Peer-reviewed veterinary case report
New gene variant found causing muscular dystrophy in young male cat
By G. Diane Shelton et al.·Published in Journal of Veterinary Internal Medicine·2024·Department of Pathology, School of Medicine University of California San Diego La Jolla California USA, GB·View original on DOAJ →
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Original publication title: Precision medicine using whole genome sequencing identifies a novel dystrophin (DMD) variant for X‐linked muscular dystrophy in a cat
- Species:
- cat
Plain-English summary
A 1-year-old male domestic shorthair cat was brought in for trouble walking, a swollen tongue, and difficulty swallowing that started when he was 6 months old. The vet performed a thorough examination and muscle biopsies, which showed signs of muscle degeneration. Blood tests revealed high levels of certain enzymes, indicating muscle damage. Whole genome sequencing identified a specific genetic variant linked to a type of muscular dystrophy in cats. This diagnosis helps in understanding the condition better and may lead to targeted treatments in the future.
People also search for: cat difficulty walking · swollen tongue in cats · muscular dystrophy in cats · cat genetic testing for diseases · cat muscle problems treatment
Abstract
Abstract Background Muscular dystrophies (MDs) are a large, heterogeneous group of degenerative muscle diseases. X‐linked dystrophin‐deficient MD in cats is the first genetically characterized cat model for a human disease and a few novel forms have been identified. Hypothesis/Objectives Muscular dystrophy was suspected in a young male domestic shorthair cat. Clinical, molecular, and genetic techniques could provide a definitive diagnosis. Animals A 1‐year‐old male domestic shorthair cat presented for progressive difficulty walking, macroglossia and dysphagia beginning at 6 months of age. The tongue was thickened, protruded with constant ptyalism, and thickening and rigidity of the neck and shoulders were observed. Methods A complete neurological examination, baseline laboratory evaluation and biopsies of the trapezius muscle were performed with owner consent. Indirect immunofluorescence staining of muscle cryosections was performed using several monoclonal and polyclonal antibodies against dystrophy‐associated proteins. DNA was isolated for genomic analyses by whole genome sequencing and comparison to DNA variants in the 99 Lives Cat Genome Sequencing dataset. Results and Clinical Importance Aspartate aminotransferase (687 IU/L) and creatine kinase (24 830 IU/L) activities were increased and mild hypokalemia (3.7 mmol/L) was present. Biopsy samples from the trapezius muscle confirmed a degenerative and regenerative myopathy and protein alterations identified by immunohistochemistry resulted in a diagnosis of a in dystrophin‐deficient form of X‐linked MD. A stop gain variant (c.4849C>T; p.Gln1617Ter) dystrophin was identified by genome sequencing. Precision/genomic medicine efforts for the domestic cat and in veterinary medicine support disease variant and animal model discovery and provide opportunities for targeted treatments for companion animals.
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Search related cases →Original publication on DOAJ: https://doi.org/10.1111/jvim.16971