| Literature DB >> 28247455 |
Ovidiu D Iancu1, Alexander Colville1, Nicole A R Walter1, Priscila Darakjian1, Denesa L Oberbeck1, James B Daunais2, Christina L Zheng1, Robert P Searles1, Shannon K McWeeney1, Kathleen A Grant1, Robert Hitzemann1.
Abstract
This is the first description of the relationship between chronic ethanol self-administration and the brain transcriptome in a non-human primate (rhesus macaque). Thirty-one male animals self-administered ethanol on a daily basis for over 12 months. Gene transcription was quantified with RNA-Seq in the central nucleus of the amygdala (CeA) and cortical Area 32. We constructed coexpression and cosplicing networks, and we identified areas of preservation and areas of differentiation between regions and network types. Correlations between intake and transcription included largely distinct gene sets and annotation categories across brain regions and between expression and splicing; positive and negative correlations were also associated with distinct annotation groups. Membrane, synaptic and splicing annotation categories were over-represented in the modules (gene clusters) enriched in positive correlations (CeA); our cosplicing analysis further identified the genes affected only at the exon inclusion level. In the CeA coexpression network, we identified Rab6b, Cdk18 and Igsf21 among the intake-correlated hubs, while in the Area 32, we identified a distinct hub set that included Ppp3r1 and Myeov2. Overall, the data illustrate that excessive ethanol self-administration is associated with broad expression and splicing mechanisms that involve membrane and synapse genes.Entities:
Keywords: RNA-Seq; addiction; cosplicing; ethanol; network analysis; non-human primate
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Year: 2017 PMID: 28247455 PMCID: PMC5671907 DOI: 10.1111/adb.12501
Source DB: PubMed Journal: Addict Biol ISSN: 1355-6215 Impact factor: 4.280