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Adjunctive GNX Treatment Compared With Placebo in Children and Adults With TSC-related Epilepsy

Sponsor
Marinus Pharmaceuticals (Industry)
Overall Status
Recruiting
CT.gov ID
NCT05323734
Collaborator
(none)
162
Enrollment
29
Locations
2
Arms
34.1
Anticipated Duration (Months)
5.6
Patients Per Site
0.2
Patients Per Site Per Month

Study Details

Study Description

Brief Summary

This is a Phase 3, global, double-blind, randomized, placebo-controlled study of adjunctive GNX treatment in children and adults with TSC-related epilepsy. The study consists of a 4-week prospective baseline phase, defined as the first 28 days following screening, followed by a double-blind phase consisting of a 4-week titration period (with 2 additional weeks allowed, if necessary, for tolerance) and a 12-week maintenance period.

Condition or Disease Intervention/Treatment Phase
  • Drug: GNX oral suspension, TID
  • Drug: Placebo
 Phase 3

Study Design

Study Type:
Interventional
Anticipated Enrollment :
162 participants
Allocation:
Randomized
Intervention Model:
Parallel Assignment
Masking:
Triple (Participant, Care Provider, Investigator)
Primary Purpose:
Treatment
Official Title:
A Phase 3, Double-blind, Randomized, Placebo-controlled Trial of Adjunctive Ganaxolone (GNX) Treatment in Children and Adults With Tuberous Sclerosis Complex (TSC)-Related Epilepsy
Actual Study Start Date :
Apr 1, 2022
Anticipated Primary Completion Date :
Jan 1, 2024
Anticipated Study Completion Date :
Feb 1, 2025

Arms and Interventions

Arm Intervention/Treatment
Experimental: GNX

GNX oral suspension, TID

Drug: GNX oral suspension, TID
Ganaxalone
Other Names:
  • Active Drug

    		•
    Placebo Comparator: Placebo

    Placebo oral suspension, TID

    Drug: Placebo
    Placebo (for Ganaxolone)
    Other Names:
  • Inactive

    		•

    Outcome Measures

    Primary Outcome Measures

    1. Seizure Frequency During 28-day double-blind phase [Day 1 through Week 16]

      percentage change from baseline in 28-day seizure frequency during the double-blind phase

    Secondary Outcome Measures

    1. Seizure Frequency During Maintenance [12 weeks - Post Titration Phase]

      Percentage change from baseline in 28-day seizure frequency during the maintenance period

    2. Number (%) of participants considered treatment responders during the double-blind phase [16 weeks - Titration through Maintenance]

      Number (%) of participants considered treatment responders during the double-blind phase. Treatment responders are defined as those participants with ≥ 50% reduction from baseline in primary endpoint seizure frequency during given period

    3. Number (%) of participants considered treatment responders during the maintenance phase. [12 weeks - Post Titration Phase]

      Number (%) of participants considered treatment responders during the maintenance phase. Treatment responders are defined as those participants with ≥ 50% reduction from baseline in primary endpoint seizure frequency during a given period.

    4. Clinical Global Impression [16 weeks - Titration through Maintenance]

      CGI-I at the last scheduled visit in the double-blind phase.

    5. Anxiety, Depression, and Mood Scale [16 weeks - Titration through Maintenance]

      Change from baseline in ADAMS total score and sub-score: Scale: 0 equates to behavior has not occurred, or is not a problem equates to behavior occurs occasionally, or is a mild problem equates to behavior occurs quite often, or is a moderate problem equates to behavior occurs a lot, or is a severe problem

    6. Short Form - 36 [16 weeks - Titration through Maintenance]

      Change from baseline in quality-of-life scale - SF-36

    7. Pediatric Quality of Life Inventory - Family Impact Module [16 weeks - Titration through Maintenance]

      Change from baseline in quality-of-life scale - Peds-QL-FIM

    8. Epilepsy and Learning Disabilities Quality of Life Scale [16 weeks - Titration through Maintenance]

      Change from baseline in quality-of-life scale - ELDQOL Note: Scale to be provided as part of necessary documentation

    9. Seizure Control [16 weeks - Titration through Maintenance]

      Change from baseline in the percentage of seizure-free days during the double-blind phase, based on primary endpoint seizure type.

