Adjunctive Zonisamide in Primary Generalised Tonic Clonic Seizures

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ClinicalTrials.gov Identifier: NCT00692003

Recruitment Status : Terminated (Sponsor's decision)

First Posted : June 6, 2008

Results First Posted : October 12, 2012

Last Update Posted : March 14, 2017

Sponsor:

Information provided by (Responsible Party):

Eisai Inc. ( Eisai Limited )

Study Description

Brief Summary:

Zonisamide is already marketed for the treatment of partial seizures in epilepsy. This study is intended to provide evidence that zonisamide is safe and effective in the treatment of primary generalised tonic-clonic seizures. The total trial duration will be 5.5-6.5 months. After that subjects who have completed the study will be eligible to enrol in an open-label extension study until zonisamide is marketed for this indication or further development in this indication stops. This extension study will be described in a separate protocol (E2090-E044-316).

Condition or disease	Intervention/treatment	Phase
Epilepsy	Drug: Zonisamide Drug: Placebo	Phase 3

Study Design

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Study Type :	Interventional (Clinical Trial)
Actual Enrollment :	21 participants
Allocation:	Randomized
Intervention Model:	Parallel Assignment
Masking:	Double (Participant, Investigator)
Primary Purpose:	Treatment
Official Title:	A Double-blind, Randomised, Placebo-controlled Multi-centre Study to Assess the Efficacy and Safety of Adjunctive Zonisamide in Primary Generalised Tonic Clonic Seizures
Actual Study Start Date :	August 1, 2008
Actual Primary Completion Date :	November 2008
Actual Study Completion Date :	January 9, 2009

Resource links provided by the National Library of Medicine

MedlinePlus Genetics related topics: Pyridoxal 5'-phosphate-dependent epilepsy

MedlinePlus related topics: Epilepsy Seizures

Drug Information available for: Zonisamide

U.S. FDA Resources

Arms and Interventions

Arm	Intervention/treatment
Active Comparator: Zonisamide	Drug: Zonisamide 25-400 mg capsules orally once daily in the evening. Maximum study duration of 28 weeks comprising: Baseline Period (Week-8/-4 to Week 0) no treatment Titration Period (Week 0 to Week 4) <12 years old: 1 mg/kg; >= 12 years old: 50 mg daily titrated weekly until a dose of 5 mg/kg or 300 mg was reached by Week 4 Maintenance Period (Week 4 to Week 16) dose from Week 4 to be maintained (4 mg/kg or 200 mg in the event of dose limiting adverse events) Down Titration Period (4 weeks) Other Name: Zonegran
Placebo Comparator: Placebo	Drug: Placebo 25-400 mg Zonisamide Placebo capsules orally once daily in the evening. Maximum study duration of 28 weeks comprising: Baseline Period (Week-8/-4 to Week 0) no treatment Titration Period (Week 0 to Week 4) <12 years old: 1 mg/kg Zonisamide Placebo; >= 12 years old: 50 mg Zonisamide Placebo capsules daily titrated weekly until a dose of 5 mg/kg or 300 mg was reached by Week 4 Maintenance Period (Week 4 to Week 16) dose from Week 4 to be maintained (4 mg/kg or 200 mg in the event of dose limiting adverse events) Down Titration Period (4 weeks)

Arm

Intervention/treatment

Active Comparator: Zonisamide

Drug: Zonisamide

25-400 mg capsules orally once daily in the evening.

Maximum study duration of 28 weeks comprising:

Baseline Period (Week-8/-4 to Week 0) no treatment

Titration Period (Week 0 to Week 4) <12 years old: 1 mg/kg; >= 12 years old: 50 mg daily titrated weekly until a dose of 5 mg/kg or 300 mg was reached by Week 4

Maintenance Period (Week 4 to Week 16) dose from Week 4 to be maintained (4 mg/kg or 200 mg in the event of dose limiting adverse events)

Down Titration Period (4 weeks)

Other Name: Zonegran

Placebo Comparator: Placebo

Drug: Placebo

25-400 mg Zonisamide Placebo capsules orally once daily in the evening.

