对 CB1 大麻受体信号的负异位调节可减少小鼠静脉注射吗啡的自我给药和复发。

IF 3.1 3区 医学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY Addiction Biology Pub Date : 2024-08-07 DOI:10.1111/adb.13429
Idaira Oliva, Fezaan Kazi, Lucas N. Cantwell, Ganesh A. Thakur, Jonathon D. Crystal, Andrea G. Hohmann
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引用次数: 0

摘要

内源性大麻素系统与奖赏系统相互作用,调节对天然强化剂和滥用药物的反应。以前的临床前研究表明,直接阻断 CB1 大麻受体(CB1R)可作为治疗药物使用障碍的一种潜在药理方法,但由于严重的精神副作用,这一策略在临床试验中失败了。为了规避 CB1 直接结合的副作用,出现了通过开发异位调节剂的替代策略。我们假设,对 CB1R 信号的负向异位调节将降低吗啡的强化特性,并减少与阿片类药物滥用相关的行为。通过小鼠静脉自我给药,我们研究了GAT358(一种功能偏倚的CB1R负异位调节剂)对吗啡摄入量、复吸行为和吗啡输注工作动机的影响。GAT358 可减少吗啡自我给药维持阶段的吗啡输注摄入量。GAT358 还能减少强迫戒断后的吗啡寻求行为。此外,在递增比率强化计划下,GAT358 的剂量依赖性降低了获取吗啡输注的动机。令人吃惊的是,在相同的累进比率任务中,GAT358 并不影响获得食物奖励的动机,这表明 GAT358 在减少阿片类药物自我给药方面的作用具有奖励特异性。此外,GAT58在旋转测试中不会产生运动共济失调。我们的研究结果表明,CB1R NAMs 可降低吗啡的强化特性,是安全减少阿片类药物滥用的可行治疗途径。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Negative allosteric modulation of CB1 cannabinoid receptor signalling decreases intravenous morphine self-administration and relapse in mice

The endocannabinoid system interacts with the reward system to modulate responsiveness to natural reinforcers, as well as drugs of abuse. Previous preclinical studies suggested that direct blockade of CB1 cannabinoid receptors (CB1R) could be leveraged as a potential pharmacological approach to treat substance use disorder, but this strategy failed during clinical trials due to severe psychiatric side effects. Alternative strategies have emerged to circumvent the side effects of direct CB1 binding through the development of allosteric modulators. We hypothesized that negative allosteric modulation of CB1R signalling would reduce the reinforcing properties of morphine and decrease behaviours associated with opioid misuse. By employing intravenous self-administration in mice, we studied the effects of GAT358, a functionally-biased CB1R negative allosteric modulator (NAM), on morphine intake, relapse-like behaviour and motivation to work for morphine infusions. GAT358 reduced morphine infusion intake during the maintenance phase of morphine self-administration under a fixed ratio 1 schedule of reinforcement. GAT358 also decreased morphine-seeking behaviour after forced abstinence. Moreover, GAT358 dose dependently decreased the motivation to obtain morphine infusions under a progressive ratio schedule of reinforcement. Strikingly, GAT358 did not affect the motivation to work for food rewards in an identical progressive ratio task, suggesting that the effect of GAT358 in decreasing opioid self-administration was reward specific. Furthermore, GAT58 did not produce motor ataxia in the rotarod test. Our results suggest that CB1R NAMs reduced the reinforcing properties of morphine and could represent a viable therapeutic route to safely decrease misuse of opioids.

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来源期刊
Addiction Biology
Addiction Biology 生物-生化与分子生物学
CiteScore
8.10
自引率
2.90%
发文量
118
审稿时长
6-12 weeks
期刊介绍: Addiction Biology is focused on neuroscience contributions and it aims to advance our understanding of the action of drugs of abuse and addictive processes. Papers are accepted in both animal experimentation or clinical research. The content is geared towards behavioral, molecular, genetic, biochemical, neuro-biological and pharmacology aspects of these fields. Addiction Biology includes peer-reviewed original research reports and reviews. Addiction Biology is published on behalf of the Society for the Study of Addiction to Alcohol and other Drugs (SSA). Members of the Society for the Study of Addiction receive the Journal as part of their annual membership subscription.
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