Peer-reviewed veterinary case report
Genetic risk factors for claw disease SLO in Gordon setter dogs
By Wilbe, Maria et al.·Published in PloS one·2010·Department of Animal Breeding and Genetics·View original on PubMed →
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Original publication title: DLA class II alleles are associated with risk for canine symmetrical lupoid onychodystrophy [corrected](SLO).
- Species:
- dog
Plain-English summary
A group of Gordon Setters with symmetrical lupoid onychodystrophy (SLO), a condition that affects their claws and is linked to immune system issues, was studied to understand genetic risk factors. Researchers found that a specific genetic marker was present in over half of the affected dogs, suggesting they are more likely to develop this condition. In contrast, a different genetic marker appeared to offer protection and was found mostly in healthy dogs. This study highlights the importance of genetics in SLO and suggests that understanding these factors could help with similar nail-related issues in dogs.
People also search for: Gordon Setter claw problems · dog nail disease treatment · immune system issues in dogs
Abstract
Symmetrical lupoid onychodystrophy (SLO) is an immune-mediated disease in dogs affecting the claws with a suggested autoimmune aethiology. Sequence-based genotyping of the polymorphic exon 2 from DLA-DRB1, -DQA1, and -DQB1 class II loci were performed in a total of 98 SLO Gordon setter cases and 98 healthy controls. A risk haplotype (DRB1*01801/DQA1*00101/DQB1*00802) was present in 53% of cases and 34% of controls and conferred an elevated risk of developing SLO with an odds ratio (OR) of 2.1. When dogs homozygous for the risk haplotype were compared to all dogs not carrying the haplotype the OR was 5.4. However, a stronger protective haplotype (DRB1*02001/DQA1*00401/DQB1*01303, OR = 0.03, 1/OR = 33) was present in 16.8% of controls, but only in a single case (0.5%). The effect of the protective haplotype was clearly stronger than the risk haplotype, since 11.2% of the controls were heterozygous for the risk and protective haplotypes, whereas this combination was absent from cases. When the dogs with the protective haplotype were excluded, an OR of 2.5 was obtained when dogs homozygous for the risk haplotype were compared to those heterozygous for the risk haplotype, suggesting a co-dominant effect of the risk haplotype. In smaller sample sizes of the bearded collie and giant schnauzer breeds we found the same or similar haplotypes, sharing the same DQA1 allele, over-represented among the cases suggesting that the risk is associated primarily with DLA-DQ. We obtained conclusive results that DLA class II is significantly associated with risk of developing SLO in Gordon setters, thus supporting that SLO is an immune-mediated disease. Further studies of SLO in dogs may provide important insight into immune privilege of the nail apparatus and also knowledge about a number of inflammatory disorders of the nail apparatus like lichen planus, psoriasis, alopecia areata and onycholysis.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/20808798/