Maximum study duration of 28 weeks comprising:

Baseline Period (Week-8/-4 to Week 0) no treatment

Titration Period (Week 0 to Week 4) <12 years old: 1 mg/kg Zonisamide Placebo; >= 12 years old: 50 mg Zonisamide Placebo capsules daily titrated weekly until a dose of 5 mg/kg or 300 mg was reached by Week 4

Maintenance Period (Week 4 to Week 16) dose from Week 4 to be maintained (4 mg/kg or 200 mg in the event of dose limiting adverse events)

Down Titration Period (4 weeks)

Outcome Measures

Primary Outcome Measures :

Number of Participants Considered Responders as Assessed During the Maintenance Period [ Time Frame: Baseline (Week -8/-4 to Week 0) and Maintenance Phase (Week 4 to Week 16) ]
The number of participants who were considered responders during the 12 week Maintenance Period (Week 4 to Week 16). A responder was defined as a participant with a decrease from baseline in Primary Generalised Tonic-Clonic Seizures (PGTCS) frequency of >= 50% (i.e. 28-day PGTC seizure frequency in the period from Week 4 to the Week 16 visit compared to Week -8/-4 to randomization at Week 0). Each participant's response to treatment was assessed on the basis of their seizure diaries. The diary was dispensed at the Screening Visit and maintained by the participant (parent/caregiver) through out the titration and maintenance treatment periods until the Early termination Visit at Week 16. Due to early termination of the study by the Sponsor, no formal analyses were conducted.

Secondary Outcome Measures :

Absolute Change From Baseline in 28-day PGTC Seizure Frequency [ Time Frame: Baseline and up to 16 weeks ]
Absolute Change from Baseline in 28-day PGTC Seizure Frequency was assessed both for the Maintenance Period alone (Week 4 to Week 16) and for the entire double-blind treatment period (Week 0 to Week 16). Due to early termination of the study by the Sponsor, no formal analyses were conducted.

Eligibility Criteria

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Ages Eligible for Study:	6 Years to 65 Years (Child, Adult, Older Adult)
Sexes Eligible for Study:	All
Accepts Healthy Volunteers:	No

Criteria

Inclusion Criteria:

Subject is male or female and aged 6-65 years.
Subject has ≥ 3 PGTCS over the two months before screening and during the eight weeks Baseline Period with at least one seizure in each one month period. PGTCS must occur in the context of Idiopathic Generalized Epilepsy (IGE) and may be accompanied by other primary generalized seizures, provided these are also consistent with a diagnosis of IGE.
Subject (or parent/caregiver, for subjects below the age of consent) is willing to sign an informed consent form. For subjects below the age of consent in their country, where appropriate they must be willing to give informed (written or verbal) assent. Subjects from the age specified in local regulations will be required to sign an appropriate informed consent form.
Subject is taking a stable regimen of one or two other Antiepileptic Drugs (AEDs) for at least two weeks prior to Visit 1 (start of the Baseline Period).
Subject has a clinical diagnosis of any type of idiopathic generalized epilepsy which has PGTCS (and which may be accompanied by other generalized seizure types), according to the International League Against Epilepsy (ILAE) Classification of Epileptic Seizures (1981) and the ILAE Classification of Epilepsies and Epileptic Syndromes (1989). Diagnosis should have been established by clinical history, electroencephalogram (EEG) and computed tomography/magnetic resonance imaging (CT/MRI) of the brain consistent with idiopathic generalized epilepsy. CT/MRI scan should have been performed within five years of the screening visit or, if not available from this period, should be performed in the Baseline Period.
EEG should have been performed within one year of the screening visit or, if not available from this period, should be performed in the Baseline Period.
Female subjects are pre-menarchal, or if of childbearing potential, are not pregnant or lactating or are post-menopausal.
Female subjects of childbearing potential must abide by the one of the following medically acceptable contraceptive measures: oral contraception pill, contraceptive injections, implants or patches, intrauterine device in place for at least three months or vasectomised partner or abstinence throughout the study.
Subject has a body weight ≥ 20 kg.

Exclusion Criteria:

