Common variants in the CPT1A gene are associated with cataracts in Northern breeds of domestic dog.
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Abstract
Primary hereditary cataract affects many purebred domestic dog breeds and is a major cause of visual impairment in dogs. Cataracts are common in Northern breeds such as the Siberian Husky, Alaskan Malamute and Samoyed, but their aetiology is currently unknown. Only two genetic loci are known to be causally related to primary hereditary cataracts in the dog. To search for genetic loci associated with cataracts in Northern breeds, we used a genome-wide association study approach in three breeds-Siberian Husky, Alaskan Malamute and Samoyed. Cases were defined as dogs with bilateral posterior polar subcapsular cataracts and controls were at least four years of age with no evidence of cataracts or other ocular abnormality. We found a genome-wide statistical association for cataracts in the Siberian Husky on canine chromosome 18 (P-value: 1.1 x 10 - 7), which was independently replicated in a second larger case-control set (P-value 9.8 x 10 - 29). The Samoyed breed also showed evidence for association in the same genomic region (P-value: 2.4 x 10 - 5). We subsequently used targeted resequencing of the associated region (6.5 Mb) in ten Siberian Huskies and whole genome sequencing of a Husky, Malamute, Samoyed and Norwegian Buhund case to conduct fine-mapping and screen for candidate causal variants. These analyses identified a region of linkage disequilibrium in the four breeds containing common variants in the carnitine palmitoyltransferase 1A (CPT1A) gene that are strongly associated with bilateral posterior polar subcapsular cataracts in the Siberian Husky, Samoyed, Icelandic Sheepdog and Norwegian Buhund and we demonstrate that CPT1A is expressed in the dog lens and retina through RNAseq. Our findings represent a novel locus for cataracts in dogs. However, further work is needed to elucidate the pathophysiology underlying the association between CPT1A and cataracts in Northern breeds.
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Acknowledgements: We would like to sincerely thank all owners for providing samples from their dogs for this study. We would also like to specifically thank the members of the Siberian Husky Club of Great Britain, Siberian Husky Club of America, Alaskan Malamute Club of Great Britain, Alaskan Malamute Club of America, Alaskan Malamute Working Association, The Danish Polar Dog Club, Icelandic Sheepdog Association of America, Samoyed Club of America Education & Research Foundation, Orthopedic Foundation for Animals, Susan Pearce-Kelling formerly of OptiGen/Wisdom Health, British and Finnish Samoyed Clubs, Finnish Lapphund Club, Southern Finnish Lapphund Society, and Norwegian Buhund Club for their assistance with sample collection, study publicity and financial contributions. We thank the High-Throughput Genomics Group at the Wellcome Trust Centre for Human Genetics for the generation of the sequencing data. We also thank Claudia Hartley (BVSc CertVOphthal DipECVO MRCVS) and Claudia Busse (Dr.med vet., MRCVS, CertVOphthal, DipECVO) for assisting with case definitions; and Hanne Ahola, Ranja Eklund, Minna Virta, Reeta Hänninen and Sini Karjalainen for technical assistance. The authors would like to thank the Banfield clinicians that diligently recorded their clinical findings, the Mars Data Curation team, and all of the pet owners who contributed samples from their dogs.
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1932-6203
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American Kennel Club Canine Health Foundation (01670-A)

