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A Study to Assess the Efficacy and Safety of Adjunctive Zonisamide in Paediatric Partial Onset Seizures (CATZ Extension Study)

Sponsor
Eisai Limited (Industry)
Overall Status
Completed
CT.gov ID
NCT01136954
Collaborator
(none)
144
Enrollment
1
Location
1
Arm
44
Duration (Months)
3.3
Patients Per Site Per Month

Study Details

Study Description

Brief Summary

The purpose of this study is to assess the long-term safety and efficacy of zonisamide used as an adjunctive treatment in pediatric subjects treated with 1 or 2 other anti-epileptic drugs (AEDs).

Condition or Disease Intervention/Treatment Phase
Phase 3

Detailed Description

Those subjects who completed the double-blind study (E2090-E044-312) will be invited to participate in this extension study. The study consists of two main parts: Transition Period (double-blind) and Open Label Period. The study will start with the Transition Period during which subjects already on zonisamide will continue on the same dose of zonisamide and those who were taking placebo will be up-titrated to an appropriate dose of zonisamide. After all subjects have completed the Transition Period, the study will become open-label with every subject on the study receiving zonisamide. The study medication will be taken once daily in the evening. For those subjects previously in the placebo group, dosing with zonisamide will start with a dose of approximately 1 mg/kg. In order that the blind is maintained from the previous study, these subjects will initially continue taking the same number of placebo capsules as they were taking in the Maintenance Period of the E2090-E044-312 study until the up- titration is completed. Those subjects previously in the zonisamide arm will continue on the same dose which they received during the Maintenance Period of the E2090-E044-312 study. In order that the blind is maintained, they will also take placebo capsules in order to mirror the up- titration dose regimen of the subjects previously randomized to receive placebo in the E2090-E044-312 study. All subjects will stop taking placebo capsules after the Transition Period is complete. The duration of the Transition Period depends on the dose the subject appeared to have received when completing the core study E2090-E044-312. For those who completed on 8 mg/kg, the Transition Period will last 7 weeks. For those on 6 mg/kg, the Transition Period will last 5 weeks. However, during the double-blind Transition Period, some subjects may experience adverse events (AEs). If this should occur, the subject may be down titrated to one level above the minimal dose. The overall duration of the study will be up to 59 weeks. The overall duration of the Transition Period may thus be as short as 2 weeks or prolonged to as many as 11 weeks.

The Open Label Period will continue for up to a maximum of 59 weeks (approximately 15 months).

At the end of the study, Eisai will continue to supply zonisamide as part of this open-label extension protocol until the marketing authorisation of zonisamide for this indication or further development in this indication is stopped. In countries where no marketing authorisation will be applied for, Eisai has a compassionate use policy which can be applied for, if required.

Study Design

Study Type:
Interventional
Actual Enrollment :
144 participants
Allocation:
N/A
Intervention Model:
Single Group Assignment
Masking:
None (Open Label)
Primary Purpose:
Treatment
Official Title:
An Open-label Extension Study Following a Double-blind, Randomized, Placebo-controlled, Multi-centre Study to Assess the Efficacy and Safety of Adjunctive Zonisamide in Pediatric Partial Onset Seizures
Study Start Date :
Jul 1, 2008
Actual Primary Completion Date :
Jan 1, 2012
Actual Study Completion Date :
Mar 1, 2012

Arms and Interventions

Arm Intervention/Treatment
Experimental: 1

Drug: Zonisamide
Transition Period from Study E2090-E044-312: Placebo Open-Label Period: 1 to 8 mg/kg orally per day for approximately 59 weeks.
Other Names:
  • Zonegran

    		•

    Outcome Measures

    Primary Outcome Measures

    1. Treatment Emergent Non-Serious Adverse Events With Greater Than 5% Frequency [Week 1 through Week 59]

      Treatment Emergent Adverse Event (TEAE) is defined as an Adverse Event with a start date on or after Day 1 and within 15 days of last dose. For each event, each participant experiencing an event is only counted once even if they had multiple episodes.

    Secondary Outcome Measures

    1. Percentage of Participants With a Decrease From Baseline in 28-day Seizure Frequency of =50%(Responder) in the Open Label Period [Baseline through Week 59]

      A participant with a decrease from baseline in seizure frequency of =50 % was considered a responder. Participants'parent or guardian maintained a seizure diary recording the date,number, and type of seizures the subject had. The primary analysis assessed the percent of responders from baseline in the Open Label Visit Period. Seizure frequency of simple partial, complex partial, and partial seizures with secondary generalization were assessed.

