Retigabine Efficacy and Safety Trial for Partial Onset Refractory Seizures in Epilepsy

Phase 3

Completed

• Conditions: Seizures
• Interventions: Drug: Retigabine; Drug: Placebo

• Registration Number: NCT00235755
• Lead Sponsor: GlaxoSmithKline

Brief Summary

This Phase 3 study is being conducted to evaluate the efficacy and safety of retigabine dosed at 900 mg/day and 600 mg/day, in three equally divided doses, compared with placebo in patients with epilepsy who are receiving up to three established antiepileptic drugs (AEDs).

Detailed Description

This Phase 3 study is being conducted in Europe, Israel, Australia, and South Africa to evaluate the efficacy and safety of retigabine dosed at 900 mg/day and 600 mg/day, in three equally divided doses, compared with placebo in patients with epilepsy who are receiving up to three established antiepileptic drugs (AEDs). The primary objective is to demonstrate a superior change in total partial seizure frequency for four weeks from baseline to the double-blind period. The proportion of responders (greater than or equal to 50% reduction in seizure frequency for four weeks from baseline to the double-blind period) will also be evaluated.

Study Timeline

• Study First Submitted: 2005-10-06
• Study First Submitted QC: 2005-10-06
• Study First Posted: 2005-10-10
• Study Start: 2005-12
• Primary Completion: 2008-04
• Study Completion: 2008-04
• Results First Submitted: 2011-07-07
• Results First Submitted QC: 2011-09-30
• Results First Posted: 2011-11-06
• Status Verified: 2017-03
• Last Update Submitted: 2017-03-23
• Last Update Posted: 2017-04-21

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 539

Inclusion Criteria

• Diagnosis of refractory epilepsy with simple or complex partial onset seizures with or without secondary generalization
• 28-day partial seizure frequency rate of four or more partial seizures over the 8-week baseline phase
• Currently treated with up to three established AEDs
• Vagal Nerve Stimulator may be included

Exclusion Criteria

• Existing medical or psychiatric condition which could affect patient's health or compromise ability to participate in the study
• Clinically significant abnormalities on physical exam, vital signs, ECG, or liver function tests
• Impaired renal function (creatinine clearance less than 50 mL/minute)
• Evidence of progressive central nervous disease, lesion, or encephalopathy
• History of primary generalized seizures
• History of clustering or flurries or status epilepticus within 12 months of study entry

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Retigabine 600 mg	Retigabine	-
Retigabine 900 mg	Retigabine	-
Placebo	Placebo	-

Primary Outcome Measures

Name	Time	Method
Number of Participants Classified as Responders and Non-responders During the Maintenance Phase	Week 5 through Week 16	Responders were participants with at least a 50% reduction in the 28-day total partial seizure frequency in the Maintenance Phase as compared to the Baseline period.
Percent Change in the 28-day Total Partial Seizure (PS) Frequency From Baseline (BL) to the End of the Double-blind (DB) Phase (Titration and Maintenance Phases)	Baseline (Week -7 through Week 0), DB Phase (Week 1 through Week 16)	28-day total PS (PSs \[also called focal seizures\] are seizures limited to a specific area of the brain) frequency in the BL period = (Number \[No.\] of total PSs reported in the BL period divided by the No. of days of available total PS data in the BL period) x 28 days. 28-day total PS frequency in the DB period = (No. of total PSs reported in the DB period divided by the No. of days of available total PS data in the DB period) x 28 days. Percent change = (\[value in the DB period minus value at BL\] divided by the BL value) x 100%. Negative valu es indicate a reduction in seizure frequency.

