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Publication : The role of clock in ethanol-related behaviors.

First Author  Ozburn AR Year  2013
Journal  Neuropsychopharmacology Volume  38
Issue  12 Pages  2393-400
PubMed ID  23722243 Mgi Jnum  J:322665
Mgi Id  MGI:6862152 Doi  10.1038/npp.2013.138
Citation  Ozburn AR, et al. (2013) The role of clock in ethanol-related behaviors. Neuropsychopharmacology 38(12):2393-400
abstractText  Mice with a mutation in the Clock gene (ClockDelta19) exhibit increased preference for stimulant rewards and sucrose. They also have an increase in dopaminergic activity in the ventral tegmental area (VTA) and a general increase in glutamatergic tone that might underlie these behaviors. However, it is unclear if their phenotype would extend to a very different class of drug (ethanol), and if so, whether these systems might be involved in their response. Continuous access voluntary ethanol intake was evaluated in ClockDelta19 mutants and wild-type (WT) mice. We found that ClockDelta19 mice exhibited significantly increased ethanol intake in a two-bottle choice paradigm. Interestingly, this effect was more robust in female mice. Moreover, chronic ethanol experience resulted in a long-lasting decrease in VTA Clock expression. To determine the importance of VTA Clock expression in ethanol intake, we knocked down Clock expression in the VTA of WT mice via RNA interference. We found that reducing Clock expression in the VTA resulted in significantly increased ethanol intake similar to the ClockDelta19 mice. Interestingly, we also discovered that ClockDelta19 mice exhibit significantly augmented responses to the sedative effects of ethanol and ketamine, but not pentobarbital. However, their drinking behavior was not affected by acamprosate, an FDA-approved drug for the treatment of alcoholism, suggesting that their increased glutamatergic tone might underlie the increased sensitivity to the sedative/hypnotic properties of ethanol but not the rewarding properties of ethanol. Taken together, we have identified a significant role for Clock in the VTA as a negative regulator of ethanol intake and implicate the VTA dopamine system in this response.
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