Epigenetics (Mar 2022)

Maternal blood metal concentrations and whole blood DNA methylation during pregnancy in the Early Autism Risk Longitudinal Investigation (EARLI)

  • Max T. Aung,
  • Kelly M. Bakulski,
  • Jason I. Feinberg,
  • John F. Dou,
  • John D. Meeker,
  • Bhramar Mukherjee,
  • Rita Loch-Caruso,
  • Christine Ladd-Acosta,
  • Heather E. Volk,
  • Lisa A. Croen,
  • Irva Hertz-Picciotto,
  • Craig J. Newschaffer,
  • M. Daniele Fallin

DOI
https://doi.org/10.1080/15592294.2021.1897059
Journal volume & issue
Vol. 17, no. 3
pp. 253 – 268

Abstract

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The maternal epigenome may be responsive to prenatal metals exposures. We tested whether metals are associated with concurrent differential maternal whole blood DNA methylation. In the Early Autism Risk Longitudinal Investigation cohort, we measured first or second trimester maternal blood metals concentrations (cadmium, lead, mercury, manganese, and selenium) using inductively coupled plasma mass spectrometry. DNA methylation in maternal whole blood was measured on the Illumina 450 K array. A subset sample of 97 women had both measures available for analysis, all of whom did not report smoking during pregnancy. Linear regression was used to test for site-specific associations between individual metals and DNA methylation, adjusting for cell type composition and confounding variables. Discovery gene ontology analysis was conducted on the top 1,000 sites associated with each metal. We observed hypermethylation at 11 DNA methylation sites associated with lead (FDR False Discovery Rate q-value 0.86). DNA methylation sites associated with lead and manganese may be potential biomarkers of exposure or implicate downstream gene pathways.

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