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Clinical Trial Details — Status: Active, not recruiting

Administrative data

NCT number NCT05323734
Other study ID # 1042-TSC-3001
Secondary ID
Status Active, not recruiting
Phase Phase 3
First received
Last updated
Start date April 1, 2022
Est. completion date October 31, 2024

Study information

Verified date May 2024
Source Marinus Pharmaceuticals
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial 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 (Day 1 to Day 28) and a 12-week maintenance period (Day 29 to Week 16).


Recruitment information / eligibility

Status Active, not recruiting
Enrollment 128
Est. completion date October 31, 2024
Est. primary completion date October 31, 2024
Accepts healthy volunteers No
Gender All
Age group 1 Year to 65 Years
Eligibility Inclusion Criteria: 1. Clinical or mutational diagnosis of TSC consistent with: 1. 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 Principal investigator (PI) or designee must review the results of the genetic analysis and confirm that the causal relationship to the epilepsy syndrome is likely. OR 2. Clinical diagnosis of definite TSC which includes 2 major features or 1 major feature with = 2 minor features. 2. Male or female participants aged 1 through 65 years, inclusive. For Europe (EU), Middle East and North Africa (MENA), and Oceania (OC) Male or Female participants aged 2 through 65 years, inclusive. 3. Participant/parent(s) or LAR(s) 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. If the participant is not qualified nor able to provide written informed consent based on age, developmental stage, intellectual capacity, or other factors, parent(s)/LAR(s) must provide consent for study participation, if appropriate. 4. Failure to control seizures despite appropriate trial of 2 or more Anti-seizure medication (ASMs) at therapeutic doses and for adequate duration of treatment per PI judgment. 5. Participants should be on a stable regimen of ASMs (including moderate or strong inducer or inhibitor ASM 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.) 6. 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. This includes seizures of any kind. 7. Have at least 8 primary endpoint seizures in the first 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 or generalized nonmotor seizures (eg, absence seizures or focal nonmotor seizures with or without impairment of awareness) 2. Infantile or epileptic spasms 3. Myoclonic seizures. 8. Participants with surgically implanted vagal nerve stimulator (VNS) will be allowed to enter the study provided that all of the following conditions are met: 1. The VNS has been in place for = 6 months prior to the screening visit. 2. The settings must have remained constant for 3 months prior to the screening visit and are expected to remain constant throughout the study. 3. The battery is expected to last for the duration of the study. 9. Parent(s)/caregiver(s)/LAR(s) or the participant, as appropriate, is (are) willing and able to maintain an accurate and complete daily seizure eDiary for the duration of the study. 10. Willing and able to take IP (suspension) as directed with food (TID). 11. Women of childbearing potential (WOCBP) must be using a medically acceptable method of birth control and have a negative quantitative serum beta-human chorionic growth hormone (ß-HCG) test collected at the initial screening and Baseline visits.Childbearing potential is defined as a female who is biologically capable of becoming pregnant. A medically acceptable method of birth control includes intrauterine devices (that have been in place for at least 1 month prior to the screening visit), hormonal contraceptives (eg, combined oral contraceptives, patch, vaginal ring, injectables, and implants), and surgical sterilization (such as oophorectomy or tubal ligation. When used consistently and correctly, "double-barrier" methods of contraception can be used as an effective alternative to highly effective contraception methods. Contraceptive measures such as Plan B™, sold for emergency use after unprotected sex, are not acceptable methods for routine use. 12. Male participants must agree to use highly effective contraceptive methods during the study and for 30 days after the last dose of IP. Highly effective methods of contraception include surgical sterilization (such as a vasectomy) and adequate "double-barrier" methods. 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 cannabidiol (CBD) preparations other than Epidiolex. 5. A positive result on plasma drug screen for CBD or tetrahydrocannabinol (THC) at Visit 1 (screening), with the exception of results that are fully explained by Epidiolex, which can be adjusted by the investigator in the event of any Adverse events (AEs). 6. Concurrent use of adrenocorticotropic hormone (ACTH), prednisone or other glucocorticoid is not permitted, nor use of the strong inducers of cytochrome P450 3A4 (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 pro re nata (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 ASMs. 7. 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. 8. Participants who have epilepsy surgery planned during the study or who have undergone surgery for epilepsy within the 6 months prior to screening. 9. An active central nervous system (CNS) infection, demyelinating disease, degenerative neurological disease, or CNS disease deemed progressive as evaluated by brain magnetic resonance imaging (MRI). This includes tumor growth which in the opinion of the investigator could affect primary endpoint seizure control. 10. 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. 11. Hepatic impairment sufficient to affect participant safety, or an aspartate aminotransferase (AST)/ serum glutamic oxaloacetic transaminase (SGOT) or alanine aminotransferase (ALT)/ serum glutamic pyruvic transaminase (SGPT) > 3 × the upper limit of normal (ULN) at screening or Baseline visits and confirmed by a repeat test. 12. Biliary impairment sufficient to affect participant 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 13. Renal impairment sufficient to affect participant safety, or estimated glomerular filtration rate (eGFR) < 30 milliliter per minute (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. Cases of temporary renal insufficiency should be discussed with the medical monitor to determine the participant's study continuation. 14. 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. 15. Unwillingness to avoid excessive alcohol use throughout the study. 16. Have active suicidal plan/intent, active suicidal thoughts or a suicide attempt in the past 6 months. 17. Known sensitivity or allergy to any component in the IP(s), progesterone, or other related steroid compounds. 18. Participants deprived of their liberty by a judicial or administrative decision, or for psychiatric treatment, or participants admitted to a health or social services facility for purposes other than research. 19. Participants receiving traditional Chinese medicine therapies within the prior 28 days of the screening.

