.

Percentage of participants with treatment-emergent adverse events (TEAEs) during the studyFrom Day 1 until End of Safety Follow-Up (up to Week 23)

An adverse event (AE) is defined as any untoward medical occurrence, unintended disease or injury, or untoward clinical signs (including abnormal laboratory finding) in study participants, users, or other persons, whether or not related to the investigational medicinal product (IMP).

Percentage of participants with serious adverse events (SAEs) during the studyFrom Screening Period (Day -14 to Day -2) until End of Safety Follow-Up (up to Week 23)

A Serious Adverse Event (SAE) is any untoward medical occurrence that at any dose:

* Results in death

* Is life-threatening

* Requires in patient hospitalization or prolongation of existing hospitalization

* Is a congenital anomaly or birth defect

* Results in permanent or significant disability/incapacity

* Other important medical events which based on medical or scientific judgement may jeopardize the patients, or may require medical or surgical intervention to prevent any of the above

Percentage of participants with treatment-emergent adverse events (TEAEs) leading to discontinuation of study treatmentFrom Day 1 until End of Down Titration Period (up to Week 21)

An adverse event (AE) is defined as any untoward medical occurrence, unintended disease or injury, or untoward clinical signs (including abnormal laboratory finding) in study participants, users, or other persons, whether or not related to the investigational medicinal product (IMP).

Percentage of participants with drug-related treatment-emergent adverse events (TEAEs) during the studyFrom Baseline (Day -1) until End of Safety Follow-Up (up to Week 23)

An adverse event (AE) is defined as any untoward medical occurrence, unintended disease or injury, or untoward clinical signs (including abnormal laboratory finding) in study participants, users, or other persons, whether or not related to the investigational medicinal product (IMP). 'Drug related AEs' are the subset of AEs that the investigator considers as related to the study drug.

Trial Locations

Locations (53)

N01269 116

🇺🇸

Denver, Colorado, United States

N01269 103

🇺🇸

Loxahatchee Groves, Florida, United States

N01269 111

🇺🇸

Miami, Florida, United States

N01269 101

🇺🇸

Tampa, Florida, United States

N01269 104

🇺🇸

Winter Park, Florida, United States

N01269 110

🇺🇸

Augusta, Georgia, United States

N01269 100

🇺🇸

New Brunswick, New Jersey, United States

N01269 353

🇪🇸

Sevilla, Spain

N01269 354

🇪🇸

Terrassa, Spain

N01269 600

🇺🇦

Dnipro, Ukraine

N01269 601

🇺🇦

Dnipro, Ukraine

N01269 604

🇺🇦

Kharkiv, Ukraine

N01269 608

🇺🇦

Kharkiv, Ukraine

N01269 603

🇺🇦

Kyiv, Ukraine

N01269 606

🇺🇦

Kyiv, Ukraine

N01269 607

🇺🇦

Uzhgorod, Ukraine

N01269 602

🇺🇦

Vinnytsia, Ukraine

N01269 631

🇸🇰

Nove Zamky, Slovakia

N01269 115

🇺🇸

Birmingham, Alabama, United States

N01269 118

🇺🇸

Long Beach, California, United States

N01269 105

🇺🇸

Orange, California, United States

N01269 109

🇺🇸

Winston-Salem, North Carolina, United States

N01269 106

🇺🇸

Philadelphia, Pennsylvania, United States

N01269 203

🇦🇺

Heidelberg, Australia

N01269 202

🇦🇺

Melbourne, Australia

N01269 200

🇦🇺

Randwick, Australia

N01269 201

🇦🇺

South Brisbane, Australia

N01269 301

🇧🇪

Bruxelles, Belgium

N01269 300

🇧🇪

Edegem, Belgium

N01269 400

🇬🇪

Tbilisi, Georgia

N01269 401

🇬🇪

Tbilisi, Georgia

N01269 402

🇬🇪

Tbilisi, Georgia

N01269 403

🇬🇪

Tbilisi, Georgia

N01269 405

🇬🇪

Tbilisi, Georgia

N01269 323

🇮🇹

Messina, Italy

N01269 321

🇮🇹

Milano, Italy

N01269 324

🇮🇹

Milano, Italy

N01269 320

🇮🇹

Pavia, Italy

N01269 322

🇮🇹

Roma, Italy

N01269 325

🇮🇹

Roma, Italy

N01269 326

🇮🇹

Verona, Italy

N01269 533

🇵🇱

Gdansk, Poland

N01269 530

🇵🇱

Krakow, Poland

N01269 534

🇵🇱

Lodz, Poland

N01269 531

🇵🇱

Lublin, Poland

N01269 532

🇵🇱

Warszawa, Poland

N01269 562

🇷🇴

Bucuresti, Romania

N01269 563

🇷🇴

Bucuresti, Romania

N01269 560

🇷🇴

Iasi, Romania

N01269 561

🇷🇴

Timişoara, Judeţ Timiş, Romania

N01269 632

🇸🇰

Bardejov, Slovakia

N01269 630

🇸🇰

Dubnica Nad Vahom, Slovakia

N01269 351

🇪🇸

Madrid, Spain

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