GeneSet Information

Tier III GS407741 • Differential gene expression in the brain associated with Alcohol Binge Drinking in bed nucleus of the stria terminalis FC

DESCRIPTION:

Alcohol use disorder (AUD) is a complex psychiatric disorder with strong genetic and environmental risk factors. We studied the molecular perturbations underlying risky drinking behavior by measuring transcriptome changes across the neurocircuitry of addiction in a genetic mouse model of binge drinking. Sixteen generations of selective breeding for high blood alcohol levels after a binge drinking session produced global changes in brain gene expression in alcohol-naïve High Drinking in the Dark (HDID-1) mice. Using gene expression profiles to generate circuit-level hypotheses, we developed a systems approach that integrated regulation of gene coexpression networks across multiple brain regions, neuron-specific transcriptional signatures, and knowledgebase analytics. Whole-cell, voltage-clamp recordings from nucleus accumbens shell neurons projecting to the ventral tegmental area showed differential ethanol-induced plasticity in HDID-1 and control mice and provided support for one of the hypotheses. There were similarities in gene networks between HDID-1 mouse brains and postmortem brains of human alcoholics, suggesting that some gene expression patterns associated with high alcohol consumption are conserved across species. This study demonstrated the value of gene networks for data integration across biological modalities and species to study mechanisms of disease.

LABEL:

Alcohol gene expression in mice BNST FC

SCORE TYPE:

Effect

DATE ADDED:

2023-11-08

DATE UPDATED:

2024-04-25

SPECIES:

AUTHORS:

Laura B Ferguson, Lingling Zhang, Daniel Kircher, Shi Wang, R Dayne Mayfield, John C Crabbe, Richard A Morrisett, R Adron Harris, Igor Ponomarev

TITLE:

Dissecting Brain Networks Underlying Alcohol Binge Drinking Using a Systems Genomics Approach.

JOURNAL:

Molecular neurobiology Apr 2019, Vol 56, pp. 2791-2810

ABSTRACT:

Alcohol use disorder (AUD) is a complex psychiatric disorder with strong genetic and environmental risk factors. We studied the molecular perturbations underlying risky drinking behavior by measuring transcriptome changes across the neurocircuitry of addiction in a genetic mouse model of binge drinking. Sixteen generations of selective breeding for high blood alcohol levels after a binge drinking session produced global changes in brain gene expression in alcohol-naïve High Drinking in the Dark (HDID-1) mice. Using gene expression profiles to generate circuit-level hypotheses, we developed a systems approach that integrated regulation of gene coexpression networks across multiple brain regions, neuron-specific transcriptional signatures, and knowledgebase analytics. Whole-cell, voltage-clamp recordings from nucleus accumbens shell neurons projecting to the ventral tegmental area showed differential ethanol-induced plasticity in HDID-1 and control mice and provided support for one of the hypotheses. There were similarities in gene networks between HDID-1 mouse brains and postmortem brains of human alcoholics, suggesting that some gene expression patterns associated with high alcohol consumption are conserved across species. This study demonstrated the value of gene networks for data integration across biological modalities and species to study mechanisms of disease. PUBMED: 30062672
Find other GeneSets from this publication

Annotation Information

No sequence read archive data associated with this GeneSet.


Brain (D001921)
Disease (D004194)
Drinking (D004326)
Behavior (D001519)
Mice (D051379)
Gene Expression (D015870)
Drinking Behavior (D004327)
Breeding (D001947)
Neurons (D009474)
Risk Factors (D012307)
Risk (D012306)
Nucleus Accumbens (D009714)
Ventral Tegmental Area (D017557)
Cells (D002477)
Blood (D001769)
Alcoholics (D057229)
Ethanol (D000431)
blood (MA:0000059)
accumbens nucleus (MA:0000892)
brain (MA:0000168)
addiction (MP:0002555)
biological regulation (GO:0065007)
nucleus (GO:0005634)
drinking behavior (GO:0042756)
gene expression (GO:0010467)
behavior (GO:0007610)
Transcriptomics (EDAM_topic:0203)
Data (EDAM_data:0006)
Pathways, networks and models (EDAM_topic:0602)
Disease resources (EDAM_topic:0634)
pyraclofos (CHEBI:38876)
ethanol (CHEBI:16236)
alcohol (CHEBI:30879)
atomic nucleus (CHEBI:33252)
alcohol abuse (DOID:1574)
disease (DOID:4)
disease (EFO:0000408)
drinking behavior (EFO:0004315)
ventral (EFO:0001662)
mental or behavioural disorder (EFO:0000677)
obsolete_accumbens nucleus (EFO:0000906)
risk factor (EFO:0003919)
area (EFO:0001696)
alcohol drinking (EFO:0004329)
obsolete_ventral tegmental area (EFO:0001935)
control (EFO:0001461)
transcriptome (EFO:0004421)
sexual interaction trait (VT:0002566)
shell of nucleus accumbens (UBERON:0012171)
exoskeleton (UBERON:0006611)
brain (UBERON:0000955)
neural nucleus (UBERON:0000125)
ventral tegmental area (UBERON:0002691)
shell (UBERON:0006612)
nucleus accumbens (UBERON:0001882)
adult cerebral ganglion (UBERON:6110636)
blood (UBERON:0000178)

Gene List • 9459 Genes

Uploaded As Gene Symbol Homology Score Priority LinkOuts Emphasis  

Manage GeneSets

Analyze GeneSets

Manage Accounts

GeneWeaver Links

Policies


Supported by NIH R01 AA18776 jointly funded by NIAAA and NIDA, and JAX Center for Precision Genetics NIH U54 OD 020351