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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT01963208
Other study ID # 1042-0603
Secondary ID
Status Completed
Phase Phase 3
First received
Last updated
Start date October 2013
Est. completion date October 2016

Study information

Verified date January 2023
Source Marinus Pharmaceuticals
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The study will evaluate the effectiveness and safety of an investigational drug-ganaxolone - on partial seizure frequency in adults with epilepsy taking a maximum of 3 antiepileptic medications (AEDs).


Description:

This is a 2-cohort study comprised of 2 phases in each cohort. Phase 1 is a double-blind (DB) phase followed by Phase 2, an open-label phase. Cohort 1 will provide tolerability, safety, and PK information for ganaxolone 1200 milligram per day (mg/day), 1800 mg/day and placebo. Cohort 2 will investigate the efficacy, tolerability and safety of ganaxolone 1800 mg/day compared to placebo. Cohort 1 (N= approximately 50) will enroll into a 67-week study comprised of a 4-week prospective baseline period plus 4 week retrospective baseline followed by two treatment phases: a 9-week randomized DB placebo-controlled treatment phase followed by a 52-week open label treatment phase. Cohort 2 (N=150) will enroll into a 72-week study comprised of a 8-week prospective baseline period followed by two treatment phases: a 14-week randomized DB placebo-controlled treatment phase followed by a 52-week open label treatment phase.


Recruitment information / eligibility

Status Completed
Enrollment 405
Est. completion date October 2016
Est. primary completion date May 2016
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: - Able to give informed consent in writing, or have a legally authorized representative able to do so - Willing to enter and participate for the full term of the double blind phase and willing to enter into the open-label phase - Male or female outpatients > 18 years of age - Have a confident diagnosis of drug-resistant epilepsy with partial-onset seizures (POS), with or without secondary generalization, for =2 years. Have residual POS despite having been treated in the past with at least 2 approved anti-epilepsy drugs (AEDs) either alone or in combination - Based on history, participants would be anticipated to have at least 3 POS during each 4-week Baseline period and unlikely to have 21 or more consecutive POS-free days - Currently being treated and maintained with a stable regimen of 1, 2, or 3 AEDs - Able and willing to maintain daily seizure calendar - Able and willing to take drug with food twice daily - Sexually active women of childbearing potential must use acceptable birth control and have a negative pregnancy test at all visits Exclusion Criteria: - Have had previous exposure to ganaxolone - Known sensitivity or allergy to any component in the study drug, progesterone, or other related steroid compounds - Exposure to any investigational drug or device <30 days prior to screening, or plans to take another investigational drug at any time during the study - Time of onset of epilepsy treatment <2 years prior to enrollment - Have generalized epilepsy, such as Lennox-Gastaut syndrome, juvenile myoclonic epilepsy, absence epilepsy, or non-epileptic seizures within the last 12- month period prior to study entry - Have less than 3 POS seizures in a 28-day period or more than 21 consecutive seizure-free days during the Baseline period - Have only simple partial seizures without any observable motor component - Have innumerable seizures or status epilepticus within the last 12-months prior to screening - Have more than 100 POS per 4-week Baseline period - Have seizures secondary to illicit drug or alcohol use, infection, neoplasm, demyelinating disease, degenerative neurological disease, or central nervous system (CNS) disease deemed progressive, metabolic illness, or progressive degenerative disease - Current use of vigabatrin is not permitted. If prior use of vigabatrin, must have documented stable visual fields - Current use of ezogabine is not permitted. If prior use, must have been off the medication for at least 3 months prior to screening and have had documented normal fundoscopic exam by ophthalmologist - Are planning surgery, or to be evaluated for surgery, during the double-blind phase to control seizures including VNS implantation - Are suffering from acute or progressive neurological disease, moderate or severe psychiatric disease, or severe mental abnormalities that are likely to require changes in drug therapy during the double-blind portion of the study or interfere with the objectives of the study or the ability to adhere to the protocol requirements - Have a history of an actual suicide attempt in the last 5 years or more than 1 lifetime suicide attempt - Have a positive urine drug screen at Screening or meet criteria for current or historical Substance Use Disorder (DSM-V criteria) within the past 5 years. - Have any medical condition that, in the investigator's judgment, is considered to be clinically significant and could potentially affect participant safety or study outcome, including but not limited to: clinically significant cardiac, renal, pulmonary, gastrointestinal, hematologic or hepatic conditions; or a condition that affects the absorption, distribution, metabolism or excretion of drugs - Have elevated ALT (SGPT) or AST (SGOT) greater than 3 times upper limits of normal, or total bilirubin greater than 1.5 times ULN - Have a history of malignancy within the past 2 years, with the exception of basal cell carcinoma - Are currently following or planning to follow a ketogenic diet - Use of dietary supplements or herbal preparations are not permitted if participant has been using them consistently for less than 6 months prior to screening, or does not plan on remaining on stable doses for the duration of the double blind phase. Use of St. John's Wort is not permitted - Females who are pregnant, currently breastfeeding or planning to become pregnant during the duration of the study - A history of chronic noncompliance with drug regimens - Inability to withhold grapefruit and grapefruit juice from diet during the entire clinical trial