    10. Clinical Global Impression of Change in Seizure Intensity and Duration [16 weeks - Titration through Maintenance]

      Change from baseline in the CGI-CSID at the end of the double-blind phase.

    11. Seizure Frequency Change - Double Blind [16 weeks - Titration through Maintenance]

      Participants with a ≥ 25% and ≥ 75% reduction from baseline in primary endpoint seizure frequency during the double-blind phase.

    12. Seizure Frequency Change - Maintenance [12 weeks - Post Titration Phase]

      Participants with a ≥ 25%, ≥ 50%, and ≥ 75% reduction from baseline in primary endpoint seizure frequency during the maintenance period.

    13. Responder Analysis [16 weeks - Titration through Maintenance]

      Responder analysis for primary endpoint seizures and all seizures during the double-blind phase using the following response categories: ≤ 0%, > 0% to < 25%, ≥ 25% to < 50%, ≥ 50% to < 75%, and ≥ 75% to 100%.

    14. Seizure Frequency - All Seizures [16 weeks - Titration through Maintenance]

      Percent change in 28-day frequency of all seizures.

    15. Seizure-Free Days [16 weeks - Titration through Maintenance]

      Change from baseline in the percentage of seizure-free days, based on all seizure types.

    16. Seizure-Free Interval [16 weeks - Titration through Maintenance]

      Change from baseline in the longest seizure-free interval, based on primary endpoint seizure type and all seizure types

    Eligibility Criteria

    Criteria

    Ages Eligible for Study:
    1 Year to 65 Years
    Sexes Eligible for Study:
    All
    Accepts Healthy Volunteers:
    No
    Inclusion Criteria:

    1. Clinical or mutational diagnosis of TSC consistent with (Northrup and Krueger, 2013):

    2. Molecular confirmation of a pathogenic mutation in TSC1 or TSC2. A pathogenic mutation is defined as a mutation that clearly prevents protein synthesis and/or inactivates the function of the TSC1 or TSC2 proteins (eg, nonsense mutation or frameshift mutations, large genomic deletions) or is a missense mutation whose effect on protein function has been established by functional assessment. The PI or designee must review the results of the genetic analysis and confirm that the causal relationship to the epilepsy syndrome is likely. OR

    3. Clinical diagnosis of definite TSC which includes 2 major features or 1 major feature with ≥ 2 minor features.

    4. Male or female participants aged 1 through 65 years, inclusive.

    5. Participant/parent or LAR willing to give written informed consent/assent, after being properly informed of the nature and risks of the study and prior to engaging in any study related procedures.

    6. Assent for participants over 7 years of age should be obtained if appropriate.

    7. Failure to control seizures despite appropriate trial of 2 or more AEDs at therapeutic doses and for adequate duration of treatment per PI judgment.

    8. Participants should be on a stable regimen of AEDs (including moderate or strong inducer or inhibitor anti-seizure medications eg, carbamazepine, phenytoin, etc.) at therapeutic doses for ≥ 28 days prior to the screening visit, and without a foreseeable change in dosing for the duration of the study. (Note: Minor dose adjustment to address tolerability and safety events may be allowed on case-by-case basis and it should be discussed with the study medical monitor.)

    9. A history of at least 8 countable seizures per month in the 2 months prior to screening with no more than 1 seizure free week in each month.

    10. Have an average of at least 2 primary endpoint seizures per week in the 28 days following the screening visit.

    The primary endpoint seizure types are defined as the following:

    1. focal motor seizures without impairment of consciousness or awareness

    2. focal seizures with impairment of consciousness or awareness with motor features

    3. focal seizures evolving to bilateral, tonic-clonic seizures

    4. generalized motor seizures including tonic-clonic, bilateral tonic, bilateral clonic, or atonic/drop seizures.

