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Peer-reviewed veterinary case report

Blistering skin disease in Cardigan Welsh Corgi puppy caused by KRT5

By Kiener, Sarah et al.·Published in Animal genetics·2022·Vetsuisse Faculty·View original on PubMed

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Original publication title: KRT5 missense variant in a Cardigan Welsh Corgi with epidermolysis bullosa simplex.

Species:
dog
Skin & coatDogs

Plain-English summary

A young Cardigan Welsh Corgi puppy was brought in with painful blisters and sores on its paw pads and inside its mouth. After examining the puppy's skin, the veterinarian confirmed it had a condition called epidermolysis bullosa, which causes the skin to blister easily. Genetic testing revealed a specific mutation in a gene called KRT5 that was responsible for the puppy's symptoms. This mutation was new and not found in the puppy's parents. Understanding this genetic issue can help guide future care and treatment for the puppy.

People also search for: puppy blisters on paws · epidermolysis bullosa in dogs · Cardigan Welsh Corgi skin problems

Abstract

Epidermolysis bullosa (EB) is a group of blistering disorders that includes several subtypes, classified according to their level of cleavage. Typical clinical signs are blisters and erosions resulting from minimal trauma. The disease has been described in many mammalian species and pathogenic variants in at least 18 different genes have been identified. In the present study, we investigated a Cardigan Welsh Corgi with congenital clinical signs consistent with epidermolysis bullosa. The puppy had blisters and erosions on the paw pads, and the oral mucosa. Histologic examination demonstrated the typical clefting between the dermis and epidermis and confirmed the clinical suspicion. We obtained whole genome sequencing data from the affected puppy and searched for variants in candidate genes known to cause EB. This revealed a heterozygous missense variant, KRT5:p.(E476K), affecting the highly conserved KLLEGE motif of keratin 5. The mutant allele in the affected puppy arose owing to a de novo mutation event as it was absent from both unaffected parents. Knowledge of the functional impact of KRT5 variants in other species together with the demonstration of the de novo mutation event establishes KRT5:p.(E476K) as causative variant for the observed EBS.

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Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/36004757/