Study Design


Intervention

Drug:
Ganaxalone
GNX will be administered
Placebo
Placebo will be administered

Locations

Country Name City State
Canada Hôtel Dieu de Montréal - CHUM Montreal
Canada CHU Sainte-Justine Montréal
Canada The Hospital for Sick Children Toronto
Canada Toronto Western Hospital Toronto
Canada BC Children's Hospital Vancouver
France University Hospital of Lyon Bron
France University Hospital of Lille Lille
France Robert-Debré Hospital Paris
France University Hospital of Rennes Rennes
France University of Strasbourg Strasbourg
Germany Epilepsie-Zentrum Bethel - Krankenhaus Mara Bielefeld
Germany University Hospital Bonn Bonn
Germany ZNN - Epilepsiezentrum Frankfurt am Main Frankfurt
Germany Universitäts Krankenhaus Freiburg Freiburg
Germany Gemeinschaftskrankenhaus Herdecke Herdecke
Germany Epilepsiezentrum Kleinwachau gGmbH Radeberg
Israel Soroka University Medical Center Beer-Sheva
Israel Hadassah Medical Center Jerusalem
Israel Schneider Children´s Medical Center Petah Tikva
Israel Sheba Medical Center Tel Hashomer
Israel Tel-Aviv Sourasky Medical Center Tel-Aviv
Italy Azienda Ospedaliero-Universitaria Meyer Firenze
Italy Pediatric Neurology and Muscular Diseases Unit - University of Genoa Genova
Italy Children's Hospital Bambino Gesù Rome
Italy Policlinico Umberto I Rome
Spain Hospital de la Santa Creu i Sant Pau Barcelona
Spain Hospital Sant Joan de Déu Barcelona
Spain Hospital Universitari Vall d'Hebron Barcelona
Spain Hospital Infantil Universitario Niño Jesús Madrid
Spain Hospital Ruber International Madrid
Spain Hospital Regional Universitario de Málaga Málaga
Spain Hospital Universitario y Politécnico La Fe Valencia
United Kingdom Royal Aberdeen Children's Hospital, NHS Grampian Aberdeen
United Kingdom Bristol Royal Hospital for Children Bristol
United Kingdom Leeds General Infirmary Leeds
United Kingdom NHS acute tertiary referral centre, John Radcliffe Hospital Oxford
United Kingdom Salford Royal Hospital Salford
United Kingdom Sheffield Children's Hospital Sheffield
United States Children's Healthcare of Atlanta Atlanta Georgia
United States Childrens Hospital Colorado Aurora Colorado
United States Child Neurology Consultants of Austin (CNCA) Austin Texas
United States Mid-Atlantic Epilepsy and Sleep Center Bethesda Maryland
United States Boston Children's Hospital, Harvard Medical School Boston Massachusetts
United States University of North Carolina at Chapel Hill Chapel Hill North Carolina
United States Medical University of South Carolina Charleston South Carolina
United States Atrium Health/Levine Children's Hospital Charlotte North Carolina
United States Ann & Robert H. Lurie Children's Hospital of Chicago Chicago Illinois
United States Cincinnati Children's Hospital Medical Center Cincinnati Ohio
United States University of Texas Southwestern Medical Center Dallas Texas
United States Children's Hospital of Michigan Central Michigan University Detroit Michigan
United States Duke University Medical Center Durham North Carolina
United States University of Florida Gainesville Gainesville Florida
United States NW FL Clinical Research Group, LLC Gulf Breeze Florida
United States TSC Clinic at Northeast Regional Epilepsy Group Hackensack New Jersey
United States Penn State Children's Hospital Hershey Pennsylvania
United States McGovern Medical School at the University of Texas Health Science Center Houston Texas
United States Children's Mercy Hosptial Kansas City Missouri
United States Arkansas Children's Research Institute Little Rock Arkansas
United States Institute of Neurology and Neurosurgery at Saint Barnabas Livingston New Jersey
United States UCLA Mattel Children's Hospital, TSC Center Los Angeles California
United States Le Bonheur Children's Hospital Memphis Tennessee
United States Nicklaus Children's Hospital Miami Florida
United States Children's Hospital of Orange County Orange California
United States Comprehensive Neurology Clinic Orlando Florida
United States Orlando Health Orlando Florida
United States Children's Hospital of Philadelphia Philadelphia Pennsylvania
United States Barrow Neurological Institute at Phoenix Children's Hospital Phoenix Arizona
United States Mayo Clinic - Rochester Rochester Minnesota
United States University of Rochester Medical Center Rochester New York
United States University of Utah Health Care-Pediatric Neurology Salt Lake City Utah
United States Seattle Children's Hospital Seattle Washington
United States Nemours Children's Hospital - Delaware Valley Wilmington Delaware