Study Design


Related Conditions & MeSH terms

  • Drug Resistant Partial Onset Seizure
  • Seizures

Intervention

Drug:
ganaxolone
200 mg and 225 mg capsules; target dose 1800 mg/day dosed 900mg 2x/day
Placebo
placebo

Locations

Country Name City State
Australia Flinders Medical Center Bedford Park South Australia
Australia Royal Prince Alfred Hospital Camperdown New South Wales
Australia St. Vincent's Hospital Fitzroy Victoria
Australia The Florey Institute of Neuroscience and Mental Health Heidelberg Victoria
Australia The Royal Melbourne Hospital Parkville Victoria
Australia The Prince of Wales Hospital Randwick New South Wales
Australia Westmead Hospital Westmead New South Wales
Bulgaria MHAT Blagoevgrad
Bulgaria UMHAT Dr. Georgi Stranski Clinic of Neurology Pleven
Bulgaria Medical Centre-Teodora Ruse
Bulgaria Medical Center Excelsior 4 Sofia
Bulgaria MHAT Lyulin Department of Neurology Sofia
Bulgaria SHATNP Sofia
Bulgaria UMHAT Alexandrovska Clinic of Nerve Diseases Sofia
Bulgaria Medical Center Ekvita Ltd Varna
Germany Epilepsieklinik Bernau
Germany Krankenhaus Mara Epilepsie-Zentrum Bielefeld
Germany Klinik fur Epileptologie Bonn
Germany Neuro-Consil Dussseldorf
Germany Universitatsklinikum GieBen und Marburg Marburg
Germany Universitatsklin Kum Ulm Ulm
Poland Novo-Med Jaworowa
Poland Centrum Medycne Dendryt Katowice
Poland Indywidualna Praktyka ul Narutowicza Lublin
Poland Wojewodzki Szpital Specjalistyczny Oddzial Lublin
Poland Fundacja Epileptologii Wiertnicza Warszawa
Poland Instytut Psychiatrii i Neurologii Warszawa
Russian Federation Kazan State Medical University Kazan
Russian Federation City Neurological Center Novosibirsk
United States University of Colorado- Anschutz Outpatient Pavilion Aurora Colorado
United States Mid-Atlantic Epilepsy Center Bethesda Maryland
United States University of Alabama at Birmingham Birmingham Alabama
United States University of Alabama Epilepsy Center Birmingham Alabama
United States Consultants in Epilepsy & Neurology Boise Idaho
United States Bringham and Women's Hospital Boston Massachusetts
United States Cooper Medical Center of Rowan University Camden New Jersey
United States Ohio Clinical Research Partners, LLC Canton Ohio
United States Five Towns Neuroscience Research Cedarhurst New York
United States The Comprehensive Epilepsy Care Center for Children and Adults Chesterfield Missouri
United States Ohio State University Columbus Ohio
United States Neurology Consultants of Dallas Dallas Texas
United States Texas Epilepsy Group Dallas Texas
United States Neuro-Pain Medical Center, Inc Fresno California
United States Minneapolis Clinic of Neurology Golden Valley Minnesota
United States Northeast Regional Epilepsy Group Hackensack New Jersey
United States Bluegrass Epilepsy Research, LLC Lexington Kentucky
United States Clinical Trials Inc. Little Rock Arkansas
United States Neuroscience Consulants Miami Florida
United States Northeast Regional Epilepsy Group Middletown New York
United States Winthrop University Hospital Mineola New York
United States New York University Comprehensive Epilepsy Center New York New York
United States Northeast Regional Epilepsy Group New York New York
United States Lynn Health Institute Oklahoma City Oklahoma
United States Sooner Clinical Research Oklahoma City Oklahoma
United States Jefferson Comprehensive Epilepsy Center Philadelphia Pennsylvania
United States Temple University School of Medicine Philadelphia Pennsylvania
United States Xenoscience Inc. Phoenix Arizona
United States Medsol Clinical Research Center Port Charlotte Florida
United States Rainier Clinical Research Center, Inc. Renton Washington
United States Neurological Research Institute Santa Monica California
United States The MORE Foundation Sun City Arizona
United States Wake Forest Health Sciences Winston-Salem North Carolina

