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Peer-reviewed veterinary case report

Gene therapy blocking myostatin in golden retriever muscular dystrophy

By Bish, Lawrence T et al.·Published in Human gene therapy·2011·Department of Physiology, United States·View original on PubMed

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Original publication title: Long-term systemic myostatin inhibition via liver-targeted gene transfer in golden retriever muscular dystrophy.

Species:
dog
Stomach & digestionDogs

Plain-English summary

A group of golden retrievers with muscular dystrophy underwent a new treatment aimed at increasing muscle mass by inhibiting a protein called myostatin. This involved a gene therapy delivered to the liver, and the dogs were monitored for 13 months using MRI scans. The results showed that the treatment successfully increased muscle size and reduced muscle damage. This promising approach could lead to new therapies for dogs and potentially for children with similar muscle diseases in the future.

People also search for: golden retriever muscular dystrophy treatment · myostatin inhibition in dogs · gene therapy for dog muscle disease

Abstract

Duchenne muscular dystrophy (DMD) is a lethal, X-linked recessive disease affecting 1 in 3,500 newborn boys for which there is no effective treatment or cure. One novel strategy that has therapeutic potential for DMD is inhibition of myostatin, a negative regulator of skeletal muscle mass that may also promote fibrosis. Therefore, our goal in this study was to evaluate systemic myostatin inhibition in the golden retriever model of DMD (GRMD). GRMD canines underwent liver-directed gene transfer of a self-complementary adeno-associated virus type 8 vector designed to express a secreted dominant-negative myostatin peptide (n = 4) and were compared with age-matched, untreated GRMD controls (n = 3). Dogs were followed with serial magnetic resonance imaging (MRI) for 13 months to assess cross-sectional area and volume of skeletal muscle, then euthanized so that tissue could be harvested for morphological and histological analysis. We found that systemic myostatin inhibition resulted in increased muscle mass in GRMD dogs as assessed by MRI and confirmed at tissue harvest. We also found that hypertrophy of type IIA fibers was largely responsible for the increased muscle mass and that reductions in serum creatine kinase and muscle fibrosis were associated with long-term myostatin inhibition in GRMD. This is the first report describing the effects of long-term, systemic myostatin inhibition in a large-animal model of DMD, and we believe that the simple and effective nature of our liver-directed gene-transfer strategy makes it an ideal candidate for evaluation as a novel therapeutic approach for DMD patients.

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Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/21787232/