Abstract
BackgroundHip dysplasia and osteoarthritis continue to be prevalent problems in veterinary and human medicine. Canine hip dysplasia is particularly problematic as it massively affects several large-sized breeds and can cause a severe impairment of the quality of life. In Finland, the complex condition is categorized to five classes from normal to severe dysplasia, but the categorization includes several sub-traits: congruity of the joint, Norberg angle, subluxation degree of the joint, shape and depth of the acetabulum, and osteoarthritis. Hip dysplasia and osteoarthritis have been proposed to have separate genetic etiologies.ResultsUsing Fédération Cynologique Internationale -standardized ventrodorsal radiographs, German shepherds were rigorously phenotyped for osteoarthritis, and for joint incongruity by Norberg angle and femoral head center position in relation to dorsal acetabular edge. The affected dogs were categorized into mild, moderate and severe dysplastic phenotypes using official hip scores. Three different genome-wide significant loci were uncovered. The strongest candidate genes for hip joint incongruity were noggin (NOG), a bone and joint developmental gene on chromosome 9, and nanos C2HC-type zinc finger 1 (NANOS1), a regulator of matrix metalloproteinase 14 (MMP14) on chromosome 28. Osteoarthritis mapped to a long intergenic region on chromosome 1, between genes encoding for NADPH oxidase 3 (NOX3), an intriguing candidate for articular cartilage degradation, and AT-rich interactive domain 1B (ARID1B) that has been previously linked to joint laxity.ConclusionsOur findings highlight the complexity of canine hip dysplasia phenotypes. In particular, the results of this study point to the potential involvement of specific and partially distinct loci and genes or pathways in the development of incongruity, mild dysplasia, moderate-to-severe dysplasia and osteoarthritis of canine hip joints. Further studies should unravel the unique and common mechanisms for the various sub-traits.
Highlights
Hip dysplasia and osteoarthritis continue to be prevalent problems in veterinary and human medicine
A standardized system for Canine hip dysplasia (CHD) grading has been developed in the countries that belong to the Fédération Cynologique Internationale (FCI)
Norberg angle (NoA) and femoral head center position in relation to dorsal acetabular edge (FHCDAE) reflect the incongruity of the hip joint, which impacts the development of CHD [2]
Summary
Hip dysplasia and osteoarthritis continue to be prevalent problems in veterinary and human medicine. Hip dysplasia and osteoarthritis have been proposed to have separate genetic etiologies. Canine hip dysplasia (CHD) is a common multifactorial hereditary disorder that has perplexed dog owners, breeders as well as veterinarians and researchers for decades. As the FCI or any other combinatory score does not accurately correlate with the various CHD sub-traits, these have to be studied separately. NoA and femoral head center position in relation to dorsal acetabular edge (FHCDAE) reflect the incongruity of the hip joint, which impacts the development of CHD [2]. Hip joint laxity is a major contributor to the development of OA. OA may have a distinct genetic background in relation to the other hip sub-traits [4,5,6]
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