Abstract

Exposure to adverse rearing environments including institutional deprivation and severe childhood abuse is associated with an increased risk for mental and physical health problems across the lifespan. Although the mechanisms mediating these effects are not known, recent work in rodent models suggests that epigenetic processes may be involved. We studied the impact of severe early-life adversity on epigenetic variation in a sample of adolescents adopted from the severely depriving orphanages of the Romanian communist era in the 1980s. We quantified buccal cell DNA methylation at ~400 000 sites across the genome in Romanian adoptees exposed to either extended (6–43 months; n=16) or limited duration (<6 months; n=17) of severe early-life deprivation, in addition to a matched sample of UK adoptees (n=16) not exposed to severe deprivation. Although no probe-wise differences remained significant after controlling for the number of probes tested, we identified an exposure-associated differentially methylated region (DMR) spanning nine sequential CpG sites in the promoter-regulatory region of the cytochrome P450 2E1 gene (CYP2E1) on chromosome 10 (corrected P=2.98 × 10−5). Elevated DNA methylation across this region was also associated with deprivation-related clinical markers of impaired social cognition. Our data suggest that environmental insults of sufficient biological impact during early development are associated with long-lasting epigenetic changes, potentially reflecting a biological mechanism linking the effects of early-life adversity to cognitive and neurobiological phenotypes.

Highlights

  • Brain circuits underpinning cognition and socioemotional functioning are sculpted by social experiences during early life.[1]

  • Using comb-p to identify differentially methylated region (DMR) for sociocognitive and intellectual impairments, we found that DNA methylation across the nine CpG sites in the deprivation-associated cytochrome P450 2E1 gene (CYP2E1) DMR on chromosome

  • Using samples from a unique ‘natural experiment’ following children exposed to prolonged severe institutional deprivation, we provide evidence for significant alterations in DNA methylation in response to severe early-life social adversity in humans

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Summary

Introduction

Brain circuits underpinning cognition and socioemotional functioning are sculpted by social experiences during early life.[1]. There is some evidence for similar epigenetic alterations in response to various environmental stressors in humans, including prenatal exposure to famine,[6] psychosocial stress during infancy and pre-school years,[7] early-life socioeconomic status,[8] and childhood abuse.[4,9,10,11] direct replication of the effects observed in experimental animal models in humans remains challenging for a number of reasons.

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