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痕量胺相关受体 1 激动剂 RO 5263397 对乙醇诱导的行为敏化的影响。

Effects of a trace amine-associated receptor 1 agonist RO 5263397 on ethanol-induced behavioral sensitization.

机构信息

Department of Pharmacology and Toxicology, University at Buffalo, Buffalo, NY, United States; School of Medicine, Yangzhou University, Yangzhou, China.

Department of Pharmacology and Toxicology, University at Buffalo, Buffalo, NY, United States.

出版信息

Behav Brain Res. 2020 Jul 15;390:112641. doi: 10.1016/j.bbr.2020.112641. Epub 2020 May 12.

Abstract

BACKGROUND

Alcohol dependence is a chronic and severe health problem which puts a heavy burden on society. Alcohol activates mesolimbic dopamine circuity to achieve its reinforcing effect. While TAAR1 is critically involved in the modulation of dopamine, there is little evidence indicating that TAAR1 could play a role in behavioral effects of ethanol.

METHODS

By using the animal model of behavioral sensitization induced by ethanol in mice, the present study was performed to investigate whether the activation of TAAR1 would affect the behavioral plasticity of ethanol.

RESULTS

Repeated administration with ethanol induced a significant increased locomotion in WT mice with females showing higher level of sensitization to ethanol than male mice. The TAAR1 agonist RO5263397 significantly decreased the expression of ethanol-induced behavioral sensitization both in male and female WT mice (0.1 and 0.32 mg/kg). Repeated RO5263397 exposure also prevented the development of behavioral sensitization to ethanol both in male and female WT mice. Moreover, while TAAR1-KO mice developed normal levels of ethanol-induced behavioral sensitization, RO5263397 did not affect this behavior in TAAR1-KO mice.

CONCLUSIONS

These results indicated that the TAAR1 agonist RO5263397 negatively regulated the expression and development of ethanol-elicited behavioral sensitization in WT but not in TAAR1-KO mice. The present study suggests that TAAR1 is probably involved in certain addiction-like effects of alcohol and could be a useful drug target for the development of new medications to treat alcohol dependence.

摘要

背景

酒精依赖是一种慢性且严重的健康问题,给社会带来了沉重的负担。酒精激活中脑边缘多巴胺回路,从而产生强化作用。虽然 TAAR1 对多巴胺的调节至关重要,但目前几乎没有证据表明 TAAR1 在乙醇的行为效应中发挥作用。

方法

本研究通过使用乙醇诱导的小鼠行为敏化动物模型,研究 TAAR1 的激活是否会影响乙醇的行为可塑性。

结果

重复给予乙醇会诱导 WT 小鼠的运动活动显著增加,且雌性小鼠对乙醇的敏化程度高于雄性小鼠。TAAR1 激动剂 RO5263397 可显著降低 WT 雄性和雌性小鼠中乙醇诱导的行为敏化表达(0.1 和 0.32 mg/kg)。重复暴露于 RO5263397 也可预防 WT 雄性和雌性小鼠对乙醇的行为敏化的发展。此外,虽然 TAAR1-KO 小鼠对乙醇诱导的行为敏化表现出正常水平,但 RO5263397 对 TAAR1-KO 小鼠的这种行为没有影响。

结论

这些结果表明,TAAR1 激动剂 RO5263397 负调节 WT 小鼠而非 TAAR1-KO 小鼠中乙醇诱发的行为敏化的表达和发展。本研究表明 TAAR1 可能参与了酒精的某些类似成瘾的效应,并且可能成为开发新的治疗酒精依赖药物的有用药物靶点。

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