Phase III Study of Edasalonexent in Boys With Duchenne Muscular Dystrophy
- Registration Number
- NCT03703882
- Lead Sponsor
- Catabasis Pharmaceuticals
- Brief Summary
The PolarisDMD study is a Phase 3, global study to evaluate the efficacy and safety of edasalonexent in pediatric patients with a genetically confirmed diagnosis of DMD. Male patients from 4-7 years of age (up to 8th birthday) will be enrolled.
Edasalonexent is an orally administered small molecule that inhibits NF-kB, which is the key link between loss of dystrophin and disease pathology and plays a fundamental role in the initiation and progression of skeletal and cardiac muscle disease in DMD.
- Detailed Description
The study includes a 52-week, randomized, double-blind, placebo-controlled period, followed by a 2-week follow- up. Approximately 125 boys with DMD will be enrolled in this trial, with 2 boys receiving edasalonexent for every 1 boy receiving placebo.
Following completion of the treatment period, patients may elect to continue in a separate open-label extension study.
Recruitment & Eligibility
- Status
- COMPLETED
- Sex
- Male
- Target Recruitment
- 131
- Written consent/assent by patient and/or legal guardian as per regional and/or Institutional Review Board (IRB)/Independent Ethics Committee (IEC) requirements
- Diagnosis of DMD based on a clinical phenotype with increased serum creatine kinase (CK) and documentation of mutation(s) in the dystrophin gene known to be associated with a DMD phenotype
- Able to perform stand from supine without assistance in โค 10 seconds
- Able to perform the 10MWT and 4-stair climb
- Followed by a doctor or medical professional who coordinates Duchenne care on a regular basis and willingness to disclose patient's study participation with medical professionals
- Use of corticosteroids within 24 weeks prior to Day 1; use of inhaled, intranasal, and topical corticosteroids is permitted
- Use of another investigational drug, idebenone, or dystrophin-focused therapy within 4 weeks. Exception: Patients who have received at least 24 weeks of a stable dose of eteplirsen prior to Day 1, and expected to continue treatment, will be eligible
- Use of the following within 4 weeks prior to Day 1: immunosuppressive therapy, warfarin, phenytoin, S mephenytoin, cyclosporine, dihydroergotamine, ergotamine, fentanyl, alfentanil, pimozide, quinidine, sirolimus, tacrolimus, or paclitaxel
- Use of human growth hormone within 3 months prior to Day 1
- Other prior or ongoing significant medical conditions
Study & Design
- Study Type
- INTERVENTIONAL
- Study Design
- PARALLEL
- Arm && Interventions
Group Intervention Description Placebo Placebo Matching placebo Dose 1 Edasalonexent Edasalonexent 100 mg/kg/day. Capsules taken by mouth three times per day.
- Primary Outcome Measures
Name Time Method Change From Baseline in North Star Ambulatory Assessment (NSAA) Baseline (Day 1) to Week 52 To assess change from baseline in North Star Ambulatory Assessment(NSAA) Total Score at Wk52. NSAA is clinician-reported outcome instrument designed to measure ambulatory function in males with Duchenne muscular dystrophy(DMD). Patients asked to perform 17 different functional activities,including 10MWT,rising from sit to stand,standing on one leg,climbing \& descending a step,stand from supine, lifting the head, standing on heels, \& jumping. Each function activity will be scored as0=(unable to achieve independently),scored as1=(modified method but achieves goal independent of physical assistance from another),or scored as2=(no obvious modification of activity)or "Not Scored". If NSAA test was performed \& any of the individual items are scored as "not scored"(i.e, for reasons unrelated to patients physical capabilities), corresponding total score will be set to missing. Sum of 17 scores will be used to form an ordinal total score(range 0-34).Higher scores imply better functional status
- Secondary Outcome Measures
Name Time Method Change From Baseline in 10-meter Walk/Run Test Baseline (Day 1) to Week 52 To assess the changes from baseline to Week 52 on the 10-meter walk/run test (10MWT). For timed function tests (TFTs), the time will be set to 12 seconds and the speed to 0 if the TFT assessment meets the following TFT grading criteria. Grade of 1 or 2 (from a 6-point scale). 1=Unable to walk independently 2=Unable to walk independently but can walk with knee-ankle foot orthoses or support from a person 3=Highly adapted wide based lordotic gait. Cannot increase walking speed 4=Moderately adapted gait. Can pick up speed but cannot run 5=Able to pick up speed, but runs with a double stance phase, i.e. cannot achieve both feet off the ground 6=Runs and gets both feet off the ground (with no double stance phase)
