A phase I/IItrial of MYO-029 in adult subjects with muscular dystrophy

Objective Myostatin is an endogenous negative regulator of muscle growth and a novel target for muscle diseases. We conducted a safety trial of a neutralizing antibody to myostatin, MYO‐029, in adult muscular dystrophies (Becker muscular dystrophy, facioscapulohumeral dystrophy, and limb‐girdle musc...

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Bibliographic Details
Published in:Annals of neurology 2008-05, Vol.63 (5), p.561-571
Main Authors: Wagner, Kathryn R., Fleckenstein, James L., Amato, Anthony A., Barohn, Richard J., Bushby, Katharine, Escolar, Diana M., Flanigan, Kevin M., Pestronk, Alan, Tawil, Rabi, Wolfe, Gil I., Eagle, Michelle, Florence, Julaine M., King, Wendy M., Pandya, Shree, Straub, Volker, Juneau, Paul, Meyers, Kathleen, Csimma, Cristina, Araujo, Tracey, Allen, Robert, Parsons, Stephanie A., Wozney, John M., LaVallie, Edward R., Mendell, Jerry R.
Format: Article
Language:English
Subjects:
Adult
Antibodies - therapeutic use
Cohort Studies
Comorbidity
Double-Blind Method
Drug Eruptions - epidemiology
Female
Humans
Incidence
Internationality
Male
Muscular Dystrophies - drug therapy
Muscular Dystrophies - epidemiology
Placebo Effect
Risk Assessment - methods
Risk Factors
Treatment Outcome
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Summary:Objective Myostatin is an endogenous negative regulator of muscle growth and a novel target for muscle diseases. We conducted a safety trial of a neutralizing antibody to myostatin, MYO‐029, in adult muscular dystrophies (Becker muscular dystrophy, facioscapulohumeral dystrophy, and limb‐girdle muscular dystrophy). Methods This double‐blind, placebo‐controlled, multinational, randomized study included 116 subjects divided into sequential dose‐escalation cohorts, each receiving MYO‐029 or placebo (Cohort 1 at 1mg/kg; Cohort 2 at 3mg/kg; Cohort 3 at 10mg/kg; Cohort 4 at 30mg/kg). Safety and adverse events were assessed by reported signs and symptoms, as well as by physical examinations, laboratory results, echocardiograms, electrocardiograms, and in subjects with facioscapulohumeral dystrophy, funduscopic and audiometry examinations. Biological activity of MYO‐029 was assessed through manual muscle testing, quantitative muscle testing, timed function tests, subject‐reported outcomes, magnetic resonance imaging studies, dual‐energy radiographic absorptiometry studies, and muscle biopsy. Results MYO‐029 had good safety and tolerability with the exception of cutaneous hypersensitivity at the 10 and 30mg/kg doses. There were no improvements noted in exploratory end points of muscle strength or function, but the study was not powered to look for efficacy. Importantly, bioactivity of MYO‐029 was supported by a trend in a limited number of subjects toward increased muscle size using dual‐energy radiographic absorptiometry and muscle histology. Interpretation This trial supports the hypothesis that systemic administration of myostatin inhibitors provides an adequate safety margin for clinical studies. Further evaluation of more potent myostatin inhibitors for stimulating muscle growth in muscular dystrophy should be considered. Ann Neurol 2008
ISSN:0364-5134
1531-8249
DOI:10.1002/ana.21338