4.5 Article

DNA methylation in neonates born to women receiving psychiatric care

期刊

EPIGENETICS
卷 7, 期 4, 页码 409-414

出版社

TAYLOR & FRANCIS INC
DOI: 10.4161/epi.19551

关键词

DNA methylation; prenatal exposures; antidepressants; depressive symptoms; HumanMethylation27 BeadChip; Infinium

资金

  1. Specialized Center for Research [P50 MH 68036]
  2. Translational Research Center in Behavioral Sciences (TRCBS) [P50 MH077928]
  3. Emory Biomarker Service Center
  4. NIH
  5. AFSP
  6. Schering Plough Pharmaceuticals
  7. NARSAD
  8. Wyeth
  9. BMS
  10. Cyberonics
  11. Eli Lilly
  12. Forest
  13. Janssen
  14. Novartis
  15. GSK
  16. Pfizer
  17. [RC1 MH088609]
  18. [MH085806]

向作者/读者索取更多资源

Prenatal exposure both to maternal psychiatric illness and psychiatric medication has been linked with adverse child outcomes that affect physiological, emotional and psychiatric development. Studies suggest that epigenetic mechanisms, such as DNA methylation, may facilitate these effects. In this report, we explore the association between maternal psychiatric illness and treatment during pregnancy and neonatal DNA methylation patterns in a prospectively-characterized clinical cohort of 201 dyads. Associations between the percent of umbilical cord blood DNA methylated at 27,578 CpG sites and maternal psychiatric diagnosis, symptoms and antidepressant use were evaluated by fitting a separate linear mixed effects model for each CpG site. There were no significant changes in neonatal DNA methylation attributable to maternal psychiatric diagnosis or depressive symptoms during pregnancy. Exposure to an antidepressant medication was associated with differential methylation of CpG sites in TNFRSF21 and CHRNA2 (false discovery rate < 0.05), but the average difference in methylation for both CpG sites was less than 3% between each group. The results were not specific to type of antidepressant or duration of the exposure. This study suggests that there are no large effects of maternal psychiatric illness, depressive symptoms or prenatal exposure to antidepressants on neonatal DNA methylation. Delineation of the influence of maternal psychiatric illness and pharmacological exposures on the developing fetuses has critical implications for clinical care during pregnancy.

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