Epigenetics (Dec 2024)

Identification and functional characterisation of DNA methylation differences between East- and West-originating Finns

  • Joanna Ciantar,
  • Saara Marttila,
  • Sonja Rajić,
  • Daria Kostiniuk,
  • Pashupati P Mishra,
  • Leo-Pekka Lyytikäinen,
  • Nina Mononen,
  • Marcus E Kleber,
  • Winfried März,
  • Mika Kähönen,
  • Olli Raitakari,
  • Terho Lehtimäki,
  • Emma Raitoharju

DOI
https://doi.org/10.1080/15592294.2024.2397297
Journal volume & issue
Vol. 19, no. 1

Abstract

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Eastern and Western Finns show a striking difference in coronary heart disease-related mortality; genetics is a known contributor for this discrepancy. Here, we discuss the potential role of DNA methylation in mediating the discrepancy in cardiometabolic disease-risk phenotypes between the sub-populations. We used data from the Young Finns Study (n = 969) to compare the genome-wide DNA methylation levels of East- and West-originating Finns. We identified 21 differentially methylated loci (FDR 2.5%) and 7 regions (smoothed FDR < 0.05; CpGs ≥ 5). Methylation at all loci and regions associates with genetic variants (p < 5 × 10−8). Independently of genetics, methylation at 11 loci and 4 regions associates with transcript expression, including genes encoding zinc finger proteins. Similarly, methylation at 5 loci and 4 regions associates with cardiometabolic disease-risk phenotypes including triglycerides, glucose, cholesterol, as well as insulin treatment. This analysis was also performed in LURIC (n = 2371), a German cardiovascular patient cohort, and results replicated for the association of methylation at cg26740318 and DMR_11p15 with diabetes-related phenotypes and methylation at DMR_22q13 with triglyceride levels. Our results indicate that DNA methylation differences between East and West Finns may have a functional role in mediating the cardiometabolic disease discrepancy between the sub-populations.

Keywords