Placental DNA methylation levels at CYP2E1 and IRS2 are associated with child outcome in a prospective autism study

Author:

Zhu YihuiORCID,Mordaunt Charles E.ORCID,Yasui Dag H.,Marathe Ria,Coulson Rochelle L.,Dunaway Keith W.,Walker Cheryl K.,Ozonoff Sally,Hertz-Picciotto Irva,Schmidt Rebecca J.,LaSalle Janine M.

Abstract

AbstractDNA methylation acts at the interface of genetic and environmental factors relevant for autism spectrum disorder (ASD). Placenta, normally discarded at birth, is a potentially rich source of DNA methylation patterns predictive of ASD in the child. Here, we performed whole methylome analyses of placentas from a prospective study of high-risk pregnancies. 400 differentially methylated regions (DMRs) discriminated placentas stored from children later diagnosed with ASD compared to typical controls. These ASD DMRs were significantly enriched at promoters, mapped to 596 genes functionally enriched in neuronal development, and overlapped genetic ASD risk. ASD DMRs at CYP2E1 and IRS2 reached genome-wide significance, replicated by pyrosequencing, and correlated with expression. Methylation at CYP2E1 associated with both ASD diagnosis and cis genotype, while methylation at IRS2 was unaffected by cis genotype but modified by preconceptional maternal prenatal vitamin use. This study therefore identified two potentially useful early epigenetic markers for ASD in placenta.

Publisher

Cold Spring Harbor Laboratory

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