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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT01091662
Other study ID # 093-046
Secondary ID
Status Completed
Phase Phase 3
First received March 17, 2010
Last updated July 15, 2016
Start date June 2010
Est. completion date November 2012

Study information

Verified date July 2016
Source Sunovion
Contact n/a
Is FDA regulated No
Health authority United States: Food and Drug Administration
Study type Interventional

Clinical Trial Summary

This is an 18-week, double-blind, multicenter study with gradual conversion from previous antiepileptic therapy to eslicarbazepine acetate monotherapy in subjects with partial epilepsy.


Description:

This is an 18-week, double-blind, randomized, historical control, multicenter study with gradual conversion to monotherapy in subjects with partial onset seizures who are not well controlled by current AEDs. The 18 week double-blind treatment period consists of a 2-week titration period, 6-week taper or conversion period, and a 10-week monotherapy period. This study was previously posted by Sepracor Inc. In October 2009, Sepracor Inc. was acquired by Dainippon Sumitomo Pharma., and in October 2010, Sepracor Inc's name was changed to Sunovion Pharmaceuticals Inc.


Recruitment information / eligibility

Status Completed
Enrollment 172
Est. completion date November 2012
Est. primary completion date November 2012
Accepts healthy volunteers No
Gender Both
Age group 16 Years to 70 Years
Eligibility Inclusion Criteria:

- Diagnosis of partial epilepsy as defined in the Classification of Seizures of the International League Against Epilepsy (ILAE) (simple partial seizures with observable motor component, or complex, with or without secondary generalization)

- Medical history of seizures;

- Absence of confounding factors (pseudoseizures, syncope);

- Documented EEG recording (done within 5 years prior to screening) consistent with focal onset epilepsy

- Documented CT or MRI scan conducted within 10 years prior to screening, showing the absence of a structural abnormality (eg, tumor or malformation)

- = 4 partial onset seizures during the 8 weeks prior screening with no 28-day seizure free period

- Stable treatment with 1-2 AEDs during the last 4 weeks prior to screening

- Subjects must have the ability to comprehend the informed consent form and be willing to provide informed consent. For subjects who are unable to comprehend the written consent, a witness/caregiver who is able to describe and provide an understanding of the informed consent to the subject must sign the consent form on behalf of the subject.

- Subjects must give written informed consent prior to participation in the study. For subjects <18 years of age, the informed consent must be signed by the subject's parent or legal guardian, and, when appropriate and/or required by state or local law, minor subjects must give written informed assent prior to participation in the study. Subjects of Asian ancestry are required to give written informed consent for genotyping. All subjects must sign a HIPAA Form. All females of child bearing potential must also sign the "Women of Childbearing Potential" Addendum.

- A female subject is eligible to enter and participate in the study if she is of:

- Non-childbearing potential (ie, physiologically incapable of becoming pregnant, including any female who is pre-menarchal or post-menopausal);

- Child-bearing potential (all females =65 years of age), has a negative pregnancy test at screening and agrees to satisfy contraception requirements

Exclusion Criteria:

- Subjects with only simple partial seizures without a motor component

- Presence of generalized seizure syndromes (eg, juvenile myoclonic epilepsy or Lennox-Gastaut syndrome)

- History of pseudo-seizures

- Current seizures related to an acute medical illness

- Seizures secondary to metabolic, toxic or infectious disorder or drug abuse

- Status epilepticus within 2 years prior to screening

- Seizures only occurring in a cluster pattern

- Subjects taking 2 of the following sodium channel blocking AEDs: phenytoin, carbamazepine, oxcarbazepine, or lamotrigine

- Subjects taking 2 AEDs with both being in the upper dose range (defined as approximately two-thirds of the defined daily dose)

- Subjects taking more than 2 AEDs

- Subjects with progressive structural central nervous system lesion or progressive encephalopathy

- Psychiatric exclusion criteria

- Medical exclusion criteria: known renal insufficiency (estimated creatinine clearance [CrCL]) <60 mL/min based on serum creatinine using the Cockcroft-Gault formula

- Clinical and laboratory exclusion criteria: Subjects of Asian ancestry who tests positive for the presence of the HLA-B*1502 allele

- Subjects who have been on benzodiazepines, phenobarbital, or primidone on a regular basis within 3 months prior to screening