Sponsors (1)

Lead Sponsor Collaborator
Marinus Pharmaceuticals

Countries where clinical trial is conducted

United States,  Australia,  Bulgaria,  Germany,  Poland,  Russian Federation, 

Outcome

Type Measure Description Time frame Safety issue
Primary Double Blind: Cohort 2: Percent Change From Baseline in 28-day Seizure Frequency During Titration + Maintenance Period Seizure frequency was based on the number of seizures per 28 days, calculated as the number of seizures over the time interval multiplied by 28 and divided by the number of days in the interval. Baseline 28-day seizure frequency was calculated as the number of seizures in the Baseline period (= 56 days) divided by the number of days with available seizure data in the Baseline period and multiplied by 28. Baseline was defined as non-missing value of last assessment before first dose. Primary analysis was performed using a rank analysis of covariance (ANCOVA). Baseline and Week 14
Secondary Double Blind: Cohort 2: Number of Participants With =50% Responder Rate During Titration + Maintenance Period A 50% responder was a participant who experienced at least a 50% decrease in 28-day seizure frequency compared to Baseline. Up to Week 14
Secondary Double Blind: Cohort 2: Change From Baseline in the Number of Seizure Free Days Per 28-day Period During Titration + Maintenance Period Baseline number of seizure free days per 28-day period was calculated as: the number of seizure free days in the entire Baseline period (<=56 days) divided by the number of days with available seizure data in the baseline period and multiplied by 28. Post-Baseline number of seizure free days per 28-day period was calculated as: the number of seizure free days in the entire treatment period divided by the number of days with available seizure data in the treatment period and multiplied by 28. Change from Baseline in number of seizure free days per 28-day period from Baseline was calculated as: Post-Baseline number of seizure free days per 28-day period minus Baseline number of seizure free days per 28-day period. Baseline was defined as non-missing value of last assessment before first dose. Baseline and Week 14
Secondary Double Blind: Cohort 2: Number of Participants With Clinical Global Impression of Change - Improvement (CGI-I) at Week 14 The CGI-I scale is a clinician-rated 7-point Likert scale used to assess the degree to which the participant's epilepsy symptoms have changed relative to Baseline. It was rated as 1. "very much improved"; 2. "much improved"; 3. "minimally improved"; 4. "no change"; 5. "minimally worse"; 6. "much worse"; 7. "very much worse". Higher scores indicated worse condition. Baseline was defined as non-missing value of last assessment before first dose. At Week 14
Secondary Double Blind: Cohort 2: Percent Change From Baseline in 28-day Seizure Frequency During Maintenance Period Seizure frequency was based on the number of seizures per 28 days, calculated as the number of seizures over the time interval multiplied by 28 and divided by the number of days in the interval. Baseline 28-day seizure frequency was calculated as the number of seizures in the Baseline period (= 56 days) divided by the number of days with available seizure data in the Baseline period and multiplied by 28. Baseline was defined as non-missing value of last assessment before first dose. Baseline and Week 2 to Week 14
Secondary Double Blind: Cohort 2: Change From Baseline in 28-day Seizure Frequency During Titration + Maintenance Period Seizure frequency was based on the number of seizures per 28 days, calculated as the number of seizures over the time interval multiplied by 28 and divided by the number of days in the interval. Baseline 28-day seizure frequency was calculated as the number of seizures in the Baseline period (= 56 days) divided by the number of days with available seizure data in the Baseline period and multiplied by 28. Baseline was defined as non-missing value of last assessment before first dose. Change from Baseline was calculated by subtracting Baseline value from the post-dose visit value. Baseline and Week 14
Secondary Double Blind: Cohort 2: Change From Baseline in 28-day Seizure Frequency During Maintenance Period Seizure frequency was based on the number of seizures per 28 days, calculated as the number of seizures over the time interval multiplied by 28 and divided by the number of days in the interval. Baseline 28-day seizure frequency was calculated as the number of seizures in the Baseline period (= 56 days) divided by the number of days with available seizure data in the Baseline period and multiplied by 28. Baseline was defined as non-missing value of last assessment before first dose. Change from Baseline was calculated by subtracting Baseline value from the post-dose visit value. Baseline and Week 2 to Week 14
