A Functional Single-Nucleotide Polymorphism Upstream of the Collagen Type III Gene Is Associated with Catastrophic Fracture Risk in Thoroughbred Horses

Author:

Palomino Lago Esther1ORCID,Baird Arabella2ORCID,Blott Sarah C.3ORCID,McPhail Rhona E.2,Ross Amy C.1,Durward-Akhurst Sian A.4ORCID,Guest Deborah J.1ORCID

Affiliation:

1. Department of Clinical Sciences and Services, The Royal Veterinary College, Hawkshead Lane, North Mymms, Hatfield AL9 7TA, UK

2. Animal Health Trust, Lanwades Park, Kentford, Newmarket CB8 7UU, UK

3. School of Veterinary Medicine and Science, University of Nottingham, Nottingham LE12 5RD, UK

4. Department of Veterinary Clinical Sciences, University of Minnesota, Saint Paul, MN 55108, USA

Abstract

Fractures caused by bone overloading are a leading cause of euthanasia in Thoroughbred racehorses. The risk of fatal fracture has been shown to be influenced by both environmental and genetic factors but, to date, no specific genetic mechanisms underpinning fractures have been identified. In this study, we utilised a genome-wide polygenic risk score to establish an in vitro cell system to study bone gene regulation in horses at high and low genetic risk of fracture. Candidate gene expression analysis revealed differential expression of COL3A1 and STAT1 genes in osteoblasts derived from high- and low-risk horses. Whole-genome sequencing of two fracture cases and two control horses revealed a single-nucleotide polymorphism (SNP) upstream of COL3A1 that was confirmed in a larger cohort to be significantly associated with fractures. Bioinformatics tools predicted that this SNP may impact the binding of the transcription factor SOX11. Gene modulation demonstrated SOX11 is upstream of COL3A1, and the region binds to nuclear proteins. Furthermore, luciferase assays demonstrated that the region containing the SNP has promoter activity. However, the specific effect of the SNP depends on the broader genetic background of the cells and suggests other factors may also be involved in regulating COL3A1 expression. In conclusion, we have identified a novel SNP that is significantly associated with fracture risk and provide new insights into the regulation of the COL3A1 gene.

Funder

Horserace Betting Levy Board

Anne Duchess of Westminster Charitable Trust

Alborada Trust

Publisher

MDPI AG

Subject

General Veterinary,Animal Science and Zoology

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