    2. Median Change From Study 312 Baseline in the 28-day Seizure Frequency During the Open Label Period [Baseline of study 312 (Week -8 to Week 0) to Week 59 of study 313]

      Participants' parent or guardian maintained a seizure diary recording the date, number, and type of seizures the subject had. Seizure frequency of simple partial, complex partial, and partial seizures with secondary generalization were assessed from baseline of study 312 through the Open Label Visit Period.

    3. Median Percent Change From Study 312 Baseline in the 28-day Seizure Frequency During the Open Label Period [Baseline of study 312 (Week -8 to Week 0) to Week 59 of study 313]

      Participants' parent or guardian maintained a seizure diary recording the date, number, and type of seizures the subject had. Seizure frequency of simple partial, complex partial, and partial seizures with secondary generalization were assessed from baseline of study 312 through the Open Label Visit Period. Percentage change = 100% x (seizure frequency at period - seizure frequency at Study 312 baseline)/seizure frequency at Study 312 baseline.

    Eligibility Criteria

    Criteria

    Ages Eligible for Study:
    6 Years to 18 Years
    Sexes Eligible for Study:
    All
    Accepts Healthy Volunteers:
    No
    INCLUSION CRITERIA:

    1. Subject has completed the double-blind study E2090-E044-312.

    2. Parent/caregiver is willing to sign an informed consent where the subject is under the age of consent.

    3. Subject is male or female aged 6 to 18 years who is willing to give informed (written or verbal) assent, if applicable. If mandated by local regulations, subjects of relevant age will be required to sign an appropriate informed consent.

    4. Subject is in general good health as determined by medical history, physical exam and screening laboratory results.

    EXCLUSION CRITERIA:

    1. Subject has a body weight < 20 kg.

    2. Subject has developed a history of renal calculi or renal insufficiency (creatinine level > 135 µmol/l (1.5 mg/dl).

    3. Subject has a known diagnosis of human immunodeficiency virus (HIV) or hepatitis B or

    1. Subject has a history of sensitivity to sulfonamide drugs or zonisamide and its excipients.

    2. Female subject of 10 years of age or greater, or of child bearing potential (i.e. started menses) and is not taking or prepared to take a medically acceptable form of contraception (i.e. oral contraceptive pill, surgical sterilization, an implant or injected form of contraception, or intrauterine device), or who is not prepared to abstain from sexual activity for the duration of the study and for one month after the last administration of study medication. NOTE: Should a female subject become of child bearing potential during the study, they must be reconsented in order to given consent to undergo pregnancy testing and either confirm abstinence or receive a medically appropriate form of contraception.

    3. Subject has a recent history of excessive alcohol use or drug abuse.

    4. Subject has a history of suicide attempt.

    5. Subject has a clinically significant organic disease.

    6. Subject has a history of demonstrated non-compliance with treatment or subject or parent/legal guardian can be reasonably expected not to be compliant with study procedures or to complete the study.

    7. Frequent need of rescue benzodiazepines (one or more times a month).

    8. Concomitant use of acetazolamide, carbonic anhydrase inhibitors such as topiramate, furosemide and drugs with anticholinergic activity.

    9. Concomitant use of felbamate or use of felbamate within 2 months prior to Visit 1 of the E2090-E044-312 study.

    Contacts and Locations

    Locations

    Site City State Country Postal Code
    1 Firenze, 50132, FI Italy 50132

    Sponsors and Collaborators

    • Eisai Limited

    Investigators

    • Study Director: Rob van Maanen, M.D., MFPM, Eisai Limited

    Study Documents (Full-Text)

    None provided.

    More Information

    Publications

    None provided.
    Responsible Party:
    Eisai Limited
    ClinicalTrials.gov Identifier:
    NCT01136954
    Other Study ID Numbers:
    • E2090-E044-313
    • 2007-000198-53
    First Posted:
    Jun 4, 2010
    Last Update Posted:
    Jan 25, 2016
    Last Verified:
    Nov 1, 2015
    Additional relevant MeSH terms:
    Seizures
    Zonisamide