    Seizures that do not count towards the primary endpoint include:

    1. Focal aware seizures without motor features

    2. Focal and generalized nonmotor seizures (eg, absence or focal nonmotor seizures with or without impairment of awareness)

    3. Infantile or epileptic spasms

    4. Myoclonic seizures.

    5. Participants with surgically implanted VNS will be allowed to enter the study provided that all of the following conditions are met:

    6. The VNS has been in place for ≥ 1 year prior to the screening visit.

    7. The settings must have remained constant for 3 months prior to the screening visit and are expected to remain constant throughout the study.

    8. The battery is expected to last for the duration of the study.

    9. Parent/caregiver or the participant, as appropriate, is able and willing to maintain an accurate and complete daily seizure eDiary for the duration of the study.

    10. Able and willing to take IP (suspension) as directed with food TID.

    11. Sexually active WOCBP must be using a medically acceptable method of birth control and have a negative quantitative serum β-HCG test collected at the initial screening visit.

    Childbearing potential is defined as a female who is biologically capable of becoming pregnant. A medically acceptable method of birth control includes intrauterine devices in place for 1 month prior to the screening visit, surgical sterilization, or adequate double barrier methods (eg, diaphragm or condom and foam). An oral contraceptive alone is not considered adequate for the purpose of this study. Use of oral contraceptives in combination with another method (eg, a spermicidal cream) is acceptable. In participants who are not sexually active, abstinence is an acceptable method of birth control.

    1. Male participants must agree to take all necessary measures to avoid causing pregnancy in their sexual partners during the study and for 30 days after the last dose of IP. Medically acceptable contraceptives include surgical sterilization (such as a vasectomy) and a condom used with a spermicidal gel or foam.
    Exclusion Criteria:

    1. Previous exposure to GNX.

    2. Pregnant or breastfeeding.

    3. Participants who have been taking felbamate for less than 1 year prior to screening.

    4. Participants taking CBD preparations other than Epidiolex.

    5. A positive result on plasma drug screen for CBD or THC at Visit 1 (screening), with the exception of results that are fully explained by Epidiolex, which is being prescribed and managed by the investigator.

    6. Concurrent use of ACTH, prednisone or other glucocorticoid is not permitted, nor use of the strong inducers of CYP3A4, rifampin and St John's Wort. Participants on ACTH, prednisone, or other systemically (non-inhaled or topical) administered steroids should be off the product > 28 days prior to screening. Rifampin and St John's Wort must be discontinued at least 28 days before Visit 2, study drug initiation.

    Note:

    1. Use of concomitant intranasal or PRN topical steroids for dermatologic reactions and allergic rhinitis are allowed during the study.

    2. This exclusion criterion does not prohibit the use of approved AEDs

    3. Changes in any chronic medications within the 4 weeks prior to the screening visit. All chronic concomitant medications must be relatively stable in dose for at least 4 weeks prior to the screening visit unless otherwise noted. Small dose adjustment to manage tolerability and safety events is permitted and should be discussed with the study medical monitor.

    4. Participants who have epilepsy surgery planned during the study or who have undergone surgery for epilepsy within the 6 months prior to screening.

    5. An active CNS infection, demyelinating disease, degenerative neurological disease, or CNS disease deemed progressive as evaluated by brain imaging (MRI). This includes tumor growth which in the opinion of the investigator could affect primary endpoint seizure control.

    6. Any disease or condition (medical or surgical; other than TSC) at the screening visit that might compromise the hematologic, cardiovascular (including any cardiac conduction defect), pulmonary, renal, gastrointestinal, or hepatic systems; or other conditions that might interfere with the absorption, distribution, metabolism, or excretion of the IP, or would place the participant at increased risk or interfere with the assessment of safety/efficacy. This may include any illness in the past 4 weeks which in the opinion of the investigator may affect seizure frequency.

    7. An AST/SGOT or ALT/SGPT > 3 × the ULN at screening or baseline visits and confirmed by a repeat test.

    8. Biliary impairment sufficient to affect patient safety, or total bilirubin levels > 1.5 × ULN at screening or baseline visit and confirmed by a repeat test. In cases of Gilbert's Syndrome, resulting in stable levels of total bilirubin greater than ULN, the medical monitor can determine if a protocol exception can be made

    9. Renal impairment sufficient to affect patient safety, or eGFR < 30 mL/min (calculated using the Cockcroft-Gault formula or Pediatric GFR calculator or Bedside Schwartz), will be excluded from study entry or will be discontinued if the criterion is met post baseline (Levey et al, 2006). Cases of temporary renal insufficiency should be discussed with the medical monitor to determine the participant's study continuation

    10. Exposed to any other investigational drug or investigational device within 30 days or fewer than 5 half-lives prior to the screening visit. For therapies in which half-life cannot be readily established, the Sponsor's Medical Monitor should be consulted.

