Department of Biomedical Sciences, Ontario Veterinary College, University of Guelph, Guelph, ON N1G 2W1, Canada.
Int J Mol Sci. 2022 May 6;23(9):5197. doi: 10.3390/ijms23095197.
Alcohol use is a contributor in the premature deaths of approximately 3 million people annually. Among the risk factors for alcohol misuse is circadian rhythm disruption; however, this connection remains poorly understood. Inhibition of the circadian nuclear receptor REV-ERBα is known to disrupt molecular feedback loops integral to daily oscillations, and impact diurnal fluctuations in the expression of proteins required for reward-related neurotransmission. However, the role of REV-ERBα in alcohol and substance use-related phenotypes is unknown. Herein, we used a α knockout mouse line and ethanol two-bottle choice preference testing to show that disruption of α reduces ethanol preference in male and female mice. α null mice showed the lowest ethanol preference in a two-bottle choice test across all genotypes, whereas there were no ethanol preference differences between heterozygotes and wildtypes. In a separate experiment, alcohol-consuming wildtype C57Bl/6N mice were administered the REV-ERBα/β inhibitor SR8278 (25 mg/kg or 50 mg/kg) for 7 days and alcohol preference was evaluated daily. No differences in alcohol preference were observed between the treatment and vehicle groups. Our data provides evidence that genetic variation in α may contribute to differences in alcohol drinking.
酒精使用是导致每年约 300 万人过早死亡的因素之一。昼夜节律紊乱是酒精滥用的风险因素之一,但这种联系仍未得到很好的理解。已知抑制昼夜核受体 REV-ERBα会破坏对日常振荡至关重要的分子反馈环,并影响与奖励相关的神经递质传递所需蛋白质的昼夜波动。然而,REV-ERBα 在酒精和物质使用相关表型中的作用尚不清楚。在此,我们使用α敲除小鼠品系和乙醇双瓶选择偏好测试表明,α的破坏会降低雄性和雌性小鼠对乙醇的偏好。在所有基因型中,α 缺失小鼠在双瓶选择测试中表现出最低的乙醇偏好,而杂合子和野生型之间没有乙醇偏好差异。在另一个实验中,给饮用酒精的野生型 C57Bl/6N 小鼠连续 7 天给予 REV-ERBα/β抑制剂 SR8278(25mg/kg 或 50mg/kg),并每天评估其对酒精的偏好。在治疗组和对照组之间未观察到酒精偏好的差异。我们的数据提供了证据表明,α中的遗传变异可能导致饮酒差异。
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