    Study Results

    Participant Flow

    Recruitment Details Subjects who completed E2090-E044-312 (NCT00566254)"Study 312" core study were invited to participate in this extension study.
    Pre-assignment Detail
    Arm/Group Title Zonisamide(Placebo During Core Study) Zonisamide (Zonisamide During Core Study)
    Arm/Group Description Participants previously receiving placebo in Study 312, started dosing with zonisamide with a dose of 1 mg/kg/day and titrated upwards with weekly dose increases until a dose of 8 mg/kg/day was reached at the end of the Transition Period (weeks 2 -11). Downtitration was allowed between the limits of 1 to 8 mg/kg/day during Transition Period. Subsequently, a 45-57 week Open-label period followed. Placebo dosing ceased in Open-label Period. Participants previously receiving zonisamide in Study 312 continued taking the same dose of study drug (8 mg/kg/day),supplemented with an increasing number of placebo capsules to mirror the up-titration regimen being followed by those previously receiving placebo.Down-titration was allowed between the limits of 1 to 8 mg/kg/day during Transition Period.Subsequently, a 45-57 week Open-label period followed.
    Period Title: Overall Study
    STARTED 72 72
    COMPLETED 48 51
    NOT COMPLETED 24 21

    Baseline Characteristics

    Arm/Group Title Zonisamide(Placebo During Core Study) Zonisamide (Zonisamide During Core Study) Total
    Arm/Group Description Participants previously receiving placebo in Study 312, started dosing with zonisamide with a dose of 1 mg/kg/day and titrated upwards with weekly dose increases until a dose of 8 mg/kg/day was reached at the end of the Transition Period (weeks 2 -11). Downtitration was allowed between the limits of 1 to 8 mg/kg/day during Transition Period. Subsequently, a 45-57 week Open-label period followed. Placebo dosing ceased in Open-label Period. Participants previously receiving zonisamide in Study 312 continued taking the same dose of study drug (8 mg/kg/day),supplemented with an increasing number of placebo capsules to mirror the up-titration regimen being followed by those previously receiving placebo.Down-titration was allowed between the limits of 1 to 8 mg/kg/day during Transition Period.Subsequently, a 45-57 week Open-label period followed. Total of all reporting groups
    Overall Participants 72 72 144
    Age, Customized (Number) [Number]
    6-11 Years
    34
    47.2%
    33
    45.8%
    67
    46.5%
    12-18 Years
    38
    52.8%
    39
    54.2%
    77
    53.5%
    Sex: Female, Male (Count of Participants)
    Female
    32
    44.4%
    41
    56.9%
    73
    50.7%
    Male
    40
    55.6%
    31
    43.1%
    71
    49.3%

    Outcome Measures

    1. Primary Outcome
    Title Treatment Emergent Non-Serious Adverse Events With Greater Than 5% Frequency
    Description Treatment Emergent Adverse Event (TEAE) is defined as an Adverse Event with a start date on or after Day 1 and within 15 days of last dose. For each event, each participant experiencing an event is only counted once even if they had multiple episodes.
    Time Frame Week 1 through Week 59

    Outcome Measure Data

    Analysis Population Description
    Safety Population (all subjects who entered the study and received at least one dose of study drug)
    Arm/Group Title Zonisamide (Placebo During Core Study) Zonisamide (Zonisamide During Core Study)
    Arm/Group Description Participants previously receiving placebo in Study 312, started dosing with zonisamide with a dose of 1 mg/kg/day and titrated upwards with weekly dose increases until a dose of 8 mg/kg/day was reached at the end of the Transition Period (weeks 2 -11). Downtitration was allowed between the limits of 1 to 8 mg/kg/day during Transition Period. Subsequently, a 45-57 week Open-label period followed. Placebo dosing ceased in Open-label Period. Participants previously receiving zonisamide in Study 312 continued taking the same dose of study drug (8 mg/kg/day),supplemented with an increasing number of placebo capsules to mirror the up-titration regimen being followed by those previously receiving placebo.Down-titration was allowed between the limits of 1 to 8 mg/kg/day during Transition Period.Subsequently, a 45-57 week Open-label period followed.
    Measure Participants 72 72
    Nasopharyngitis
    6
    8.3%
    9
    12.5%
    Bronchitis
    4
    5.6%
    3
    4.2%
    Respiratory tract infection
    2
    2.8%
    4
    5.6%
    Headache
    4
    5.6%
    7
    9.7%
    Weight decreased
    6
    8.3%
    6
    8.3%
    Abdominal pain
    1
    1.4%
    4
    5.6%
    Decreased Appetite
    5
    6.9%
    4
    5.6%
    2. Secondary Outcome
    Title Percentage of Participants With a Decrease From Baseline in 28-day Seizure Frequency of =50%(Responder) in the Open Label Period
    Description A participant with a decrease from baseline in seizure frequency of =50 % was considered a responder. Participants'parent or guardian maintained a seizure diary recording the date,number, and type of seizures the subject had. The primary analysis assessed the percent of responders from baseline in the Open Label Visit Period. Seizure frequency of simple partial, complex partial, and partial seizures with secondary generalization were assessed.
    Time Frame Baseline through Week 59