Secondary Outcome Measures

Name	Time	Method
Number of Participants Who Were Responders and Non-responders During the DB Phase	Week 1 through Week 16	Responders were participants with at least a 50% reduction in the 28-day total partial seizure frequency in the DB Phase as compared to the Baseline period. Participants without any post-baseline data were considered non-responders.
Percent Change From Baseline (BL) in the 28-day Total Partial Seizure Frequency During the Maintenance Phase	Baseline (Week -7 through Week 0), Week 5 through Week 16	28-day total partial seizure frequency in the BL period = (No. of total partial seizures reported in the BL period divided by the No. of days of available total partial seizure data in the BL period) x 28 days. 28-day total partial seizure frequency in the Maintenance Phase = (No. of total partial seizures reported in the Maintenance Phase divided by the No. of days of available total partial seizure data in the same phase) x 28 days. Percent change = (value in the Maintenance Phase minus value at BL divided by the BL value) x 100%. Negative values indicate a reduction in seizure frequency.
Number of Participants With a Reduction in the 28-day Total Partial Seizure Frequency From Baseline to the End of DB Phase (Titration and Maintenance Phases) by Indicated Quartile Reduction Categories	Baseline (Week -7 through Week 0), Week 1 through Week 16	Participants who experienced a reduction from Baseline in the 28-day total partial seizure frequency were categorized as having a reduction of 75-100%, 50-\<75%, 25-\<50%, or \<25%, in addition to having no reduction. This quartile cutting was specified in the study protocol. Participants without any post-baseline data are included in the "No reduction" category.
Number of Participants With a Reduction in the 28-day Total Partial Seizure Frequency From Baseline to the DB Phase (Titration and Maintenance Phases) by Indicated Decile Reduction and Increase Categories	Baseline (Week -7 through Week 0), Week 1 through Week 16	Participants who experienced a reduction from Baseline in the 28-day total partial seizure frequency were categorized in decile cutting, i.e., reduction categories of 90-100%, 80-\<90%, 70-\<80%, 60-\<70%, 50-\<60%, 40-\<50%, 30-\<40%, 20-\<30%, 10-\<20%, \>0-\<10%, and increase categories of 0-10%, \>10-20%, \>20-30%, \>30% (FDA endpoint). Participants without any post-baseline data were included in the category 0-10% increase category.
Number of Participants With the Indicated Reduction From Baseline in the 28-day Total Partial Seizure Frequency During the Maintenance Phase	Baseline (Week -7 through Week 0), Week 5 through Week 16	Participants who experienced a reduction from Baseline in the 28-day total partial seizure frequency were categorized as having a \>75%, a 50-75%, or a \<50% reduction, in addition to having no reduction (EMEA endpoint).
Number of Participants Who Experienced the Indicated Level of Exacerbation and Reduction in the 28-day Total Partial Seizure Frequency From Baseline During the Maintenance Phase	Baseline (Week -7 through Week 0), Week 5 through Week 16	Participants who experienced an exacerbation from Baseline in the 28-day total partial seizure frequency were categorized as having a 0-25% or a \>25% increase (EMEA endpoint). The number of participants experiencing a \>0% reduction from Baseline in the 28-day total partial seizure frequency are also presented.
Number of Participants Reporting New Seizure Types in the Indicated Categories During the DB Phase (Titration and Maintenance Phases) That Were Not Reported at Baseline	Baseline (Week -7 through Week 0), Week 1 through Week 16	New seizure types included those seizures which were not reported by any participant at Baseline.
Number of Participants Who Were Seizure-free During the DB Phase (Titration and Maintenance Phases)	Week 1 through Week 16	Participants were considered to be seizure-free if they had not reported any seizures during the DB treatment period (Weeks 1-18). For a participant to be seizure free during the DB Phase, the participant had to be seizure free both Week 7 to Week 18 and Week 1 to Week 6. A participant could be seizure free Week 7 to Week 18 (during the Maintenance Phase), but not seizure free Week 1 to Week 6. Hence, there are fewer participants being reported as seizure free from Week 1 to Week 18 than from Week 7 to Week 18.
Patient Global Impression (PGI) Score at the End of the Maintenance Phase	Week 16/end of treatment phase	PGI is a participant-rated scale of improvement that was administered at the end of the Maintenance Phase in order to assess the participant's impression of his or her own improvement. PGI assessments were scored using a 7-point scale: 1, very much improved; 2, much improved; 3, minimally improved; 4, no change; 5, minimally worse; 6, much worse; or 7, very much worse.
Number of Participants With a >=7% Increase in Body Weight During Weeks 2 and 4 of theTitration Phase and Weeks 6, 8, 12, and 16 of the Maintenance Phase	Weeks 2 and 4 of Titration Phase and Weeks 6, 8, 12, and 16 of Maintenance Phase	The number of participants with recorded weight gain of \>=7% over their baseline weight was measured.
Number of Participants Who Were Seizure-free During the Maintenance Phase	Week 5 through Week 16	Participants were considered to be seizure-free if they had not reported any seizures during the Maintenance Phase.
Percentage of Seizure-free Days During the DB Phase (Titration and Maintenance Phases)	Week 1 through Week 16	A seizure-free day was a day without any seizures. For a participant to be seizure free during the DB Phase, the participant had to be seizure free both Week 7 to Week 18 and Week 1 to Week 6. A participant could be seizure free Week 7 to Week 18 (during the Maintenance Phase), but not seizure free Week 1 to Week 6. Hence, there are fewer participants being reported as seizure free from Week 1 to Week 18 than from Week 7 to Week 18. The percentage of seizure-free days was calculated as the total number of days without seizures in the DB period divided by the number of days in DB period x 100%.
Percentage of Seizure-free Days During the Maintenance Phase	Week 5 through Week 16	A seizure-free day was a day without any seizures. The percentage of seizure-free days was calculated as the total number of days without seizures in the Maintenance Phase divided by the number of days in the Maintenance Phase x 100%.
Clinical Global Impression-Improvement (CGI-I) Score at the End of the Maintenance Phase	Week 16/end of treatment phase	Clinical Global Impression of Improvement (CGI-I) is a 7-point scale that requires the clinician to assess how much the participant's illness has improved or worsened relative to a baseline state at the beginning of the treatment. Scores on the scale are rated as: 1, very much improved; 2, much improved; 3, minimally improved; 4, no change; 5, minimally worse; 6, much worse; or 7, very much worse.
Number of Participants Whose Clinical Laboratory Values Were Deemed an Adverse Event by the Investigator (>=2% in Any Treatment Arm)	Week 1 through Week 16	Clinically important changes in laboratory values were to be reported as an adverse event if they met one of the following criteria: (1) intervention required; (2) change in dose of study drug required; (3) other treatment/therapy required; (4) association with other diagnoses.
Quality of Life Assessed by Quality of Life in Epilepsy-Problems Questionnaire (QOLIE-31-P) at BL (Week 0) and Weeks 4, 8, and 16	End of Baseline (Week 0), Weeks 4, 8, and 16	The QOLIE-31-P is a 31-item questionnaire evaluating a participant's QOL perception in 7 domains: seizure worry, emotional well being, energy/fatigue, cognitive functioning, medication effects, social functioning, overall QOL. Precoded numeric values for some domains are such that a higher number reflects a more favorable health state; others are such that a higher number reflects a less favorable state. Precoded values are first converted to 0-100 point scores; higher converted scores always reflect better QOL. The overall score is derived by weighting and then summing the 7 domain scores.
Number of Participants Who Reported the Indicated Renal and Urinary Disorder Adverse Events at a Frequency Threshold of 2% (in Any Treatment Arm)	Week 1 through Week 16	A summary of the adverse events classified as renal or urinary disorders and in which at least 2% (rounded to an integer) of participants in any treatment arm reported during the study is presented.
Change From Baseline in Post-void Residual Urine Volume at Weeks 8 and 16 of the Maintenance Phase	Baseline (Week -7 through 0), Weeks 8 and 16	Post-void residual (PVR) urine refers to the amount of urine remaining in the bladder after normal urination. To investigate the possible effects of retigabine on bladder function, all participants underwent post-void residual bladder ultrasound at Baseline and during the Maintenance Phase. The PVR bladder ultrasound was performed by a urologist, a qualified ultrasound technician, or a qualified study nurse who was certified to do PVR bladder ultrasound. Change from Baseline in PVR residual volume was calculated as the values at Week 10 and Week 16 minus the value at Baseline.