Sponsors (1)

Lead Sponsor Collaborator
Marinus Pharmaceuticals

Countries where clinical trial is conducted

United States,  Canada,  France,  Germany,  Israel,  Italy,  Spain,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Double-blind phase: Percent change from Baseline in 28-day seizure frequency during titration and maintenance period Seizure frequency will be calculated as the total number of seizures divided by the number of days with seizure data, multiplied by 28. Baseline (Day 1) through Week 16
Secondary Double-blind phase: Percent change from Baseline in 28-day seizure frequency during maintenance period Baseline (Day 1) and Day 29 to Week 16
Secondary Double-blind phase: Number of participants who will be considered as treatment responders during titration and maintenance phase Treatment responders are defined as those participants with = 50% reduction from Baseline in seizure frequency Up to 16 weeks
Secondary Double-blind phase: Number of participants who will be considered as treatment responders during maintenance phase Day 29 to Week 16
Secondary Double-blind phase: Number of Participants with Clinical Global Impression of Improvement (CGI-I) during titration and maintenance phase The CGI-I is a 7-point Likert scale that the parent(s)/caregiver(s)/legally authorized representative (LAR)(s) and clinician uses to rate the change in overall seizure control, behavior, safety, and tolerability after initiation of the Investigational product (IP) relative to Baseline (prior to treatment with the IP). It was rated as: 1- "very much improved", 2- "much improved', 3- "minimally improved", 4- "no change", 5- "minimally worse", 6- "much worse", and 7- "very much worse". Higher scores indicated worse condition. Up to 16 weeks
Secondary Double-blind phase: Change from Baseline in Anxiety, Depression, and Mood Scale (ADAMS) during titration and maintenance phase The ADAMS is a rating scale designed to screen for anxiety and depression in individuals with intellectual disability. The 28-question scale is filled out by the parent(s)/caregiver(s)/LAR(s) and is based on the participant's behavior. Each question will be rated on 4-point Likert scale as follows: 0- "behavior has not occurred or is not a problem"; 1- "behavior occurs occasionally or is a mild problem"; 2- "behavior occurs quite often or is a moderate problem"; and 3- "behavior occurs a lot or is a severe problem". Higher scores indicated worse condition. Baseline (Day 1) through Week 16
Secondary Double-blind phase: Change from Baseline in Short Form-36 (SF-36) during titration and maintenance phase The SF-36 is a multi-purpose survey designed to capture participant or parent(s)/caregiver(s)/LAR(s) perceptions of own health and well-being. The SF-36 has 36 items grouped in 8 dimensions: physical functioning, physical and emotional limitations, social functioning, bodily pain, general, and mental health, which are the weighted sums of the questions in each section. Each scale is directly transformed into a 0-100 scale on the assumption that each question carries equal weight. Higher scores represent better health-related quality-of-life. Baseline (Day 1) through 16 weeks
