Contributions of prenatal risk factors and neonatal epigenetics to cognitive outcome in children born very preterm.

Creator(s)

Marie Camerota
Barry M. Lester
Elisabeth C. McGowan
Brian S. Carter, Children's Mercy HospitalFollow
Jennifer Check
Lynne M. Dansereau
Sheri A. DellaGrotta
Jennifer B. Helderman
Julie A. Hofheimer
Cynthia M. Loncar
Charles R. Neal
T Michael O'Shea
Steven L. Pastyrnak
Lynne M. Smith
Sarina Abrishamcar
Anke Hüls
Carmen J. Marsit
Todd M. Everson

Document Type

Article

Publication Date

9-2024

Identifier

DOI: 10.1037/dev0001709

Abstract

Children born less than 30 weeks gestational age (GA) are at high risk for neurodevelopmental delay compared to term peers. Prenatal risk factors and neonatal epigenetics could help identify preterm children at highest risk for poor cognitive outcomes. We aimed to understand the associations among cumulative prenatal risk, neonatal DNA methylation, and child cognitive ability at age 3 years, including whether DNA methylation mediates the association between prenatal risk and cognitive ability. We studied 379 neonates (54% male) born less than 30 weeks GA who had DNA methylation measured at neonatal intensive care unit discharge along with 3-year follow-up data. Cumulative prenatal risk was calculated from 24 risk factors obtained from maternal report and medical record and epigenome-wide neonatal DNA methylation was assayed from buccal swabs. At 3-year follow-up, child cognitive ability was assessed using the Bayley Scales of Infant and Toddler Development (third edition). Cumulative prenatal risk and DNA methylation at two cytosine-phosphate-guanines (CpGs) were uniquely associated with child cognitive ability. Using high-dimensional mediation analysis, we also identified differential methylation of 309 CpGs that mediated the association between cumulative prenatal risk and child cognitive ability. Many of the associated CpGs were located in genes (TNS3, TRAPPC4, MAD1L1, APBB2, DIP2C, TRAPPC9, DRD2) that have previously been associated with prenatal exposures and/or neurodevelopmental phenotypes. Our findings suggest a role for both prenatal risk factors and DNA methylation in explaining outcomes for children born preterm and suggest we should further study DNA methylation as a potential mechanism underlying the association between prenatal risk and child neurodevelopment.

Journal Title

Developmental psychology

Volume

60

Issue

9

First Page

1606

Last Page

1619

MeSH Keywords

Humans; Female; Male; DNA Methylation; Risk Factors; Child, Preschool; Infant, Newborn; Epigenesis, Genetic; Infant, Extremely Premature; Pregnancy; Cognition; Child Development; Follow-Up Studies; Prenatal Exposure Delayed Effects

Keywords

DNA Methylation; Risk Factors; Genetic Epigenesis; Pregnancy; Cognition; Child Development; Follow-Up Studies; Prenatal Exposure Delayed Effects

Comments

Grants and funding

• NH/NIH HHS/United States
• MH/NIMH NIH HHS/United States
• NH/NIH HHS/United States
• MH/NIMH NIH HHS/United States

Recommended Citation

Camerota M, Lester BM, McGowan EC, et al. Contributions of prenatal risk factors and neonatal epigenetics to cognitive outcome in children born very preterm. Dev Psychol. 2024;60(9):1606-1619. doi:10.1037/dev0001709