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Peer-reviewed veterinary case report

ARHGEF10 gene deletion linked to nerve disease in young Leonberger

By Ekenstedt, Kari J et al.·Published in PLoS genetics·2014·Department of Veterinary and Biomedical Sciences, United States·View original on PubMed

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Original publication title: An ARHGEF10 deletion is highly associated with a juvenile-onset inherited polyneuropathy in Leonberger and Saint Bernard dogs.

Species:
dog

Plain-English summary

A young Leonberger or Saint Bernard dog with exercise intolerance, trouble walking, and muscle weakness in the back legs may be suffering from a severe inherited nerve condition. Researchers found that a specific genetic mutation in the ARHGEF10 gene is linked to this condition, which resembles a type of nerve disorder seen in humans. The mutation leads to serious issues with nerve function, causing the symptoms to appear at a young age and worsen over time. Unfortunately, there is currently no cure, but understanding this genetic link can help owners and vets manage the dog's care more effectively.

People also search for: Leonberger exercise intolerance · Saint Bernard muscle weakness · inherited polyneuropathy in dogs

Abstract

An inherited polyneuropathy (PN) observed in Leonberger dogs has clinical similarities to a genetically heterogeneous group of peripheral neuropathies termed Charcot-Marie-Tooth (CMT) disease in humans. The Leonberger disorder is a severe, juvenile-onset, chronic, progressive, and mixed PN, characterized by exercise intolerance, gait abnormalities and muscle atrophy of the pelvic limbs, as well as inspiratory stridor and dyspnea. We mapped a PN locus in Leonbergers to a 250 kb region on canine chromosome 16 (Praw = 1.16×10-10, Pgenome, corrected = 0.006) utilizing a high-density SNP array. Within this interval is the ARHGEF10 gene, a member of the rho family of GTPases known to be involved in neuronal growth and axonal migration, and implicated in human hypomyelination. ARHGEF10 sequencing identified a 10 bp deletion in affected dogs that removes four nucleotides from the 3'-end of exon 17 and six nucleotides from the 5'-end of intron 17 (c.1955_1958+6delCACGGTGAGC). This eliminates the 3'-splice junction of exon 17, creates an alternate splice site immediately downstream in which the processed mRNA contains a frame shift, and generates a premature stop codon predicted to truncate approximately 50% of the protein. Homozygosity for the deletion was highly associated with the severe juvenile-onset PN phenotype in both Leonberger and Saint Bernard dogs. The overall clinical picture of PN in these breeds, and the effects of sex and heterozygosity of the ARHGEF10 deletion, are less clear due to the likely presence of other forms of PN with variable ages of onset and severity of clinical signs. This is the first documented severe polyneuropathy associated with a mutation in ARHGEF10 in any species.

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Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/25275565/