    Outcome Measure Data

    Analysis Population Description
    Safety Population
    Arm/Group Title Zonisamide(Placebo During Core Study) Zonisamide (Zonisamide During Core Study)
    Arm/Group Description Participants previously receiving placebo in Study 312, started dosing with zonisamide with a dose of 1 mg/kg/day and titrated upwards with weekly dose increases until a dose of 8 mg/kg/day was reached at the end of the Transition Period (weeks 2 -11). Downtitration was allowed between the limits of 1 to 8 mg/kg/day during Transition Period. Subsequently, a 45-57 week Open-label period followed. Placebo dosing ceased in Open-label Period. Participants previously receiving zonisamide in Study 312 continued taking the same dose of study drug (8 mg/kg/day),supplemented with an increasing number of placebo capsules to mirror the up-titration regimen being followed by those previously receiving placebo.Down-titration was allowed between the limits of 1 to 8 mg/kg/day during Transition Period.Subsequently, a 45-57 week Open-label period followed.
    Measure Participants 72 72
    Number [Percentage of Participants]
    55.6
    77.2%
    56.9
    79%
    3. Secondary Outcome
    Title Median Change From Study 312 Baseline in the 28-day Seizure Frequency During the Open Label Period
    Description Participants' parent or guardian maintained a seizure diary recording the date, number, and type of seizures the subject had. Seizure frequency of simple partial, complex partial, and partial seizures with secondary generalization were assessed from baseline of study 312 through the Open Label Visit Period.
    Time Frame Baseline of study 312 (Week -8 to Week 0) to Week 59 of study 313

    Outcome Measure Data

    Analysis Population Description
    Safety Population
    Arm/Group Title Zonisamide(Placebo During Core Study) Zonisamide (Zonisamide During Core Study)
    Arm/Group Description Participants previously receiving placebo in Study 312, started dosing with zonisamide with a dose of 1 mg/kg/day and titrated upwards with weekly dose increases until a dose of 8 mg/kg/day was reached at the end of the Transition Period (weeks 2 -11). Downtitration was allowed between the limits of 1 to 8 mg/kg/day during Transition Period. Subsequently, a 45-57 week Open-label period followed. Placebo dosing ceased in Open-label Period. Participants previously receiving zonisamide in Study 312 continued taking the same dose of study drug (8 mg/kg/day),supplemented with an increasing number of placebo capsules to mirror the up-titration regimen being followed by those previously receiving placebo.Down-titration was allowed between the limits of 1 to 8 mg/kg/day during Transition Period.Subsequently, a 45-57 week Open-label period followed.
    Measure Participants 72 72
    Median (Full Range) [Seizures]
    -3.8
    -4.7
    4. Secondary Outcome
    Title Median Percent Change From Study 312 Baseline in the 28-day Seizure Frequency During the Open Label Period
    Description Participants' parent or guardian maintained a seizure diary recording the date, number, and type of seizures the subject had. Seizure frequency of simple partial, complex partial, and partial seizures with secondary generalization were assessed from baseline of study 312 through the Open Label Visit Period. Percentage change = 100% x (seizure frequency at period - seizure frequency at Study 312 baseline)/seizure frequency at Study 312 baseline.
    Time Frame Baseline of study 312 (Week -8 to Week 0) to Week 59 of study 313

    Outcome Measure Data

    Analysis Population Description
    Safety Population
    Arm/Group Title Zonisamide(Placebo During Core Study) Zonisamide (Zonisamide During Core Study)
    Arm/Group Description Participants previously receiving placebo in Study 312, started dosing with zonisamide with a dose of 1 mg/kg/day and titrated upwards with weekly dose increases until a dose of 8 mg/kg/day was reached at the end of the Transition Period (weeks 2 -11). Downtitration was allowed between the limits of 1 to 8 mg/kg/day during Transition Period. Subsequently, a 45-57 week Open-label period followed. Placebo dosing ceased in Open-label Period. Participants previously receiving zonisamide in Study 312 continued taking the same dose of study drug (8 mg/kg/day),supplemented with an increasing number of placebo capsules to mirror the up-titration regimen being followed by those previously receiving placebo.Down-titration was allowed between the limits of 1 to 8 mg/kg/day during Transition Period.Subsequently, a 45-57 week Open-label period followed.
    Measure Participants 72 72
    Median (Full Range) [Percentage Change]
    -64.6
    -67.9

