SNP-based heritability and genetic architecture of tarsal osteochondrosis in North American Standardbred horses

A. M. McCoy, E. M. Norton, A. M. Kemper, S. K. Beeson, J. R. Mickelson, M. E. McCue

Research output: Contribution to journalArticlepeer-review

9 Scopus citations

Abstract

Osteochondrosis is a common developmental orthopedic disease characterized by a failure of endochondral ossification. Standardbred horses are recognized as being predisposed to tarsal osteochondrosis. Prior heritability estimates for tarsal osteochondrosis in European Standardbreds and related trotting breeds have been based on pedigree data and range from 17–29%. Here, we report on genetic architecture and heritability based on high-density genotyping data in a cohort of North American Standardbreds (n = 479) stringently phenotyped for tarsal osteochondrosis. Whole-genome array genotyping data were imputed to ~2 million single nucleotide polymorphisms (SNPs). SNP-based heritability of osteochondrosis in this population was explained by 2326 SNPs. The majority of these SNPs (86.6%) had small effects, whereas fewer SNPs had moderate or large effects (10% and 2.9% respectively), which is consistent with a polygenic/complex disease. Heritability was estimated at 0.24 ± 0.16 using two methods of restricted maximum likelihood analysis, as implemented in gcta (with and without a weighted relatedness matrix) and ldak software. Estimates were validated using bootstrapping. Heritability estimates were within the range previously reported and suggest that osteochondrosis is moderately heritable but that a significant portion of disease risk is due to environmental factors and/or genotype × environment interactions. Future identification of the genes/variants that have the most impact on disease risk may allow early recognition of high-risk individuals.

Original languageEnglish (US)
Pages (from-to)78-81
Number of pages4
JournalAnimal Genetics
Volume50
Issue number1
DOIs
StatePublished - Feb 1 2019

Bibliographical note

Funding Information:
Funding support for genotyping provided by USDA-NIFA-AFRI 2011-03216 (Genetic Diversity and Selection in the Domestic Horse), USDA Hatch Funds (University of Illinois), CVM Animal Health & Disease (University of Minnesota USDA Formula Funds), Minnesota Agricultural Experiment Station, Morris Animal Foundation (D16EQ-311) and the United States Equestrian Federation, Inc.

Publisher Copyright:
© 2018 Stichting International Foundation for Animal Genetics

Keywords

  • complex trait
  • equine
  • hock OCD
  • imputation
  • inherited
  • restricted maximum likelihood analysis

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