GeneSet Information

Tier III GS407721 • Blood gene expression signatures of chronic intermittent ethanol consumption in mice in females q-value

DESCRIPTION:

Alcohol Use Disorder (AUD) is a chronic, relapsing syndrome diagnosed by a heteroge- neous set of behavioral signs and symptoms. There are no laboratory tests that provide direct objective evidence for diagnosis. Microarray and RNA-Seq technologies enable genome-wide transcriptome profiling at low costs and provide an opportunity to identify bio- markers to facilitate diagnosis, prognosis, and treatment of patients. However, access to brain tissue in living patients is not possible. Blood contains cellular and extracellular RNAs that provide disease-relevant information for some brain diseases. We hypothesized that blood gene expression profiles can be used to diagnose AUD. We profiled brain (prefrontal cortex, amygdala, and hypothalamus) and blood gene expression levels in C57BL/6J mice using RNA-seq one week after chronic intermittent ethanol (CIE) exposure, a mouse model of alcohol dependence. We found a high degree of preservation (rho range: [0.50, 0.67]) between blood and brain transcript levels. There was small overlap between blood and brain DEGs, and considerable overlap of gene networks perturbed after CIE related to cell- cell signaling (e.g., GABA and glutamate receptor signaling), immune responses (e.g., anti- gen presentation), and protein processing / mitochondrial functioning (e.g., ubiquitination, oxidative phosphorylation). Blood gene expression data were used to train classifiers (logis- tic regression, random forest, and partial least squares discriminant analysis), which were highly accurate at predicting alcohol dependence status (maximum AUC: 90.1%). These results suggest that gene expression profiles from peripheral blood samples contain a bio- logical signature of alcohol dependence that can discriminate between CIE and Air subjects.

LABEL:

Alcohol blood gene expression in females q-value

SCORE TYPE:

Q-Value

DATE ADDED:

2023-11-08

DATE UPDATED:

2024-04-25

SPECIES:

AUTHORS:

Laura B Ferguson, Amanda J Roberts, R Dayne Mayfield, Robert O Messing

TITLE:

Blood and brain gene expression signatures of chronic intermittent ethanol consumption in mice.

JOURNAL:

PLoS computational biology Feb 2022, Vol 18, pp. e1009800

ABSTRACT:

Alcohol Use Disorder (AUD) is a chronic, relapsing syndrome diagnosed by a heterogeneous set of behavioral signs and symptoms. There are no laboratory tests that provide direct objective evidence for diagnosis. Microarray and RNA-Seq technologies enable genome-wide transcriptome profiling at low costs and provide an opportunity to identify biomarkers to facilitate diagnosis, prognosis, and treatment of patients. However, access to brain tissue in living patients is not possible. Blood contains cellular and extracellular RNAs that provide disease-relevant information for some brain diseases. We hypothesized that blood gene expression profiles can be used to diagnose AUD. We profiled brain (prefrontal cortex, amygdala, and hypothalamus) and blood gene expression levels in C57BL/6J mice using RNA-seq one week after chronic intermittent ethanol (CIE) exposure, a mouse model of alcohol dependence. We found a high degree of preservation (rho range: [0.50, 0.67]) between blood and brain transcript levels. There was small overlap between blood and brain DEGs, and considerable overlap of gene networks perturbed after CIE related to cell-cell signaling (e.g., GABA and glutamate receptor signaling), immune responses (e.g., antigen presentation), and protein processing / mitochondrial functioning (e.g., ubiquitination, oxidative phosphorylation). Blood gene expression data were used to train classifiers (logistic regression, random forest, and partial least squares discriminant analysis), which were highly accurate at predicting alcohol dependence status (maximum AUC: 90.1%). These results suggest that gene expression profiles from peripheral blood samples contain a biological signature of alcohol dependence that can discriminate between CIE and Air subjects. PUBMED: 35176017
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Ubiquitination (D054875)
Gene Expression (D015870)
Oxidative Phosphorylation (D010085)
Ethanol (D000431)
cell-cell signaling (GO:0007267)
oxidative phosphorylation (GO:0006119)
protein processing (GO:0016485)
antigen processing and presentation (GO:0019882)
extracellular region (GO:0005576)
gene expression (GO:0010467)
phosphorylation (GO:0016310)
signaling (GO:0023052)
Transcriptomics (EDAM_topic:0203)
alcohol abuse (DOID:1574)
alcohol dependence (DOID:0050741)
transcription profiling by high throughput sequencing (EFO:0002770)
transcriptome (EFO:0004421)
RNA-seq assay (MMO:0000659)
high throughput transcription profiling by microarray (MMO:0000649)

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