Subject has progressive or focal neurological disease (as determined by pre-existing brain imaging such as CT or MRI performed maximally five years before the screening visit), or clinically significant organic disease.
Subject has a history of, or results of clinical investigations (including EEG data) that are suggestive of, partial seizures as defined by the ILAE, including generalized tonic clonic seizures which are suspected to be secondarily generalized.
Subjects with cryptogenic or symptomatic generalized epilepsy.
Subjects with psychogenic seizures.
Subject has a history of status epilepticus within a year of screening while complying with AEDs.
Subject has seizures that only occur in clustered patterns.
Subject has a history of renal calculi or renal insufficiency (above the upper normal limits of creatinine).
Subject has a known diagnosis of human immunodeficiency virus (HIV) or hepatitis B or C.
Subject had a predisposing condition that might interfere with absorption, distribution, or excretion of zonisamide.
Subject has a history of sensitivity to sulfonamide drugs or zonisamide and its excipients.
Subject has a recent history of excessive alcohol use or drug abuse.
Subject has a history of suicide attempt in the five years before the screening visit..
Subject has abnormal screening laboratory values that were clinically significant.
Subject has a history of demonstrated non-compliance with treatment or the subject or parent/caregiver can be reasonably expected not to be compliant with study procedures or to complete the study.
Subject has participated in a study of an investigational drug or device within 30 days prior to screening.
Subject has received previous treatment with zonisamide.
Subject is treated with ketogenic diet or vagus nerve stimulator.
Subject has a history of necessary treatment with rescue benzodiazepines which is foreseen to continue during the study. Rescue benzodiazepines will not be allowed in this study (stable dosing with a benzodiazepine as (one of the) baseline anti-epileptic drug(s) is allowed).
Current psychosis or moderate to severe depression, or use of anti-psychotic drugs, MAOIs, tricyclic antidepressants, benzodiazepine or barbiturate treatment for disorders other than epilepsy, and stimulants (amphetamine derivatives) within 28 days before the screening visit.
Concomitant use of acetazolamide, carbonic anhydrase inhibitors such as topiramate and drugs with anticholinergic activity.
Concomitant use of felbamate or use of felbamate within two months prior to Visit 1.
Subject is not able to swallow capsules.
Subject is not in general good health as determined by medical history, physical exam and screening laboratory results.

Contacts and Locations

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To learn more about this study, you or your doctor may contact the study research staff using the contact information provided by the sponsor.

Please refer to this study by its ClinicalTrials.gov identifier (NCT number): NCT00692003

