Peer-reviewed veterinary case report
FAS ligand gene variant linked to autoimmune disease in New Zealand
By Aberdein, D et al.·Published in New Zealand veterinary journal·2017·a Institute of Veterinary·View original on PubMed →
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Original publication title: Frequency of a FAS ligand gene variant associated with inherited feline autoimmune lymphoproliferative syndrome in British shorthair cats in New Zealand.
- Species:
- cat
Plain-English summary
A group of British Shorthair cats in New Zealand was tested for a genetic variant linked to a serious condition called feline autoimmune lymphoproliferative syndrome (FALPS), which can be fatal in young cats. Out of 32 cats tested, one kitten was found to be affected by the disease, while seven others were carriers of the gene variant. This means that about 22% of the healthy cats had the potential to pass on the condition. To help prevent future cases, it is recommended that all British Shorthair cats be tested for this variant before breeding, and carriers should be spayed or neutered.
People also search for: British Shorthair cat genetic testing · FALPS in cats · inherited diseases in cats · cat breeding health tests
Abstract
AIMS To determine the frequency of the FAS-ligand gene (FASLG) variant associated with feline autoimmune lymphoproliferative syndrome (FALPS) and the proportion of carriers of the variant in three British shorthair (BSH) breeding catteries in New Zealand. METHODS Buccal swabs were collected from all cats in two BSH breeding catteries from the South Island and one from the North Island of New Zealand. DNA was extracted and was tested for the presence of the FASLG variant using PCR. Cats with the FASLG variant were identified and the frequency of the FASLG variant allele calculated. Pedigree analysis was performed and inbreeding coefficients were calculated for cats with the FASLG variant. RESULTS Of 32 BSH cats successfully tested for the presence of the FASLG variant, one kitten (3%) was homozygous (FALPS-affected), and seven (22%) cats were heterozygous (carriers) for the FASLG variant allele, and 24 (75%) cats were homozygous for the wild type allele. The overall frequency of the FASLG variant allele in these 32 cats was 0.14. Cats carrying the FASLG variant were from all three breeding catteries sampled, including two catteries that had not previously reported cases of FALPS. Pedigree analysis revealed common ancestry of FALPS-affected and carrier cats within six generations, as well as frequent inbreeding, with inbreeding coefficients >0.12 for five cats with the FASLG variant. CONCLUSIONS AND CLINICAL RELEVANCE There was a high frequency of the FASLG variant allele (0.14) in this small sample of BSH cats, with 22% of healthy cats identified as carriers of the FASLG variant. For an inherited disease, lethal at a young age, in a small population in which inbreeding is common, these results are significant. To prevent future cases of disease and stop further spread of the FASLG variant allele within the BSH population in New Zealand, it is recommended that all BSH and BSH-cross cats be tested for the presence of the FASLG variant before mating. Cats identified as carriers of the variant allele should be desexed and not used for breeding. Results support the need for further investigations of the true frequency of the FASLG variant allele and occurrence of FALPS in the wider population of BSH cats in New Zealand.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/28814155/