4.6 Article

Prenatal Exposures to Common Phthalates and Prevalent Phthalate Alternatives and Infant DNA Methylation at Birth

期刊

FRONTIERS IN GENETICS
卷 13, 期 -, 页码 -

出版社

FRONTIERS MEDIA SA
DOI: 10.3389/fgene.2022.793278

关键词

phthalates; DNA methylation; epigenetics; development; DOHAD

资金

  1. National Institutes of Health (NIH) [UG3OD023285, UH3OD023285, R01ES017500, P01ES022844, P30ES017885, 1UG3 OD023285-01, R35 ES031686, P30ES020957]
  2. National Institute of Environmental Health Sciences (NIEHS) Children's Health Exposure Analysis Resource (CHEAR) program [U2CES026553]
  3. US Environmental Protection Agency (EPA) [RD83543601]
  4. Michigan Health Endowment Fund [G-1608-140432, R-1605-140007]
  5. Michigan State University Center for Research in Autism, Intellectual and Neurodevelopmental Disabilities (C-RAIND)
  6. NIEHS [T32ES007062]

向作者/读者索取更多资源

This study investigated the impact of prenatal exposure to phthalates on fetal DNA methylation and found sex-specific alterations in infant DNA methylation.
Phthalates are a diverse group of chemicals used in consumer products. Because they are so widespread, exposure to these compounds is nearly unavoidable. Recently, growing scientific consensus has suggested that phthalates produce health effects in developing infants and children. These effects may be mediated through mechanisms related to the epigenome, the constellation of mitotically heritable chemical marks and small compounds that guide transcription and translation. The present study examined the relationship between prenatal, first-trimester exposure of seven phthalates and epigenetics in two pregnancy cohorts (n = 262) to investigate sex-specific alterations in infant blood DNA methylation at birth (cord blood or neonatal blood spots). Prenatal exposure to several phthalates was suggestive of association with altered DNA methylation at 4 loci in males (all related to sigma DEHP) and 4 loci in females (1 related to sigma DiNP; 2 related to BBzP; and 1 related to MCPP) at a cutoff of q < 0.2. Additionally, a subset of dyads (n = 79) was used to interrogate the relationships between two compounds increasingly used as substitutions for common phthalates (sigma DINCH and sigma DEHTP) and cord blood DNA methylation. sigma DINCH, but not sigma DEHTP, was suggestive of association with DNA methylation (q < 0.2). Together, these results demonstrate that prenatal exposure to both classically used phthalate metabolites and their newer alternatives is associated with sex-specific infant DNA methylation. Research and regulatory actions regarding this chemical class should consider the developmental health effects of these compounds and aim to avoid regrettable substitution scenarios in the present and future.

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