Trial Locations

Locations (70)

Royal Prince Alfred Hospital; 🇦🇺 Camperdown, New South Wales, Australia

Neurological Clinic-Texas; 🇺🇸 Dallas, Texas, United States

University of Bonn -- Department for Epileptplogy; 🇩🇪 Bonn, Germany

Universitaetsklinik Mainz Neurologische Klinik; 🇩🇪 Mainz, Germany

Rambam Medical Center; 🇮🇱 Haifa, Israel

Specjalistyczna Przychodnia Lekarska Medikard; 🇵🇱 Padlewskiego 4, Plock, Poland

Katedra i Klinika Neurologii Slaskiej Akademii Medycznej; 🇵🇱 Katowice, Poland

Wojewodzki Szpital Specjalistyczny im.Mikolaja Kopernika; 🇵🇱 Gdansk, Poland

Instytut Psychiatrii i Neurologii II Oddzial Neurologii; 🇵🇱 Warsaw, Poland

City Hospital # 1; 🇷🇺 Moscow, Russian Federation

District Antiepileptic Centre City Clinical Hospital # 71; 🇷🇺 Moscow, Russian Federation

Triple M Research; 🇿🇦 Port Elizabeth, East Cape, South Africa

Military Medical Academy n.a. S.M.Kirov; 🇷🇺 St. Petersburg, Russian Federation

St.Petersburg State Medical University n.a. I.P.Pavlov; 🇷🇺 St. Petersburg, Russian Federation

Wilgers MR & Medical Centre; 🇿🇦 Pretoria, Gauteng, South Africa

University of the Free State; 🇿🇦 Bloemfontein, Gauteng, South Africa

Carl Bremer Hospital; 🇿🇦 Belville, West Cape, South Africa

Panorama Medi-Clinic; 🇿🇦 Cape Town, South Africa

Hospital de La Santa Creu i Sant Pau; 🇪🇸 Barcelona, Spain

Hospital de Cruces; 🇪🇸 Bilbao, Spain

Groote Schuur Hospital; 🇿🇦 Cape Town, Western Cape, South Africa

Hosp. Virgen de las Nieves; 🇪🇸 Granada, Spain

Hosp de Donostia; 🇪🇸 San Sebastian, Spain

Hospital Ruber Internacional de Madrid; 🇪🇸 Madrid, Spain

Kharkiv State Medical University; 🇺🇦 Kharkiv, Ukraine

Institute of Neurology, Psychiatry and Narcology of AMS, Ukr; 🇺🇦 Kharkov, Ukraine

