Overview
Phase II Study of NPC-14 (Arbekacin Sulfate) to Explore Safety, Tolerability, and Efficacy in Duchenne Muscular Dystrophy
Status:
Unknown status
Unknown status
Trial end date:
2015-10-01
2015-10-01
Target enrollment:
0
0
Participant gender:
Male
Male
Summary
Duchenne Muscular Dystrophy (DMD) is inherited neuromuscular disorders due to mutation in the gene that encodes critical muscle protein called dystrophin. Currently, there is no effective treatment option for the disease. A pharmacological approach by promoting mRNA translation regardless of the presence of premature stop codons by nonsense mutation, called the readthrough strategy, has been developing recently for DMD with nonsense mutation. NPC-14 is a candidate compound for the readthrough strategy, since effective readthrough activities were demonstrated in nonclinical studies. This study is a phase II study designed to assess safety, tolerability, and efficacy of NPC-14 in ambulant DMD patients with nonsense mutation that were confirmed by whole genome analysis. These goals will be accomplished by monitoring adverse events by physical examination, cardiac, pulmonary, auditory, balance, and laboratory tests as safety endpoints, and dystrophin expression in muscle biopsy as primary efficacy endpoint, muscle function (NSAA, timed test, muscle strength (QMT, MMT) , dairy activities by lifecorder), and biomarkers as secondary efficacy endpoints. The study is a randomized, double blind, placebo-controlled study in 21 DMD patients. After screening, eligible patients are allocated dynamically to weekly NPC-14 or a placebo (saline) in a 2:1 ratio and will receive study drugs for 36 weeks.Phase:
Phase 2Accepts Healthy Volunteers?
NoDetails
Lead Sponsor:
Kobe UniversityCollaborators:
Japan Medical Association
NobelpharmaTreatments:
Arbekacin
Dibekacin
Habekacin
Criteria
Inclusion Criteria:1. Diagnosis of DMD resulting from a nonsense mutation by whole genome sequencing of the
dystrophin gene
2. To have intact right or left biceps muscles, or an alternative muscle group that is
able to be underwent for appropriate evaluation of efficacy
3. To meet the following criteria at screening (baseline visit), within 30 days prior to
the first dose of study drug
- Ambulant and able to walk at least 75 meters during the 6MWT
- Able to comply with and complete all protocol requirements, and judged by the
investigator to be appropriate to participate in the study from the screening
results
4. Aged at least 4 years at the time of giving informed consent
5. Male
6. Able to be hospitalized for the study requirement
7. Signed Informed consent by parents/legal guardian and/or signed assent by the subject
(age of assent to be determined by IRB)
Exclusion Criteria:
1. Prior exposure to investigational medicines that have a potential of restoring
dystrophin or other functional protein (readthrough, exon skipping, utrophin
upregulation therapy etc.)
2. Known mutation at nucleotide 1555 in 12S rRNA gene of mitochondrial DNA, and/or
personally or families have been treated or have a history of eight cranial nerve
disorder (hearing loss、vertigo、tinnitus etc.)as a result of aminoglycoside use
3. Inability to hear within the range of 0 to 25 dB by pure tone audiometry,
abnormalities on auditory brainstem response audiometry, and/or loss of frequency by
distortion product oto acoustic emissions at screening
4. Poor oral intake or enable to oral intake, and/or bad general status
5. Known allergies to NPC-14, other aminoglycosides, and/or bacitracin
6. Presence of anti-dystrophin antibody at the baseline assessments
7. Cys-C ≥1.2 mg/L and/or creatinine concentration >1.5 times the upper limit of age
corrected normal range
8. Left ventricular ejection fraction (EF) <40% or left ventricular fractional shortening
(FS) <25%, and/or ≥480 msec QTc (corrected QT interval by Fridericia's method)
9. Need of mechanical ventilation
10. Forced vital capacity (FVC) <50% predicted
11. Clinically significant concomitant diseases (hematology, psychoneurotic, hepatic,
pulmonary, endocrine, immune, renal, and gastroenterological diseases), and/or cancer
12. Impairment of intellectual functions, and/or expressive language ability which might
interfere with study assessments
13. Treatment with other systemic aminoglycoside within 6 months prior to the first
administration of study drug
14. Initiation of systemic glucocorticosteroids treatment, and/or start exercise cure,
physical therapy, or occupational therapy which might interfere with study
assessments. Changing of dose and schedule of systemic glucocorticosteroids within 6
months prior to the first administration of study drug
15. History of any surgical procedure within months prior to the first administration of
study drug or have a plan during study
16. History of sever allergy from food and medicine like an anaphylaxis shock or
generalized rash
17. Participation in any other clinical trial and intake of any investigational drug
within 6month of study entry