Persistent DNA methylation changes associated with prenatal mercury exposure and cognitive performance during childhood

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作者
Andres Cardenas
Sheryl L. Rifas-Shiman
Golareh Agha
Marie-France Hivert
Augusto A. Litonjua
Dawn L. DeMeo
Xihong Lin
Chitra J. Amarasiriwardena
Emily Oken
Matthew W. Gillman
Andrea A. Baccarelli
机构
[1] Harvard T.H. Chan School of Public Health,Department of Environmental Health
[2] Harvard Medical School and Harvard Pilgrim Health Care Institute,Obesity Prevention Program, Department of Population Medicine
[3] Brigham and Women’s Hospital,Channing Division of Network Medicine, Department of Medicine
[4] Harvard T.H. Chan School of Public Health,Department of Biostatistics
[5] Icahn School of Medicine at Mount Sinai,Department of Preventive Medicine
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Scientific Reports | / 7卷
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摘要
Prenatal exposure to mercury, a known neurotoxic metal, is associated with lower cognitive performance during childhood. Disruption of fetal epigenetic programming could explain mercury’s neurodevelopmental effects. We screened for epigenome-wide methylation differences associated with maternal prenatal blood mercury levels in 321 cord blood DNA samples and examined the persistence of these alterations during early (n = 75; 2.9–4.9 years) and mid-childhood (n = 291; 6.7–10.5 years). Among males, prenatal mercury levels were associated with lower regional cord blood DNA methylation at the Paraoxonase 1 gene (PON1) that persisted in early childhood and was attenuated in mid-childhood blood. Cord blood methylation at the PON1 locus predicted lower cognitive test scores measured during early childhood. Methylation at the PON1 locus was associated with PON1 expression in an independent set of cord blood samples. The observed persistent epigenetic disruption of the PON1 gene may modulate mercury toxicity in humans and might serve as a biomarker of exposure and disease susceptibility.
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