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Peer-reviewed veterinary case report

AMissense Variant Is Associated with Canine Laryngeal Paralysis and Polyneuropathy.

Journal:
Genes
Year:
2020
Authors:
Letko, Anna et al.
Affiliation:
Institute of Genetics
Species:
dog

Abstract

Laryngeal paralysis associated with a generalized polyneuropathy (LPPN) most commonly exists in geriatric dogs from a variety of large and giant breeds. The purpose of this study was to discover the underlying genetic and molecular mechanisms in a younger-onset form of this neurodegenerative disease seen in two closely related giant dog breeds, the Leonberger and Saint Bernard. Neuropathology of an affected dog from each breed showed variable nerve fiber loss and scattered inappropriately thin myelinated fibers. Using across-breed genome-wide association, haplotype analysis, and whole-genome sequencing, we identified a missense variant in thegene (c.2810G>A; p.Gly937Glu) in which homozygotes in both studied breeds are affected.encodes a contactin-associated protein important for organization of myelinated axons. The herein described likely pathogenicvariant occurs in unrelated breeds at variable frequencies. Individual homozygous mutant LPPN-affected Labrador retrievers that were on average four years younger than dogs affected by geriatric onset laryngeal paralysis polyneuropathy could be explained by this variant. Pathologic changes in a Labrador retriever nerve biopsy from a homozygous mutant dog were similar to those of the Leonberger and Saint Bernard. The impact of this variant on health in English bulldogs and Irish terriers, two breeds with highervariant allele frequencies, remains unclear. Pathogenic variants inhave previously been reported in human patients with lethal congenital contracture syndrome and hypomyelinating neuropathy, including vocal cord palsy and severe respiratory distress. This is the first report of contactin-associated LPPN in dogs characterized by a deleterious variant that most likely predates modern breed establishment.

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Original publication: https://pubmed.ncbi.nlm.nih.gov/33261176/