Change From Baseline in Time to Stand From Supine Baseline (Day 1) to Week 52 To assess the change from baseline in the stand from supine speed at Week 52. For timed function tests (TFTs) , the time will be set to 12 seconds and the speed to 0 if the TFT assessment meets the following TFT grading criteria. Grade of 1 or 2 (from a 6-point scale). 1 = Unable to stand from supine, even with use of a chair, 2 = Assisted Gowers - requires furniture for assist in arising from supine to full upright posture (no time to be recorded) 3=Rolls over, stands up with both hands "climbing up" the legs to achieve full upright posture 4=Rolls over, stands up with 1 hand support on leg 5=Rolls to the side and stands up with one or both hands on the floor to start to rise but does not touch legs 6=Stands up without rolling over or using hands on legs or floor
Change From Baseline in 4-stair Climb Baseline (Day 1) to Week 52 To assess the change from baseline to Week 52 on the 4-Stair Climb. For timed function tests (TFTs) , the time will be set to 12 seconds and the speed to 0 if the TFT assessment meets the following TFT grading criteria. Grade of 1(from a 6-point scale)1=Unable to climb 4 standard stairs(no time recorded) 2=Climbs 4 standard stairs "marking time"(climbs one foot at a time, with both feet on a step before moving to next step), uses both arms on one or both handrails or uses 1 handrail and the other arm pushes on the leg 3=Climbs 4 standard stairs "marking time", using one arm on one handrail or one hand pushing on leg or body 4=Climbs 4 standard stairs "marking time", not needing handrail and not using hands to push on leg 5=Climbs 4 standard stairs alternating feet, needs handrail/s for support or uses arms to push on the leg or body 6=Climbs 4 standard stairs alternating feet, not needing handrail support or using arm to push on the leg
Safety and Tolerability Measured by Number of Treatment- Emergent Adverse Events (TEAEs) and Serious Adverse Events (SAEs) Up to Week 52 Adverse events that occurred from the time of the administration of the first dose of investigational product (IP) through the end of the safety follow-up were considered treatment-emergent AEs (TEAEs). Serious adverse event (SAE).
Trial Locations
- Locations (40)
Children's Hospital of Philadelphia
๐บ๐ธPhiladelphia, Pennsylvania, United States
Alberta Children's Hospital
๐จ๐ฆCalgary, Alberta, Canada
Children's Hospital of the King's Daughters
๐บ๐ธNorfolk, Virginia, United States
Great Ormond Street Hospital (GOSH)
๐ฌ๐งLondon, United Kingdom
University of Munich
๐ฉ๐ชMunich, Germany
University of Iowa Children's Hospital
๐บ๐ธIowa City, Iowa, United States
Queen Silvia Children's Hospital
๐ธ๐ชGothenburg, Sweden
Cook Children's Medical Center
๐บ๐ธFort Worth, Texas, United States
Rare Disease Research, LLC
๐บ๐ธAtlanta, Georgia, United States
The Children's Hospital at Westmead
๐ฆ๐บWestmead, New South Wales, Australia
Evelina Children's Hospital
๐ฌ๐งLondon, United Kingdom
Kennedy Krieger Institute
๐บ๐ธBaltimore, Maryland, United States
Johns Hopkins School of Medicine
๐บ๐ธBaltimore, Maryland, United States
Arkansas Children's Hospital
๐บ๐ธLittle Rock, Arkansas, United States
Children's University Hospital
๐ฎ๐ชDublin, Ireland
CHU Sainte-Justine
๐จ๐ฆMontrรฉal, Quebec, Canada
Children's Hospital of Los Angeles
๐บ๐ธLos Angeles, California, United States
Children's Hospital of Richmond at VCU
๐บ๐ธRichmond, Virginia, United States
Royal Children's Hospital
๐ฆ๐บParkville, Victoria, Australia
University of Hamburg
๐ฉ๐ชHamburg, Germany
Hadassah Medical Center
๐ฎ๐ฑJerusalem, Israel
London Health Sciences Centre - Children's Hospital
๐จ๐ฆLondon, Ontario, Canada
Bristol Children's Hospital
๐ฌ๐งBristol, United Kingdom
Royal Manchester Children's Hospital
๐ฌ๐งManchester, United Kingdom
Children's Health Queensland Children's Hospital and Health Service
๐ฆ๐บSouth Brisbane, Queensland, Australia
Children's Hospital of Eastern Ontario
๐จ๐ฆOttawa, Ontario, Canada
UC Davis
๐บ๐ธSacramento, California, United States
Las Vegas Clinic
๐บ๐ธLas Vegas, Nevada, United States
Nemours Children's Hospital
๐บ๐ธOrlando, Florida, United States
Rush University Children's Hospital
๐บ๐ธChicago, Illinois, United States
University of Michigan
๐บ๐ธAnn Arbor, Michigan, United States
Vanderbilt University Medical Center
๐บ๐ธNashville, Tennessee, United States
Boston Children's Hospital
๐บ๐ธBoston, Massachusetts, United States
University of Minnesota
๐บ๐ธMinneapolis, Minnesota, United States
Cincinnati Children's Hospital
๐บ๐ธCincinnati, Ohio, United States
MetroHealth Medical Center
๐บ๐ธCleveland, Ohio, United States
Shriners Hospitals for Children
๐บ๐ธPortland, Oregon, United States
University of Texas Health Science Center at San Antonio
๐บ๐ธSan Antonio, Texas, United States
University of Utah
๐บ๐ธSalt Lake City, Utah, United States
University of Kansas Medical Center
๐บ๐ธFairway, Kansas, United States