Secondary Double-blind phase: Change from Baseline in Pediatric Quality of Life Inventory - Family Impact Module (Peds-QL-FIM) during titration and maintenance phase Peds-QL-FIM is designed to measure the impact of pediatric chronic health conditions on parents and the family. It composes of 6 scales measuring parent self-reported functioning: 1) Physical functioning (6 items), 2) Emotional functioning (5 items), 3) Social functioning (4 items), 4) Cognitive functioning (5 items), 5) Communication (3 items), 6) Worry (5 items), and in addition two scales measuring parent-reported family functioning: 7) Daily activities (3 items) and 8) Family relationships (5 items). Each of the items have five Likert response options: 0 = never a problem, 1 = almost never, 2 = sometimes, 3 = often, 4= almost always. Items are reverse-scored and linearly transformed to a 0-100 scale (0 = 100, 1 = 75, 2 = 50, 3 = 25, 4 = 0); higher scores indicate better functioning (less negative impact). Baseline (Day 1) through 16 weeks
Secondary Double-blind phase: Change from Baseline in Epilepsy and Learning Disabilities Quality of Life (ELDQOL) Scale during titration and maintenance phase The ELDQOL is a parent/caregiver/LAR-reported measure that examines seizure severity, seizure related injury, anti-seizure medication (ASM) side effects, behavior, mood, physical status, cognitive and social functioning, communication, overall health and quality of life, and family concerns. There are a total of 70 items, some of which are responded as 1=yes/2=no, some of which range 1-4 and others 1-5. For those items, higher is more severe. For mood-related items, however, the scoring is always/often/sometimes/never which are coded as 1-4 but may be good or bad, depending on the mood. Finally: there are qualitative questions with open-ended answers related to "were any questions difficult to answer" and "are there any other comments you would like to make". Each of the 70 items is characterized as its own measurement, and they are not aggregated or tabulated into an overall score. Baseline (Day 1) through 16 weeks
Secondary Double-blind phase: Change from Baseline in the percentage of seizure-free day during titration and maintenance phase Baseline (Day 1) through 16 weeks
Secondary Double-blind phase: Change from Baseline in Caregiver Global Impression of Change in Seizure Intensity/Duration (CGI-CSID) during titration and maintenance phase The CGI-CSID is a 7-point Likert scale in which the parent(s)/caregiver(s)/LAR(s) assesses change in seizure intensity and/or duration after initiation of investigational product relative to Baseline (prior to treatment with investigational product). The scale ranges from 1- very much improved, 2- much improved, 3- minimally improved, 4- no change, 5- minimally worse, 6- much worse, and 7- very much worse. Higher scores indicate worse condition Baseline (Day 1) through 16 weeks
Secondary Double-blind phase: Number of participants with a = 25% and = 75% reduction from Baseline during titration and maintenance phase Up to 16 weeks
Secondary Double-blind phase: Number of participants with a = 25%, = 50%, and = 75% reduction from Baseline during maintenance phase Day 29 to Week 16
Secondary Double-blind phase: Number of participants with Responder Analysis using = 0%, > 0% to < 25%, = 25% to < 50%, = 50% to < 75%, and = 75% to 100% during titration and maintenance phase Up to 16 weeks
Secondary Double-blind phase: Percent change in 28-day frequency of all seizures during titration and maintenance phase Up to 16 weeks
Secondary Double-blind phase: Change from Baseline in percentage of Seizure-Free Days during titration and maintenance phase Baseline (Day 1) and through 16 weeks
Secondary Double-blind phase: Change from Baseline in longest Seizure-Free Interval during titration and maintenance phase Baseline (Day 1) through 16 weeks
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