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雄性和雌性小鼠在自发的 Δ-9-四氢大麻酚戒断期间纹状体多巴胺释放、睡眠和行为的变化。

Changes in striatal dopamine release, sleep, and behavior during spontaneous Δ-9-tetrahydrocannabinol abstinence in male and female mice.

机构信息

National Institute on Alcohol Abuse and Alcoholism, Intramural Research Program, NIH, Bethesda, MD, USA.

Center on Compulsive Behaviors, Intramural Research Program, NIH, Bethesda, MD, USA.

出版信息

Neuropsychopharmacology. 2022 Jul;47(8):1537-1549. doi: 10.1038/s41386-022-01326-0. Epub 2022 Apr 27.

Abstract

Withdrawal symptoms are observed upon cessation of cannabis use in humans. Although animal studies have examined withdrawal symptoms following exposure to delta-9-tetrahydrocannabinol (THC), difficulties in obtaining objective measures of spontaneous withdrawal using paradigms that mimic cessation of use in humans have slowed research. The neuromodulator dopamine (DA) is affected by chronic THC treatment and plays a role in many behaviors related to human THC withdrawal symptoms. These symptoms include sleep disturbances that often drive relapse, and emotional behaviors like irritability and anhedonia. We examined THC withdrawal-induced changes in striatal DA release and the extent to which sleep disruption and behavioral maladaptation manifest during abstinence in a mouse model of chronic THC exposure. Using a THC treatment regimen known to produce tolerance, we measured electrically elicited DA release in acute brain slices from different striatal subregions during early and late THC abstinence. Long-term polysomnographic recordings from mice were used to assess vigilance state and sleep architecture before, during, and after THC treatment. We additionally assessed how behaviors that model human withdrawal symptoms are altered by chronic THC treatment in early and late abstinence. We detected altered striatal DA release, sleep disturbances that mimic clinical observations, and behavioral maladaptation in mice following tolerance to THC. Altered striatal DA release, sleep, and affect-related behaviors associated with spontaneous THC abstinence were more consistently observed in male mice. These findings provide a foundation for preclinical study of directly translatable non-precipitated THC withdrawal symptoms and the neural mechanisms that affect them.

摘要

在人类停止使用大麻时会出现戒断症状。尽管动物研究已经检查了接触 delta-9-四氢大麻酚 (THC) 后出现的戒断症状,但由于难以获得模仿人类停止使用的范式来测量自发戒断的客观指标,因此研究进展缓慢。神经调节剂多巴胺 (DA) 受到慢性 THC 处理的影响,并且在与人类 THC 戒断症状相关的许多行为中发挥作用。这些症状包括经常导致复发的睡眠障碍,以及易怒和快感缺失等情绪行为。我们研究了慢性 THC 暴露小鼠模型中纹状体 DA 释放的 THC 戒断诱导变化,以及在戒断期间睡眠中断和行为适应不良的程度。我们使用已知会产生耐受性的 THC 治疗方案,测量了急性脑片中不同纹状体亚区在早期和晚期 THC 戒断期间电诱发 DA 释放的情况。从小鼠进行的长期多导睡眠描记术记录用于评估在 THC 治疗之前、期间和之后的警觉状态和睡眠结构。我们还评估了慢性 THC 治疗如何改变早期和晚期戒断时模拟人类戒断症状的行为。我们在对 THC 产生耐受性的小鼠中检测到纹状体 DA 释放改变、模拟临床观察的睡眠障碍以及行为适应不良。在雄性小鼠中更一致地观察到与自发 THC 戒断相关的纹状体 DA 释放、睡眠和与情感相关的行为改变。这些发现为直接可转化的非诱发性 THC 戒断症状以及影响它们的神经机制的临床前研究提供了基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fc38/9205922/a5a3b0b639a9/41386_2022_1326_Fig1_HTML.jpg

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