Odessa Regional Clinical Hospital; 🇺🇦 Odessa, Ukraine

Epilepsy Center of Municipal Clinical Psychoneurological Hospital; 🇺🇦 Kiev, Ukraine

The James Cook University Hospital; 🇬🇧 Middlesbrough, Mersyd, United Kingdom

Western Infirmary (Epilepsy); 🇬🇧 Glasgow, United Kingdom

Fylde Coast Hospital; 🇬🇧 Blackpool, United Kingdom

Inkosi Albert Luthuli Central Hospital; 🇿🇦 Durban, KwaZulu-Natal, South Africa

AZ Sint-Jan; 🇧🇪 Brugge, Belgium

Theatinerstrasse 44; 🇩🇪 Munich, Germany

Royal Melbourne Hospital; 🇦🇺 Parkville, Victoria, Australia

Hopital Neurologique Pierre Wertheimer; 🇫🇷 Lyon, Lyonnais, France

Centre Medical de La Teppe; 🇫🇷 Tain L'Hermitage, France

Universitaetsklinikum Ulm; 🇩🇪 Ulm, Germany

Tel-Aviv Sourasky Medical Center; 🇮🇱 Tel Aviv, Israel

Orszagos Idegsebeszeti Tudomanyos Intezet; 🇭🇺 Budapest, Hungary

Prywatna Wielospecjalistyczna Lecznica Medyczna "Zycie"; 🇵🇱 Warsaw, Poland

Clinic of Nervous Diseases of Sechenov's Moscow Med. Academy; 🇷🇺 Moscow, Russian Federation

Walton Centre for Neurology & Neurosurgery; 🇬🇧 Liverpool, United Kingdom

Royal London Hospital; 🇬🇧 London, United Kingdom

Hosp. Clinico Univ. Lozano Blesa; 🇪🇸 Zaragoza, Spain

Centre Neurologique William Lennox; 🇧🇪 Ottignies, Belgium

Mid-Atlantic Epilepsy and Sleep Center; 🇺🇸 Bethesda, Maryland, United States

Zentrum Epilepsie Erlangen (ZEE) der Universitaet Erlangen; 🇩🇪 Erlangen, Germany

Wolfson Medical Center; 🇮🇱 Holon, Israel

Western Galilee Hospital; 🇮🇱 Nahariya, Israel

Interregional Clinical Diagnostic Centre; 🇷🇺 Kazan, Russian Federation

Austin & Repatriation Medical Centre; 🇦🇺 West Heidelberg, Victoria, Australia

A. Z. Middelheim -- Department of Neurology; 🇧🇪 Antwerp, Belgium

Hopital Civil de Strasbourg; 🇫🇷 Strasbourg, France

Universitaet Giessen / Marburg Neurologie; 🇩🇪 Marburg, Germany

Assaf Harofeh Medical Center; 🇮🇱 Beer Yaakov, Israel

Kaplan Medical Center; 🇮🇱 Rechovot, Israel

Sunninghill & Kopano Clinical Trials; 🇿🇦 Sunninghill, Gauteng, South Africa

Johannesburg Hospital; 🇿🇦 Johannesburg, Gauten, South Africa

Psychosomatic Center of Dnepropetr. Regional Clinic; 🇺🇦 Dnepropetrovsk, Ukraine

Natl. Inst. of Psychiatry and Neurology; 🇭🇺 Budapest, Hungary

Universitaire Ziekenhuizen Gasthuisberg -- Department Neurology; 🇧🇪 Leuven, Belgium

CHU Pontchaillou; 🇫🇷 Rennes Cedex, France

Georg-August-Universitaet Goettingen; 🇩🇪 Goettingen, Germany

Barzilai Medical Center; 🇮🇱 Ashkelon, Israel

Chaim Sheba Medical Center; 🇮🇱 Ramat Gan, Israel

North Coast Neurology Centre; 🇦🇺 Maroochydore, Queensland, Australia

Monash Medical Centre; 🇦🇺 Clayton, Victoria, Australia

NZOZ Przychodnia Internistyczno - Stomatologiczna "Kendron"; 🇵🇱 Bialystok, Poland

WSS im.Kardynala S. Wyszynskiego; 🇵🇱 Lublin, Poland