    11. Unwillingness to avoid excessive alcohol use throughout the study.

    12. Have active suicidal plan/intent, active suicidal thoughts or a suicide attempt in the past 6 months.

    13. Known sensitivity or allergy to any component in the IP(s), progesterone, or other related steroid compounds.

    Contacts and Locations

    Locations

    Site City State Country Postal Code
    1 Phoenix Children's Hospital Phoenix Arizona United States 85106
    2 Arkansas Children's Hospital Little Rock Arkansas United States 72202
    3 UCLA Mattel Children's Hospital Los Angeles Tuberous Sclerosis Clinic Los Angeles California United States 90095
    4 University of Colorado Denver Aurora Colorado United States 80045
    5 Yale University School of Medicine New Haven Connecticut United States 06510
    6 Nemours Children's Hospital of Delaware (TSC Clinic at Nemours/duPont Hospital for Children) Wilmington Delaware United States 19803
    7 NW FL Clinical Research Group, LLC Gulf Breeze Florida United States 32561
    8 Nicklaus Children's Hospital Miami Florida United States 33155
    9 Arnold Palmer Hospital Orlando Florida United States 32806
    10 Comprehensive Neurology Clinic Orlando Florida United States 32825
    11 Ann & Robert H. Lurie Children's Hospital of Chicago Chicago Illinois United States 60611
    12 Mid Atlantic Epilepsy & Sleep Center Bethesda Maryland United States 20817
    13 Boston Children's Hospital, Harvard Medical School Boston Massachusetts United States 02115
    14 TSC Clinic at Children's Hospital of Michigan Detroit Michigan United States 48201
    15 Mayo Clinic Rochester Minnesota United States 55905
    16 University of Missouri Child Health Columbia Missouri United States 65201
    17 TSC Clinic at Children's Mercy Hosptial Kansas City Missouri United States 64108
    18 Northeast Regional Epilepsy Group Hackensack New Jersey United States 07601
    19 NYU Comprehensive Epilepsy Center New York New York United States 10016
    20 University of North Carolina at Chapel Hill Chapel Hill North Carolina United States 27599
    21 Atrium Healthcare TSC Clinic at Levine Children's Hospital Charlotte North Carolina United States 28025
    22 Duke University Medical Center Durham North Carolina United States 27710
    23 Cincinnati Children's Hospital Medical Center Cincinnati Ohio United States 45229
    24 Medical Univ. of SC (MUSC) Charleston South Carolina United States 29425
    25 Le Bonheur Children's Hospital Memphis Tennessee United States 38103
    26 Child Neurology Consultants of Austin (CNCA) Austin Texas United States 78749
    27 U of TX Health Sciences Center Houston Texas United States 77030
    28 University of Utah Health Care-Pediatric Neurology Salt Lake City Utah United States 84113
    29 Seattle Children's Hospital, Research and Foundation Seattle Washington United States 98105

    Sponsors and Collaborators

    • Marinus Pharmaceuticals

    Investigators

    None specified.

    Study Documents (Full-Text)

    None provided.

    More Information

    Publications

    None provided.
    Responsible Party:
    Marinus Pharmaceuticals
    ClinicalTrials.gov Identifier:
    NCT05323734
    Other Study ID Numbers:
    • 1042-TSC-3001
    First Posted:
    Apr 12, 2022
    Last Update Posted:
    Aug 19, 2022
    Last Verified:
    Jul 1, 2022
    Studies a U.S. FDA-regulated Drug Product:
    Yes
    Studies a U.S. FDA-regulated Device Product:
    No
    Additional relevant MeSH terms:
    Tuberous Sclerosis
    Epilepsy
    Sclerosis

    Study Results

    No Results Posted as of Aug 19, 2022