Secondary Double Blind: Cohort 2: Change From Baseline in the Number of Seizure Free Days Per 28-day Period During Maintenance Period Baseline number of seizure free days per 28-day period was calculated as: the number of seizure free days in the entire Baseline period (= 56 days) divided by the number of days with available seizure data in the Baseline period and multiplied by 28. Post-Baseline number of seizure free days per 28-day period was calculated as: the number of seizure free days in the entire treatment period divided by the number of days with available seizure data in the treatment period and multiplied by 28. Change from Baseline in number of seizure free days per 28-day period from Baseline was calculated as: Post-Baseline number of seizure free days per 28-day period minus Baseline number of seizure free days per 28-day period. Baseline was defined as non-missing value of last assessment before first dose. Baseline and Week 2 to Week 14
Secondary Double Blind: Cohort 2: Percentage of Responders Experiencing a =R% (80%, 60%, 40%, and 20%) Reduction From Baseline to the End of Treatment Period in 28-day Seizure Frequency During Titration + Maintenance Period Percentage of participants who had reductions of = 80%, = 60%, = 40%, and = 20% in 28-day seizure frequency from Baseline is presented. A responder is an individual whose reduction of percent change from Baseline in 28-day seizure frequency was = 50%. Baseline was defined as non-missing value of last assessment before first dose. Up to Week 14
Secondary Double Blind: Cohort 2: Percentage of Responders Experiencing a =R% (80%, 60%, 40%, and 20%) Reduction From Baseline to the End of Treatment Period in 28-day Seizure Frequency During Maintenance Period Percentage of participants who had reductions of = 80%, = 60%, = 40%, and = 20% in 28-day seizure frequency from Baseline is presented. A responder is an individual whose reduction of percent change from Baseline in 28-day seizure frequency was = 50%. Baseline was defined as non-missing value of last assessment before first dose. Week 2 to Week 14
Secondary Double Blind: Cohort 2: Percentage of Seizure Free Participants During the Maintenance Period Percentage of participants who completed the study without any seizures is presented Week 2 to Week 14
Secondary Double Blind: Cohort 2: Percentage of Participants Who Experienced at Least One 28-day Seizure Free Period During Titration + Maintenance Phase Percentage of participants who experienced at least one 28-day seizure free period is presented Up to Week 14
Secondary Double Blind: Cohort 2: Longest Percent of Time Spent Seizure-free During Titration + Maintenance Period The longest period of time seizure-free was defined as the percent of the longest seizure-free period (days) divided by the days with available seizure data, and then multiplied by 100%. Up to Week 14
Secondary Double Blind: Cohort 2: Percent Change From Baseline in 28-day Seizure Frequency for Different Subtypes of Seizures During Titration + Maintenance Period Seizure frequency was based on the number of seizures per 28 days, calculated as the number of seizures over the time interval multiplied by 28 and divided by the number of days in the interval. The analysis was conducted for Partial-Onset Seizure (POS) only which included seizure subtypes: Complex partial seizures (CPS), secondarily generalized tonic-clonic (SGTC) seizures, simple partial seizure with motor/observable component (SPS-Motor) and Simple partial seizure (SPS) without motor/observable component. Baseline 28-day seizure frequency was calculated as the number of seizures in the Baseline period (= 56 days) divided by the number of days with available seizure data in the Baseline period and multiplied by 28. Baseline was defined as non-missing value of last assessment before first dose. Baseline and Week 14
Secondary Double Blind: Cohort 2: Number of Participants With Patient Global Impression of Change - Improvement (PGI-I) at Week 8 and Week 14 The PGI-I scale was a 7-point Likert scale completed by the Patient or Caregiver representing the degree to which the participant's epilepsy symptoms had changed relative to Baseline. It was rated as 1. "very much improved"; 2. "much improved"; 3. "minimally improved"; 4. "no change"; 5. "minimally worse"; 6. "much worse"; 7. "very much worse". Higher score indicated worse condition. Baseline was defined as non-missing value of last assessment before first dose. Week 8 and Week 14
Secondary Double Blind: Cohort 2: Number of Participants With Clinical Global Impression of Change - Improvement (CGI-I) at Week 8 The CGI-I scale is a clinician-rated 7-point Likert scale used to assess the degree to which the participant's epilepsy symptoms have changed relative to Baseline. It was rated as 1. "very much improved"; 2. "much improved"; 3. "minimally improved"; 4. "no change"; 5. "minimally worse"; 6. "much worse"; 7. "very much worse". Higher scores indicated worse condition. Baseline was defined as non-missing value of last assessment before first dose. At Week 8
See also
  Status Clinical Trial Phase
Terminated NCT02519439 - A Two-year Open-label Extension Study of Ganaxolone in Patients With Drug-resistant Partial-onset Seizures Phase 3