| Literature DB >> 34274109 |
Robert Hitzemann1, Susan E Bergeson2, Ari E Berman3, Jason A Bubier3, Elissa J Chesler3, Deborah A Finn4, Matthew Hein2, Paula Hoffman5, Andrew Holmes6, Brent R Kisby2, Denesa Lockwood7, Kerrie H Lodowski2, Michelle McManus2, Julie A Owen2, Angela R Ozburn4, Praneetha Panthagani2, Igor Ponomarev2, Laura Saba8, Boris Tabakoff8, Aashlesha Walchale2, Robert W Williams9, Tamara J Phillips4.
Abstract
There is compelling evidence that sex and gender have crucial roles in excessive alcohol (ethanol) consumption. Here, we review some of the data from the perspective of brain transcriptional differences between males and females, focusing on rodent animal models. A key emerging transcriptional feature is the role of neuroimmune processes. Microglia are the resident neuroimmune cells in the brain and exhibit substantial functional differences between males and females. Selective breeding for binge ethanol consumption and the impacts of chronic ethanol consumption and withdrawal from chronic ethanol exposure all demonstrate sex-dependent neuroimmune signatures. A focus is on resolving sex-dependent differences in transcriptional responses to ethanol at the neurocircuitry level. Sex-dependent transcriptional differences are found in the extended amygdala and the nucleus accumbens. Telescoping of ethanol consumption is found in some, but not all, studies to be more prevalent in females. Recent transcriptional studies suggest that some sex differences may be due to female-dependent remodeling of the primary cilium. An interesting theme appears to be developing: at least from the animal model perspective, even when males and females are phenotypically similar, they differ significantly at the level of the transcriptome.Entities:
Keywords: Binge; Ethanol; Functional genomics; Neural circuitry; Neuroimmune function; Therapeutics
Mesh:
Year: 2021 PMID: 34274109 PMCID: PMC8558111 DOI: 10.1016/j.biopsych.2021.04.016
Source DB: PubMed Journal: Biol Psychiatry ISSN: 0006-3223 Impact factor: 12.810