- Subjects taking antipsychotics, tricyclic antidepressants, anxiolytics, sedative hypnotics including non-benzodiazepines, central opioid agonists/antagonists, monoamine oxidase inhibitors (MAOIs) within at least 5 half lives (or for at least 2 weeks whichever is longer) prior to randomization

- Subjects presently on felbamate or vigabatrin

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment


Related Conditions & MeSH terms


Intervention

Drug:
Eslicarbazepine acetate 1600 mg
1600 mg once per day
Eslicarbazepine acetate 1200 mg
1200 once per day

Locations

Country Name City State
Bulgaria Multirprofile Hospital for Active Treatment "Pulse," AD, town of Blagoevgrad Blagoevgrad
Bulgaria University Multiprofile Hospital for Active Treatment "Dr. Georgi Stranski," EAD, town of Pleven Pleven
Bulgaria Second Multiprofile Hospital for Active Treatment - Sofia, AD, city of Sofia Neurology Department Sofia
Bulgaria Diagnostic and Consultative Center "Equita" EOOD, town of Varna Varna
Czech Republic Neurologicka ordinance Kolejni Praha
Czech Republic Poradna pro epilepsie Koterova Zin
Czech Republic Cerebrovaskularni poradna s.r.o. Ostrava Tiebovice
Czech Republic CTC Rycnov nad Kneznou Rychnov nad Kneznou Praugue
Czech Republic Policlinic Chocen, private neurology Smetanova Chocen
Serbia Clinic of Neurology, Clinical Center of Serbia Belgrade
Serbia Institute of Mental Health, Department of epilepsy and clinical neurophysiology Palmoticeva Belgrade
Ukraine Communal Institution "Dnipropetrovsk Regional Clinical Hospital named after l.l. Mechnikov" Regional Center of psychosomatic disorders, Psychoneurology department for patients with psychosomatic disorders and borderline condtions Dnipropetrovsk
Ukraine Communal Medical and Preventive Treatment Institution "Regional Clincal Psychiatric Hospital" Donetsk National Medical University Donetsk
Ukraine State Institution "Institute of neurology, psychiatry and narcology of AMS of Ukraine" Department of cerebrovascular patology Kharkiv
Ukraine State Institution "Institute of the Health Care of Children & Adolescents of Academy of Medical Sciences of Ukraine" Dept of Psychiatry Kharkov
Ukraine State Treatment and Prevention Institution Kharkov
Ukraine State Institution Railway Clinical Hospital #1 of Kiev Railway Station of DTGO South Western Railroad Psycho-neurological Department Kiev
Ukraine Communal Institution "Lviv Regional Clinical Psychiatric Hospital" Department #20, Lviv National Medical University, named after Danylo Lviv
Ukraine Communal Institution "Odessa Regional Clinical Psych Hospital #1" Department of Day Care Odessa
Ukraine Poltava Regional Clinical Psychiatric Hospital named O.F. Maltsev Poltava
Ukraine Crimean Republic Institution "Clinical Psychiatric Hospital #1" Simferopol
Ukraine Communal Institution "Vinnytsia Regional Psycho-Neurological Hospital named after O.I. Yuschenko, Vinnytsia National Medical University named after M.I. Pirogov, Dispensary department, Department of Psychiatry and Addictology Vinnytsia
United States Community Clinical Research Inc. Austin Texas
United States Kern County Neurological Medical Group, INC. Bakersfield California
United States The Sandra and Malcom Berman Brain & Spine Institute Baltimore Maryland
United States Montefiore Medical Center Bronx New York
United States Brownwood Regional Medical Center Brownwood Texas
United States Lahey Clinic Burlington Massachusetts
United States Ohio Clinical Research Partners, LLC Canton Ohio
United States University Hospitals Case Medical Center Cleveland Ohio
United States Arkansas Neurology Conway Arkansas
United States MD Dallas Texas
United States Vital Clinical Research DeSoto Texas
United States Wayne State University/Detroit Medical Center Detroit Michigan
United States Specialty Nuerology, PC Englewood Colorado
United States Neuro-Pain Medical Center Fresno California
United States Minneappolis Clinic of Neurology Golden Valley Minnesota
United States East Carolina Neurology Greenville North Carolina
United States Northeast Regional Epilepsy Group Hackensack New Jersey
United States Palm Springs Research Institute, Inc Hialeah Florida
United States Josephson Wallack Munshower Neurology PC Indianapolis Indiana
United States University of Kentucky Department of Neurology Lexington Kentucky
United States University of Arkansas for Medical Sciences Little Rock Arkansas
United States West Los Angeles VA Medical Center Los Angeles California
United States Marshfield Clinic Marshfield Wisconsin
United States Miami Children's Hospital Miami Florida
United States Pharma Care Research LLC Miami Florida
United States Regional Epilepsy Center Milwaukee Wisconsin
United States UMDNJ DOC 8th Floor 8100 Newark New Jersey
United States Dent Neurologic Institute Orchard Park New York
United States Bay Neurological Institute Panama City Florida
United States Drexel University College of Medicine Philadelphia Pennsylvania
United States Temple University School of Medicine Philadelphia Pennsylvania
United States Global Medical Institutes, LLC Princeton New Jersey
United States Louisiana State University Health Science Center - Shreveport Shreveport Louisiana
United States SUNY Upstate Medical University Department of Neurology Syracuse New York
United States Shore Neurology, PA Toms River New Jersey
United States University of Arizona Health Sciences Center Tucson Arizona
United States Tulsa Clinical Research LLC Tulsa Oklahoma
United States Loveland Scientific Resources Inc. Venice Florida
United States Neurosearch II Inc. Ventura California

