4.4 Article

Evaluation of an HMGA2 variant contribution to height and basal insulin concentrations in ponies

Journal

JOURNAL OF VETERINARY INTERNAL MEDICINE
Volume 37, Issue 3, Pages 1186-1192

Publisher

WILEY
DOI: 10.1111/jvim.16723

Keywords

endocrinology; equine metabolic syndrome; genetics; hyperinsulinemia-associated laminitis; insulin dysregulation; Shetland; Welsh pony

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The study revealed that the HMGA2:c.83G>A variant is associated with decreased height and higher insulin concentrations in ponies across different breeds. This variant explains 90.5% of the height variation and 7.1% of the insulin variation. Ponies with the A/A genotype are over 10 cm shorter than other genotypes, and A/A and G/A individuals have significantly higher basal insulin concentrations compared to G/G individuals.
BackgroundThe HMGA2:c.83G>A variant was identified in Welsh ponies having pleiotropic effects on height and insulin concentration. ObjectiveDetermine whether the HMGA2:c.83G>A variant is associated with decreased height and higher basal insulin concentrations across pony breeds. AnimalsTwo hundred thirty-six ponies across 6 breeds. MethodsCross-sectional study. Ponies were genotyped for the HMGA2:c.83G>A variant and phenotyped for height and basal insulin concentrations. Stepwise regression was performed for model analysis using a linear regression model for height and mixed linear model for insulin with farm as a random effect. Coefficient of determination, pairwise comparison of the estimated marginal means and partial correlation coefficients (parcor) were calculated to assess the relationship between HMGA2 genotype and height or insulin. ResultsBreed and genotype accounted for 90.5% of the variation in height across breeds, and genotype explained 21% to 44% of the variation within breeds. Breed, genotype, cresty neck score, sex, age, and farm accounted for 45.5% of the variation in insulin, with genotype accounting for 7.1%. The HMGA2 A allele frequency was 62% and correlated with both height (parcor = -0.39; P < .001) and insulin (parcor = 0.22; P = .02). Pairwise comparisons found A/A ponies were >10 cm shorter than other genotypes. Compared with G/G individuals, A/A and G/A individuals had 4.3 mu IU/mL (95% confidence interval [CI]: 1.8-10.5) and 2.7 mu IU/mL (95% CI: 1.4-5.3) higher basal insulin concentrations, respectively. Conclusions and Clinical ImportanceThese data demonstrate the pleiotropic effects of the HMGA2:c.83G>A variant and its role in identifying ponies at increased risk for insulin dysregulation.

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