Peer-reviewed veterinary case report
Systemic morpholino exon-skipping treatment tested in Duchenne
By Yokota, Toshifumi et al.·Published in Annals of neurology·2009·Research Center for Genetic Medicine, United States·View original on PubMed →
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Original publication title: Efficacy of systemic morpholino exon-skipping in Duchenne dystrophy dogs.
- Species:
- dog
Plain-English summary
A group of dogs with Duchenne muscular dystrophy (DMD) received a new treatment involving a combination of drugs delivered through intravenous injections. Over 5 to 22 weeks, this therapy successfully increased the production of a crucial protein called dystrophin, which is missing in these dogs. The treatment led to improved muscle function and reduced inflammation, with no signs of harmful side effects. This approach shows promise for helping dogs with DMD and could potentially benefit many more dogs with similar conditions.
People also search for: dog Duchenne muscular dystrophy treatment · DMD dog symptoms · dystrophin therapy for dogs
Abstract
OBJECTIVE: Duchenne muscular dystrophy (DMD) is caused by the inability to produce dystrophin protein at the myofiber membrane. A method to rescue dystrophin production by antisense oligonucleotides, termed exon-skipping, has been reported for the mdx mouse and in four DMD patients by local intramuscular injection. We sought to test efficacy and toxicity of intravenous oligonucleotide (morpholino)-induced exon skipping in the DMD dog model. METHODS: We tested a series of antisense drugs singly and as cocktails, both in primary cell culture, and two in vivo delivery methods (intramuscular injection and systemic intravenous injection). The efficiency and efficacy of multiexon skipping (exons 6-9) were tested at the messenger RNA, protein, histological, and clinical levels. RESULTS: Weekly or biweekly systemic intravenous injections with a three-morpholino cocktail over the course of 5 to 22 weeks induced therapeutic levels of dystrophin expression throughout the body, with an average of about 26% normal levels. This was accompanied by reduced inflammatory signals examined by magnetic resonance imaging and histology, improved or stabilized timed running tests, and clinical symptoms. Blood tests indicated no evidence of toxicity. INTERPRETATION: This is the first report of widespread rescue of dystrophin expression to therapeutic levels in the dog model of DMD. This study also provides a proof of concept for systemic multiexon-skipping therapy. Use of cocktails of morpholino, as shown here, allows broader application of this approach to a greater proportion of DMD patients (90%) and also offers the prospect of selecting deletions that optimize the functionality of the dystrophin protein.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/19288467/