Opposite Epigenetic Associations With Alcohol Use and Exercise Intervention

Jiayu Chen; Kent E. Hutchison; Angela D. Bryan; Francesca M. Filbey; Vince D. Calhoun; Eric D. Claus; Dongdong Lin; Jing Sui; Yuhui Du; Jingyu Liu

doi:10.3389/fpsyt.2018.00594

Opposite Epigenetic Associations With Alcohol Use and Exercise Intervention

Jiayu Chen, Kent E. Hutchison, Angela D. Bryan, Francesca M. Filbey, Vince D. Calhoun, Eric D. Claus, Dongdong Lin, Jing Sui, Yuhui Du, Jingyu Liu

School of Medicine

Research output: Contribution to journal › Article › peer-review

4 Scopus citations

Abstract

Alcohol use disorder (AUD) is a devastating public health problem in which both genetic and environmental factors play a role. Growing evidence supports that epigenetic regulation is one major mechanism in neuroadaptation that contributes to development of AUD. Meanwhile, epigenetic patterns can be modified by various stimuli including exercise. Thus, it is an intriguing question whether exercise can lead to methylation changes that are opposite to those related to drinking. We herein conducted a comparative study to explore this issue. Three cohorts were profiled for DNA methylation (DNAm), including a longitudinal exercise intervention cohort (53 healthy participants profiled at baseline and after a 12-months exercise intervention), a cross-sectional case-control cohort (81 hazardous drinkers and 81 healthy controls matched in age and sex), and a cross-sectional binge drinking cohort (281 drinkers). We identified 906 methylation sites showing significant DNAm differences between drinkers and controls in the case-control cohort, as well as, associations with drinking behavior in the drinking cohort. In parallel, 341 sites were identified for significant DNAm alterations between baseline and follow-up in the exercise cohort. Thirty-two sites overlapped between these two set of findings, of which 15 sites showed opposite directions of DNAm associations between exercise and drinking. Annotated genes of these 15 sites were enriched in signaling pathways related to synaptic plasticity. In addition, the identified methylation sites significantly associated with impaired control over drinking, suggesting relevance to neural function. Collectively, the current findings provide preliminary evidence that exercise has the potential to partially reverse DNAm differences associated with drinking at some CpG sites, motivating rigorously designed longitudinal studies to better characterize epigenetic effects with respect to prevention and intervention of AUD.

Original language	English (US)
Article number	594
Journal	Frontiers in Psychiatry
Volume	9
DOIs	https://doi.org/10.3389/fpsyt.2018.00594
State	Published - Nov 15 2018

Keywords

alcohol
exercise
impaired control
methylation
synaptic plasticity

ASJC Scopus subject areas

Psychiatry and Mental health

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10.3389/fpsyt.2018.00594

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@article{20f013a1ee8640ba896985712aa6d3bb,

title = "Opposite Epigenetic Associations With Alcohol Use and Exercise Intervention",

abstract = "Alcohol use disorder (AUD) is a devastating public health problem in which both genetic and environmental factors play a role. Growing evidence supports that epigenetic regulation is one major mechanism in neuroadaptation that contributes to development of AUD. Meanwhile, epigenetic patterns can be modified by various stimuli including exercise. Thus, it is an intriguing question whether exercise can lead to methylation changes that are opposite to those related to drinking. We herein conducted a comparative study to explore this issue. Three cohorts were profiled for DNA methylation (DNAm), including a longitudinal exercise intervention cohort (53 healthy participants profiled at baseline and after a 12-months exercise intervention), a cross-sectional case-control cohort (81 hazardous drinkers and 81 healthy controls matched in age and sex), and a cross-sectional binge drinking cohort (281 drinkers). We identified 906 methylation sites showing significant DNAm differences between drinkers and controls in the case-control cohort, as well as, associations with drinking behavior in the drinking cohort. In parallel, 341 sites were identified for significant DNAm alterations between baseline and follow-up in the exercise cohort. Thirty-two sites overlapped between these two set of findings, of which 15 sites showed opposite directions of DNAm associations between exercise and drinking. Annotated genes of these 15 sites were enriched in signaling pathways related to synaptic plasticity. In addition, the identified methylation sites significantly associated with impaired control over drinking, suggesting relevance to neural function. Collectively, the current findings provide preliminary evidence that exercise has the potential to partially reverse DNAm differences associated with drinking at some CpG sites, motivating rigorously designed longitudinal studies to better characterize epigenetic effects with respect to prevention and intervention of AUD.",

keywords = "alcohol, exercise, impaired control, methylation, synaptic plasticity",

