PER1 rs3027172 genotype interacts with early life stress to predict problematic alcohol use, but not reward-related ventral striatum activity

PER1 rs3027172 genotype interacts with early life stress to predict problematic alcohol use, but not reward-related ventral striatum activity

Increasing evidence suggests that the circadian and stress regulatory systems contribute to alcohol use disorder (AUD) risk, which may partially arise through effects on reward-related neural function. The C allele of the PER1 rs3027172 single nucleotide polymorphism reduces PER1 expression in cells...

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Bibliographic Details
Main Authors: David eBaranger, Chloe eIfrah, Aric A Prather, Caitlin E Carey, Nadia S Corral-Frias, Emily D Conley, Ahmad R Hariri, Ryan eBogdan
Format: Article
Language:English
Published: Frontiers Media S.A. 2016-03-01
Series:Frontiers in Psychology
Subjects:
stress
alcohol
circadian
ventral striatum
early life stress
GxE
Online Access:http://journal.frontiersin.org/Journal/10.3389/fpsyg.2016.00464/full
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spelling doaj-fa1aabb11d1e468baa6b52f78faa67222020-11-24T21:40:15ZengFrontiers Media S.A.Frontiers in Psychology1664-10782016-03-01710.3389/fpsyg.2016.00464179306PER1 rs3027172 genotype interacts with early life stress to predict problematic alcohol use, but not reward-related ventral striatum activityDavid eBaranger0Chloe eIfrah1Aric A Prather2Caitlin E Carey3Nadia S Corral-Frias4Emily D Conley5Ahmad R Hariri6Ryan eBogdan7Washington University in St. LouisWashington University in St. LouisUniversity of California, San FranciscoWashington University in St. LouisWashington University in St. Louis23andMeDuke UniversityWashington University in St. LouisIncreasing evidence suggests that the circadian and stress regulatory systems contribute to alcohol use disorder (AUD) risk, which may partially arise through effects on reward-related neural function. The C allele of the PER1 rs3027172 single nucleotide polymorphism reduces PER1 expression in cells incubated with cortisol and has been associated with increased risk for adult AUD and problematic drinking among adolescents exposed to high levels of familial psychosocial adversity. Using data from undergraduate students who completed the ongoing Duke Neurogenetics Study (n=665), we tested whether exposure to early life stress (ELS; Childhood Trauma Questionnaire) moderates the association between rs3027172 genotype and later problematic alcohol use (Alcohol Use Disorders Identification Test) as well as ventral striatum (VS) reactivity to reward (card-guessing task while functional magnetic resonance imaging data were acquired). Initial analyses found that PER1 rs3027172 genotype interacted with ELS to predict both problematic drinking and VS reactivity; minor C allele carriers, who were also exposed to elevated ELS reported greater problematic drinking and exhibited greater ventral striatum reactivity to reward-related stimuli. When gene x covariate and environment x covariate interactions were controlled for, the interaction predicting problematic alcohol use remained significant (p<0.05, corrected) while the interaction predicting VS reactivity was no longer significant. These results extend our understanding of relationships between PER1 genotype, early life stress, and problematic alcohol use, and serve as a cautionary tale on the importance of controlling for potential confounders in studies of moderation including gene x environment interactions.http://journal.frontiersin.org/Journal/10.3389/fpsyg.2016.00464/fullstressalcoholcircadianventral striatumearly life stressGxE
collection DOAJ
language English
format Article
sources DOAJ
author David eBaranger
Chloe eIfrah
Aric A Prather
Caitlin E Carey
Nadia S Corral-Frias
Emily D Conley
Ahmad R Hariri
Ryan eBogdan
spellingShingle David eBaranger
Chloe eIfrah
Aric A Prather
Caitlin E Carey
Nadia S Corral-Frias
Emily D Conley
Ahmad R Hariri
Ryan eBogdan
PER1 rs3027172 genotype interacts with early life stress to predict problematic alcohol use, but not reward-related ventral striatum activity
Frontiers in Psychology
stress
alcohol
circadian
ventral striatum
early life stress
GxE
author_facet David eBaranger
Chloe eIfrah
Aric A Prather
Caitlin E Carey
Nadia S Corral-Frias
Emily D Conley
Ahmad R Hariri
Ryan eBogdan
author_sort David eBaranger
title PER1 rs3027172 genotype interacts with early life stress to predict problematic alcohol use, but not reward-related ventral striatum activity
title_short PER1 rs3027172 genotype interacts with early life stress to predict problematic alcohol use, but not reward-related ventral striatum activity
title_full PER1 rs3027172 genotype interacts with early life stress to predict problematic alcohol use, but not reward-related ventral striatum activity
title_fullStr PER1 rs3027172 genotype interacts with early life stress to predict problematic alcohol use, but not reward-related ventral striatum activity
title_full_unstemmed PER1 rs3027172 genotype interacts with early life stress to predict problematic alcohol use, but not reward-related ventral striatum activity
title_sort per1 rs3027172 genotype interacts with early life stress to predict problematic alcohol use, but not reward-related ventral striatum activity
publisher Frontiers Media S.A.
series Frontiers in Psychology
issn 1664-1078
publishDate 2016-03-01
description Increasing evidence suggests that the circadian and stress regulatory systems contribute to alcohol use disorder (AUD) risk, which may partially arise through effects on reward-related neural function. The C allele of the PER1 rs3027172 single nucleotide polymorphism reduces PER1 expression in cells incubated with cortisol and has been associated with increased risk for adult AUD and problematic drinking among adolescents exposed to high levels of familial psychosocial adversity. Using data from undergraduate students who completed the ongoing Duke Neurogenetics Study (n=665), we tested whether exposure to early life stress (ELS; Childhood Trauma Questionnaire) moderates the association between rs3027172 genotype and later problematic alcohol use (Alcohol Use Disorders Identification Test) as well as ventral striatum (VS) reactivity to reward (card-guessing task while functional magnetic resonance imaging data were acquired). Initial analyses found that PER1 rs3027172 genotype interacted with ELS to predict both problematic drinking and VS reactivity; minor C allele carriers, who were also exposed to elevated ELS reported greater problematic drinking and exhibited greater ventral striatum reactivity to reward-related stimuli. When gene x covariate and environment x covariate interactions were controlled for, the interaction predicting problematic alcohol use remained significant (p<0.05, corrected) while the interaction predicting VS reactivity was no longer significant. These results extend our understanding of relationships between PER1 genotype, early life stress, and problematic alcohol use, and serve as a cautionary tale on the importance of controlling for potential confounders in studies of moderation including gene x environment interactions.
topic stress
alcohol
circadian
ventral striatum
early life stress
GxE
url http://journal.frontiersin.org/Journal/10.3389/fpsyg.2016.00464/full
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