Locations

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Australia, New South Wales
Strategic Health Evaluators Pty Ltd
Chatswood, New South Wales, Australia, 2067
The Prince of Wales Hospital
Randwick, New South Wales, Australia, 2031
Australia, Victoria
Austin Health
Heidelburg, Victoria, Australia, 3084
The Royal Melbourne Hospital
Melbourne, Victoria, Australia, 3050
Australia
St. Vincents Hospital
Melbourne, Australia
Croatia
CH Split
Split, HR, Croatia, 10000
CH Sestre Milosrdnice University Hospital
Zagreb, HR, Croatia, 10000
UHC Zagreb
Zagreb, HR, Croatia, 10000
Czech Republic
Neurologicke oddeleni
Hradec Kralove, Czech Republic, 500 03
Private Neurologi Office
Kromeriz, Czech Republic, 767 01
Fakultni nemocnice Olomouc
Olomouc, Czech Republic, 775 20
Fakultni nemocnice s poliklinikou Ostrava
Ostrava, Czech Republic, 708 52
Fakultni nemocnice Plzen
Plzen, Czech Republic, 305 99
Nemocnice Na Homolce
Praha 5, Czech Republic, 150 30
Centrum neurologicke pece
Rychnov nad Kneznou, Czech Republic, 516 01
Estonia
West-Tallinn Central Hospital
Tallinn, Estonia, 10611
Neurodiagnostica AP OY
Tallinn, Estonia, 11312
Tartu University Hospital
Tartu, Estonia, 51014
Finland
Kuopio Epilepsy Center
Kuopio, SF, Finland, 70211
Oulu University Central Hospital
Oulu, Finland, 90220
Germany
Institut fur Diagnostik der Epilepsien
Berlin, Germany, 10365
Neurochirurgische Klinik der Universitat Freiburg
Freiburg, Germany, 79106
Interdisziplinares Epilepsiezentrum am Klinikum der Philipps-Universitat Marburg
Marburg, Germany, 35039
Neurologische Gemeinschaftspraxis
Munchen, Germany, 80333
Universitatsklinikum Ulm
Ulm, Germany, 89081
Hungary
National Institute of Psychiatry and Neurology
Budapest, Hungary, 1021
Heim Pal Hospital
Budapest, Hungary, 1089
Szent Istvan Hospital
Budapest, Hungary, 1091
Orszagos Idegsebeszeti Tudomanyos Intezet
Budapest, Hungary, 1145
Bethesda Hospital for Children
Budapest, Hungary, 1146
Bekes County Pandy Kalman Hospital
Gyula, Hungary, 5703
Bacs-Kiskun County ONK Hospital
Kecskemet, Hungary, 6000
Vas County Markusovszky Hospital
Szombathely, Hungary, 9400
Veszpem County Csolnoky F. Hospital
Veszpem, Hungary, 8200
Lithuania
Kaunas Medical University Hospital
Kaunas, Lithuania, 50009
Neuromeda
Kaunas, Lithuania, 50185
Vilnius University Hospital Santariskiu klinikos
Vilnius, Lithuania, 8661
Poland
Niepubliczny ZOZ KENDRON
Bialystok, Poland, 15-420
Wojewodzki Szpital Specjalistyczny im. M. Kopernika
Gdansk, Poland, 80-803
Specjalistyczny Szpital Wieloprofilowy
Katowice, Poland, 40-635
Centrum Neurologii Klinicznej
Krakow, Poland, 31-530
Szpital im. M. Kopernika
Lodz, Poland, 93-513
Uniwersytet Medyczny
Poznan, Poland, 60-355
Romania
Spitalul Clinic de Psihiatrie
Bucharest, Romania, 041914
Spitalul Universitar de Urgenta Bucuresti
Bucharest, Romania, 050098
Centrul Medical Sana
Bucharest, Romania, 11025
Spitalul Clinic Judetean de Urgenta Cluj
Cluj-Napoca, Romania, 400006
Spitalul Clinic Judetean de Urgenta Sf Spiridon Iasi
Iasi, Romania, 700111
Spitalul Clinic de Urgenta Sfanta Treime
Iasi, Romania, 700309
Spitalul Clinic Judetean de Urgenta Tg Mures
Tg Mures, Romania, 540136
Russian Federation
GOU VPO Krasnoyarskaya State Medical Academy of Roszdrav
Krasnoyarsk, Russian Federation, 660022
FGU Moscow Research Institute of Psychiatry of Roszdrav
Moscow, Russian Federation, 107076
GOU VPO Russian State Medical University of Roszdrav
Moscow, Russian Federation, 117997/119034
GOU VPO Smolensk State Medical Academy of Roszdrav
Moscow, Russian Federation, 119049
GOU VPO Moscow State University of Medicine and Dentistry of Roszdrav
Moscow, Russian Federation, 127473 / 107006
GOU VPO Novosibirsk State Medical University of Roszdrav
Novosibirsk, Russian Federation, 630091
GOU VPO Smolensk State Medical Academy of Roszdrav
Smolensk, Russian Federation, 214018
GOU VPO Smolensk State Medical Academy of Roszdrav
Smolensk, Russian Federation, 214019
St. Petersburg State Medical Pediatric Academy
St. Petersburg, Russian Federation, 194100
GU St. Petersburg Research Institute of Psychoneurology
St.Petersburg, Russian Federation, 192019
GOU VPO St. Petersburg State Medical University
St.Petersburg, Russian Federation, 197022
Yaroslavskaya State Medical Academy
Yaroslavl, Russian Federation, 150000
Serbia
Clinical Center of Serbia
Belgrade, Serbia, 11000
University Medical Center Zvezdara
Belgrade, Serbia, 11000
Clinical Center Kragujevac
Kragujevac, Serbia, 34000
Clinical Center of Nis
Nis, Serbia, 18000
Ukraine
Tsentr Psihosomatychnoyi Patologiyi Dnipropetrovskoyi oblasnoyi klinichnoyi likarni imeni Mechnikova
Dniepropetrovsk, Ukraine, 49005
Derzhavna Ustanova Institut Nevrologiy
Kharkiv, Ukraine, 61068
Kyiv City Psychiatric Hospital #2, Poliklinichne Viddilenya
Kyiv, Ukraine, 2660
Miska Klinichna psihonevrologichna Tsentr Epilepsiyi
Kyiv, Ukraine, 3080
Lvivskyiy oblasnyi Protyepileptuchnyy tsentr
Lviv, Ukraine, 7910
Odesskyy Derzhavnyy Medychnyy Universitet
Odesa, Ukraine, 65006
Vinnitskyy Natsionalnyy Medychnyy Universitet
Vinnitsa, Ukraine, 21005

Sponsors and Collaborators

Eisai Limited

Investigators

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Study Director:	Rob Van Maanen	Eisai Limited

More Information

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Responsible Party:	Eisai Limited
ClinicalTrials.gov Identifier:	NCT00692003
Other Study ID Numbers:	E2090-E044-315 Eudra ID #2007-003557-91.
First Posted:	June 6, 2008 Key Record Dates
Results First Posted:	October 12, 2012
Last Update Posted:	March 14, 2017
Last Verified:	February 2017

Additional relevant MeSH terms:

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Seizures Nervous System Diseases Neurologic Manifestations Zonisamide Anticonvulsants	Calcium Channel Blockers Membrane Transport Modulators Molecular Mechanisms of Pharmacological Action Calcium-Regulating Hormones and Agents Physiological Effects of Drugs

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