author = "Jiayu Chen and Hutchison, {Kent E.} and Bryan, {Angela D.} and Filbey, {Francesca M.} and Calhoun, {Vince D.} and Claus, {Eric D.} and Dongdong Lin and Jing Sui and Yuhui Du and Jingyu Liu",

note = "Publisher Copyright: {\textcopyright} Copyright {\textcopyright} 2018 Chen, Hutchison, Bryan, Filbey, Calhoun, Claus, Lin, Sui, Du and Liu.",

year = "2018",

month = nov,

day = "15",

doi = "10.3389/fpsyt.2018.00594",

language = "English (US)",

volume = "9",

journal = "Frontiers in Psychiatry",

issn = "1664-0640",

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TY - JOUR

T1 - Opposite Epigenetic Associations With Alcohol Use and Exercise Intervention

AU - Chen, Jiayu

AU - Hutchison, Kent E.

AU - Bryan, Angela D.

AU - Filbey, Francesca M.

AU - Calhoun, Vince D.

AU - Claus, Eric D.

AU - Lin, Dongdong

AU - Sui, Jing

AU - Du, Yuhui

AU - Liu, Jingyu

PY - 2018/11/15

Y1 - 2018/11/15

N2 - Alcohol use disorder (AUD) is a devastating public health problem in which both genetic and environmental factors play a role. Growing evidence supports that epigenetic regulation is one major mechanism in neuroadaptation that contributes to development of AUD. Meanwhile, epigenetic patterns can be modified by various stimuli including exercise. Thus, it is an intriguing question whether exercise can lead to methylation changes that are opposite to those related to drinking. We herein conducted a comparative study to explore this issue. Three cohorts were profiled for DNA methylation (DNAm), including a longitudinal exercise intervention cohort (53 healthy participants profiled at baseline and after a 12-months exercise intervention), a cross-sectional case-control cohort (81 hazardous drinkers and 81 healthy controls matched in age and sex), and a cross-sectional binge drinking cohort (281 drinkers). We identified 906 methylation sites showing significant DNAm differences between drinkers and controls in the case-control cohort, as well as, associations with drinking behavior in the drinking cohort. In parallel, 341 sites were identified for significant DNAm alterations between baseline and follow-up in the exercise cohort. Thirty-two sites overlapped between these two set of findings, of which 15 sites showed opposite directions of DNAm associations between exercise and drinking. Annotated genes of these 15 sites were enriched in signaling pathways related to synaptic plasticity. In addition, the identified methylation sites significantly associated with impaired control over drinking, suggesting relevance to neural function. Collectively, the current findings provide preliminary evidence that exercise has the potential to partially reverse DNAm differences associated with drinking at some CpG sites, motivating rigorously designed longitudinal studies to better characterize epigenetic effects with respect to prevention and intervention of AUD.

AB - Alcohol use disorder (AUD) is a devastating public health problem in which both genetic and environmental factors play a role. Growing evidence supports that epigenetic regulation is one major mechanism in neuroadaptation that contributes to development of AUD. Meanwhile, epigenetic patterns can be modified by various stimuli including exercise. Thus, it is an intriguing question whether exercise can lead to methylation changes that are opposite to those related to drinking. We herein conducted a comparative study to explore this issue. Three cohorts were profiled for DNA methylation (DNAm), including a longitudinal exercise intervention cohort (53 healthy participants profiled at baseline and after a 12-months exercise intervention), a cross-sectional case-control cohort (81 hazardous drinkers and 81 healthy controls matched in age and sex), and a cross-sectional binge drinking cohort (281 drinkers). We identified 906 methylation sites showing significant DNAm differences between drinkers and controls in the case-control cohort, as well as, associations with drinking behavior in the drinking cohort. In parallel, 341 sites were identified for significant DNAm alterations between baseline and follow-up in the exercise cohort. Thirty-two sites overlapped between these two set of findings, of which 15 sites showed opposite directions of DNAm associations between exercise and drinking. Annotated genes of these 15 sites were enriched in signaling pathways related to synaptic plasticity. In addition, the identified methylation sites significantly associated with impaired control over drinking, suggesting relevance to neural function. Collectively, the current findings provide preliminary evidence that exercise has the potential to partially reverse DNAm differences associated with drinking at some CpG sites, motivating rigorously designed longitudinal studies to better characterize epigenetic effects with respect to prevention and intervention of AUD.

KW - alcohol

KW - exercise

KW - impaired control

KW - methylation

KW - synaptic plasticity

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JO - Frontiers in Psychiatry

JF - Frontiers in Psychiatry

M1 - 594

ER -

Opposite Epigenetic Associations With Alcohol Use and Exercise Intervention

Abstract

Keywords

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