Sponsors (1)

Lead Sponsor Collaborator
Sunovion

Countries where clinical trial is conducted

United States,  Bulgaria,  Czech Republic,  Serbia,  Ukraine, 

References & Publications (1)

Jacobson MP, Pazdera L, Bhatia P, Grinnell T, Cheng H, Blum D; study 046 team. Efficacy and safety of conversion to monotherapy with eslicarbazepine acetate in adults with uncontrolled partial-onset seizures: a historical-control phase III study. BMC Neurol. 2015 Mar 28;15:46. doi: 10.1186/s12883-015-0305-5. — View Citation

Outcome

Type Measure Description Time frame Safety issue
Primary Cumulative 112-day Exit Rate as Estimated by Kaplan-Meier Method Cumulative exit rate was defined as the proportion of subjects meeting at least one of the following five exit criteria over a 16-week study period (from start of AED taper/con. period (Wk 3) to end of double blind monotherapy period (Wk 18)).1.One episode of status epilepticus.2.One secondary gen. partial seizure (in subjects who did not have gen.seizures during 6 mo. prior to screening).3.A two fold increase in any consecutive 28 day seizure rate compared to the highest consecutive 28 day seizure rate during the 8 week baseline period. 4.A two fold increase in any consecutive 2 day seizure rate compared to the highest consecutive 2 day seizure rate during the 8 week baseline period. If the highest number of seizures in any consecutive 2 day period during the 8 week baseline was 1 then 3 seizures in a consecutive 2 day period was required to exit.
5.Worsening of seizures or increase in seizure frequency considered serious or requiring intervention as judged by the investigator
From beginning of Week 3 to end of Week 18 No
Secondary Proportion (%) of Subjects That Are Seizure-free During the 10-week Double-blind Monotherapy Treatment Period. Seizure-free subjects during the monotherapy period were determined as subjects who had seizure assessments during the monotherapy period, and did not have any seizures in the 10 weeks between Visits 6 and 9 (Weeks 9 through 18). Subjects who discontinued during this period were considered not seizure-free even if they were seizure-free at the time of discontinuation, i.e., to be considered seizure-free, subjects must complete the 10-week period without any seizures. Week 9 through 18 No
Secondary Percentage of Subjects Seizure-free During the Last 4 Weeks on Eslicarbazepine Acetate Monotherapy. Percentage of participants that were Seizure-free during the last four weeks of monotherapy were determined as subjects who had seizure assessments during the 4 weeks between Visits 8 and 9 (Weeks 15 through 18), and did not have any seizures. Week 15 through 18 No
Secondary Completion Rate (% of Subjects Completing the 18 Weeks of Double-blind Treatment). Subjects completing the study were determined as subjects who completed the 18 weeks of double-blind treatment. 18 weeks No
Secondary Completion Rate During the 10 Weeks of Monotherapy (% of Subjects Entering the Monotherapy Period Who Complete). Monotherapy completion rate was defined as the proportion (%) of subjects entering the monotherapy period who completed the 10 weeks of monotherapy treatment. Week 8 through 18 No
Secondary Time on Eslicarbazepine Acetate Monotherapy. The start of the monotherapy period was defined as the date of termination of all other AEDs while taking study monotherapy medication. Time on monotherapy was defined from the start of monotherapy period to the last dose of monotherapy treatment. Week 8 to Week 18 No
Secondary Change in Seizure Frequency From Baseline. The relative (%) change in standardized seizure frequency was evaluated for four periods: titration (Weeks 1 to 2), AED taper/conversion (Weeks 3 to 8), monotherapy (Weeks 9 to 18), and double-blind (Weeks 1 to 18). 18 weeks, Double-blind:weeks 1-18; Baseline: weeks -8to -1; titration: weeks 1 to 2; AED taper/conversion: weeks 3 to 8; monotherapy; weeks 9 to 18 No
