Targeting the Glucocorticoid Receptor Reduces Binge-Like Drinking in High Drinking in the Dark (HDID-1) Mice.

Antonia M Savarese Angela R Ozburn Pamela Metten Jason P Schlumbohm Wyatt R Hack Kathryn LeMoine Hazel Hunt Felix Hausch Michael Bauder John C Crabbe

Alcohol Clin Exp Res

Department of Behavioral Neuroscience, Portland Alcohol Research Center, Oregon Health & Science University, Portland, Oregon.

Published: May 2020

Chronic alcohol exposure can change how glucocorticoid receptors (GR) function in certain brain areas, leading to increased binge drinking problems, particularly in specially bred mice that tend to consume more alcohol.
In experiments, blocking GR with specific compounds led to a significant decrease in binge drinking and blood alcohol concentrations (BECs) in HDID-1 mice, but did not affect consumption in HS/NPT mice, indicating potential differences in GR sensitivity due to selective breeding.
Despite finding that GR antagonism did not intensify the aversive reactions to alcohol in conditioned taste or place aversion tests, the results highlight the complex relationship between GR function and alcohol intake behaviors, warranting further investigation into selective

Background: Chronic alcohol exposure can alter glucocorticoid receptor (GR) function in some brain areas that promotes escalated and compulsive-like alcohol intake. GR antagonism can prevent dependence-induced escalation in drinking, but very little is known about the role of GR in regulating high-risk nondependent alcohol intake. Here, we investigate the role of GR in regulating binge-like drinking and aversive responses to alcohol in the High Drinking in the Dark (HDID-1) mice, which have been selectively bred for high blood ethanol (EtOH) concentrations (BECs) in the Drinking in the Dark (DID) test, and in their founder line, the HS/NPT.

Methods: In separate experiments, male and female HDID-1 mice were administered one of several compounds that inhibited GR or its negative regulator, FKBP51 (mifepristone [12.5, 25, 50, 100 mg/kg], CORT113176 [20, 40, 80 mg/kg], and SAFit2 [10, 20, 40 mg/kg]) during a 2-day DID task. EtOH consumption and BECs were measured. EtOH conditioned taste and place aversion (CTA and CPA, respectively) were measured in separate HDID-1 mice after mifepristone administration to assess GR's role in regulating the conditioned aversive effects of EtOH. Lastly, HS/NPT mice were administered CORT113176 during DID to assess whether dissimilar effects from those of HDID-1 would be observed, which could suggest that selective breeding had altered sensitivity to the effects of GR antagonism on binge-like drinking.

Results: GR antagonism (with both mifepristone and CORT113176) selectively reduced binge-like EtOH intake and BECs in the HDID-1 mice, while inhibition of FKBP51 did not alter intake or BECs. In contrast, GR antagonism had no effect on EtOH intake or BECs in the HS/NPT mice. Although HDID-1 mice exhibit attenuated EtOH CTA, mifepristone administration did not enhance the aversive effects of EtOH in either a CTA or CPA task.

Conclusion: These data suggest that the selection process increased sensitivity to GR antagonism on EtOH intake in the HDID-1 mice, and support a role for the GR as a genetic risk factor for high-risk alcohol intake.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7211124	PMC
http://dx.doi.org/10.1111/acer.14318	DOI Listing

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