Nature Communications (Nov 2024)

Effect of genetically predicted sclerostin on cardiovascular biomarkers, risk factors, and disease outcomes

  • Marta Alcalde-Herraiz,
  • JunQing Xie,
  • Danielle Newby,
  • Clara Prats,
  • Dipender Gill,
  • María Gordillo-Marañón,
  • Daniel Prieto-Alhambra,
  • Martí Català,
  • Albert Prats-Uribe

DOI
https://doi.org/10.1038/s41467-024-53623-5
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 12

Abstract

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Abstract Sclerostin inhibitors protect against osteoporotic fractures, but their cardiovascular safety remains unclear. We conducted a cis-Mendelian randomisation analysis to estimate the causal effect of sclerostin levels on cardiovascular risk factors. We meta-analysed three GWAS of sclerostin levels including 49,568 Europeans and selected 2 SNPs to be used as instruments. We included heel bone mineral density and hip fracture risk as positive control outcomes. Public GWAS and UK Biobank patient-level data were used for the study outcomes, which include cardiovascular events, risk factors, and biomarkers. Lower sclerostin levels were associated with higher bone mineral density and 85% reduction in hip fracture risk. However, genetically predicted lower sclerostin levels led to 25–85% excess coronary artery disease risk, 40% to 60% increased risk of type 2 diabetes, and worse cardiovascular biomarkers values, including higher triglycerides, and decreased HDL cholesterol levels. Results also suggest a potential (but borderline) association with increased risk of myocardial infarction. Our study provides genetic evidence of a causal relationship between reduced levels of sclerostin and improved bone health and fracture protection, but increased risk of cardiovascular events and risk factors.