Peer-reviewed veterinary case report
Muscle weakness in a 5-month Border Collie linked to new gene change
By Van Poucke, Mario et al.·Published in Animal genetics·2024·Department of Veterinary and Biosciences·View original on PubMed →
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Original publication title: Exonisation of an intronic L1 element in the dystrophin gene associated with X-linked muscular dystrophy in a Border Collie dog.
- Species:
- dog
Plain-English summary
A 5-month-old male Border Collie was diagnosed with a mild form of muscular dystrophy after showing signs of muscle weakness. Tests, including blood work and muscle biopsies, revealed a genetic mutation affecting the dystrophin gene, which is important for muscle function. Although muscular dystrophy often has a poor outlook, this dog has remained stable and healthy, reaching 2 years of age without significant deterioration. Regular monitoring and supportive care have helped maintain his condition.
People also search for: Border Collie muscular dystrophy symptoms · dog muscle weakness treatment · what is dystrophin deficiency in dogs
Abstract
X-linked recessive dystrophinopathies are the most common muscular dystrophies (MDs) in humans and dogs. To date, 20 breed-specific MD-associated variants are described in the canine dystrophin gene (DMD), including one associated with dystrophin-deficient MD in the Border Collie mixed breed. Here, we report the diagnosis and follow-up of mild dystrophin-deficient MD in a 5-month-old male Border Collie, associated with a novel DMD variant. Diagnosis was based on neurological examination and laboratory evaluations including creatine kinase activity, electromyography and muscle biopsies with immunofluorescent staining. Inspection of the Sashimi plots of the RNA-seq data from the affected muscle biopsy led to the discovery of a 162-bp L1 pseudoexon in DMD intron 63, introducing a frameshift and a premature stop codon (NM_001003343.1: c.9271_9272insN[162] p.(Ala3091fs*21)). Reduced DMD mRNA levels were detected for both the non-pseudoexon (50× less) and pseudoexon (3× less) containing transcripts in the affected muscle, compared with the level of the non-pseudoexon containing transcript in a control muscle, resulting in very low dystrophin protein levels and the upregulation of utrophin. Because the variant was only found in the affected dog, not in the healthy mother and grandmother, or in 108 unrelated Border Collies from the Belgian population (46 males and 62 females), it was considered a de novo variant. Although the prognosis for dystrophinopathy is generally regarded as poor, the dog stabilised at the age of 6 months and is still clinically stable at the age of 2 years.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/39152696/