    Adverse Events

    Time Frame "Treatment-Emergent Adverse Events (TEAE) were collected, and includes all Adverse Events (AE) with a start date on or after Day 1 and within 15 Days of last dose, including AEs with missing start dates. Participants were followed for up to 61 weeks.
    Adverse Event Reporting Description Treatment-emergent AEs were summarized by period (Transition, Open-label, Down-titration), treatment group,body system, and preferred term (PT).
    Arm/Group Title Zonisamide(Placebo During Core Study) Zonisamide (Zonisamide During Core Study)
    Arm/Group Description Participants previously receiving placebo in Study 312, started dosing with zonisamide with a dose of 1 mg/kg/day and titrated upwards with weekly dose increases until a dose of 8 mg/kg/day was reached at the end of the Transition Period (weeks 2 -11). Downtitration was allowed between the limits of 1 to 8 mg/kg/day during Transition Period. Subsequently, a 45-57 week Open-label period followed. Placebo dosing ceased in Open-label Period. Participants previously receiving zonisamide in Study 312 continued taking the same dose of study drug (8 mg/kg/day),supplemented with an increasing number of placebo capsules to mirror the up-titration regimen being followed by those previously receiving placebo.Down-titration was allowed between the limits of 1 to 8 mg/kg/day during Transition Period.Subsequently, a 45-57 week Open-label period followed.
    All Cause Mortality
    Zonisamide(Placebo During Core Study) Zonisamide (Zonisamide During Core Study)
    Affected / at Risk (%) # Events Affected / at Risk (%) # Events
    Total / (NaN) / (NaN)
    Serious Adverse Events
    Zonisamide(Placebo During Core Study) Zonisamide (Zonisamide During Core Study)
    Affected / at Risk (%) # Events Affected / at Risk (%) # Events
    Total 3/72 (4.2%) 7/72 (9.7%)
    Cardiac disorders
    Ventricular extrasystoles 0/72 (0%) 1/72 (1.4%)
    Gastrointestinal disorders
    Abdominal pain 1/72 (1.4%) 0/72 (0%)
    Infections and infestations
    Bronchitis 0/72 (0%) 1/72 (1.4%)
    Lymph gland infection 1/72 (1.4%) 0/72 (0%)
    Pneumonia 1/72 (1.4%) 0/72 (0%)
    Urinary tract infection 1/72 (1.4%) 0/72 (0%)
    Viral infection 0/72 (0%) 1/72 (1.4%)
    Injury, poisoning and procedural complications
    Foot fracture 0/72 (0%) 1/72 (1.4%)
    Nervous system disorders
    Partial seizures with secondary generalisation 0/72 (0%) 1/72 (1.4%)
    Status epilepticus 0/72 (0%) 1/72 (1.4%)
    Renal and urinary disorders
    Renal colic 0/72 (0%) 1/72 (1.4%)
    Respiratory, thoracic and mediastinal disorders
    Foreign body aspiration 0/72 (0%) 1/72 (1.4%)
    Other (Not Including Serious) Adverse Events
    Zonisamide(Placebo During Core Study) Zonisamide (Zonisamide During Core Study)
    Affected / at Risk (%) # Events Affected / at Risk (%) # Events
    Total 18/72 (25%) 25/72 (34.7%)
    Gastrointestinal disorders
    Abdominal pain 1/72 (1.4%) 4/72 (5.6%)
    Infections and infestations
    Nasopharyngitis 6/72 (8.3%) 9/72 (12.5%)
    Bronchitis 4/72 (5.6%) 3/72 (4.2%)
    Respiratory tract infection 2/72 (2.8%) 4/72 (5.6%)
    Investigations
    Weight decreased 6/72 (8.3%) 6/72 (8.3%)
    Metabolism and nutrition disorders
    Decreased Appetite 5/72 (6.9%) 4/72 (5.6%)
    Nervous system disorders
    Headache 4/72 (5.6%) 7/72 (9.7%)

    Limitations/Caveats

    [Not Specified]

    More Information

    Certain Agreements

    Principal Investigators are NOT employed by the organization sponsoring the study.

    There is NOT an agreement between Principal Investigators and the Sponsor (or its agents) that restricts the PI's rights to discuss or publish trial results after the trial is completed.

    Results Point of Contact

    Name/Title Eisai Inc.
    Organization Eisai Call Center
    Phone 888-422-4743
    Email
    Responsible Party:
    Eisai Limited
    ClinicalTrials.gov Identifier:
    NCT01136954
    Other Study ID Numbers:
    • E2090-E044-313
    • 2007-000198-53
    First Posted:
    Jun 4, 2010
    Last Update Posted:
    Jan 25, 2016
    Last Verified:
    Nov 1, 2015