Secondary Responder Rate (Proportion [%] of Subjects With a =50% Reduction of Seizure Frequency From Baseline). Responder rate was defined as the proportion (%) of subjects with a = 50% reduction of seizure frequency from baseline. This analysis was done for the titration (Weeks 1 to 2), AED taper/conversion (Weeks 3 to 8), monotherapy (Weeks 9 to 18), and double-blind (Weeks 1 to 18) periods. Week 0 to Week 18, Double-blind weeks 1-18; baseline: weeks -8 to -1; Titration: weeks 1-2; AED taper/conversion; weeks 3-8; monotherapy weeks 9-18 No
Secondary Proportion (%) of Subjects Reaching Each Exit Criteria The proportion (%) of subjects reaching each of the 5 exit criteria-1.One episode of status epilepticus.2.One secondary gen. partial seizure (in subjects who did not have gen.seizures during 6 mo. prior to screening).3.A two fold increase in any consecutive 28 day seizure rate compared to the highest consecutive 28 day seizure rate during the 8 week baseline period. 4.A two fold increase in any consecutive 2 day seizure rate compared to the highest consecutive 2 day seizure rate during the 8 week baseline period. If the highest number of seizures in any consecutive 2 day period during the 8 week baseline was 1 then 3 seizures in a consecutive 2 day period was required to exit.
5.Worsening of seizures or increase in seizure frequency considered serious or requiring intervention as judged by the investigator
Week 1 to Week 18, (beginning of week 1 to end of week 18) No
Secondary Change in Total Score From Baseline in 31-Item Quality of Life in Epilepsy (QOLIE-31). The QOLIE-31 overall score was obtained by using a weighted average of multi-item scale scores. The recorded responses were converted to 0-100 point scales. The mean of the individual item scores in each subgroup were calculated, with higher converted scores reflecting better quality of life. Week 0 to Week 18, Baseline: Day 0: End of AED taper/conversion period: end of week 8; End of monotherapy period: end of week 18 No
Secondary Change in Total Score in Montgomery-Asberg Depression Rating Scale (MADRS),From Baseline . The total score of MADRS is defined as the sum of all individual item scores. From 0-60, high score indicates more severe Week 0 to Week 18,baseline day 0; end of AED taper/conversion period; end of week 8; end of monotherapy period; end of week 18 No
Secondary Change in Total Score of MADRS From Baseline in Those Subjects With a MADRS Score of =14 at Randomization. The total score of MADRS is defined as the sum of all individual item scores. From 0-60, higher score indicates more severe Week 0 to Week 18, baseline:day 0;end of AED taper/conversion period; end of week 8; end of monotherapy period: end of week 18 No
Secondary Proportion (%) of Subjects With Increase of Body Weight >= 7% From Baseline 18 Week Double-blind treatment period Yes
Secondary Proportion (%) of Subjects With Normal Baseline Sodium Reaching Blood Sodium =135 mmol/L, =130 mmol/L, and =125 mmol/L. Proportion (%) of Subjects With Normal Baseline Sodium Reaching Blood Sodium =135 mmol/L, =130 mmol/L, and =125 mmol/L Week 0 to Week 18 Yes
Secondary Proportion (%) of Events in Each Classification of the Columbia Suicide Severity Rating Scale (C SSRS). 18 Week Double-blind treatment period Yes
Secondary Standardized Seizure Frequency (SSF) by Period Seizure frequency was evaluated by using a standardized frequency per 4 weeks (28 days). It was evaluated for five periods: baseline (Weeks -8 to -1), titration (Weeks 1 to 2), AED taper/conversion (Weeks 3 to 8), monotherapy (Weeks 9 to 18), and double-blind (Weeks 1 to 18). Double-blind: week to 18; Baseline: weeks -8 to -1; titration: weeks 1 to 2; AED taper/conversion weeks 3 to 8; monotherapy: weeks 9 to 18 No
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