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Increased Responding for Alcohol and Resistance to Aversion in Female Mice.雌性小鼠对酒精的反应增强和对厌恶的抵抗。
Alcohol Clin Exp Res. 2020 Jul;44(7):1400-1409. doi: 10.1111/acer.14384. Epub 2020 Jun 18.
2
The transition to compulsion in addiction.成瘾的强制转变。
Nat Rev Neurosci. 2020 May;21(5):247-263. doi: 10.1038/s41583-020-0289-z. Epub 2020 Mar 30.
3
Prefrontal Regulation of Punished Ethanol Self-administration.前额叶对受罚乙醇自我给药的调节。
Biol Psychiatry. 2020 Jun 1;87(11):967-978. doi: 10.1016/j.biopsych.2019.10.030. Epub 2019 Nov 13.
4
A cortical-brainstem circuit predicts and governs compulsive alcohol drinking.皮质脑干回路预测和控制强迫性饮酒。
Science. 2019 Nov 22;366(6468):1008-1012. doi: 10.1126/science.aay1186.
5
Ghrelin receptor antagonism of fentanyl-induced conditioned place preference, intravenous self-administration, and dopamine release in the nucleus accumbens in rats.胃饥饿素受体拮抗芬太尼诱导的条件性位置偏爱、静脉内自我给药和伏隔核多巴胺释放在大鼠中的作用。
Addict Biol. 2020 Nov;25(6):e12845. doi: 10.1111/adb.12845. Epub 2019 Nov 6.
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Additive influences of acute early life stress and sex on vulnerability for aversion-resistant alcohol drinking.急性早期生活应激与性别对耐厌恶酒精饮用易感性的累加影响。
Addict Biol. 2020 Nov;25(6):e12829. doi: 10.1111/adb.12829. Epub 2019 Oct 27.
7
Oral prescription opioid-seeking behavior in male and female mice.雄性和雌性小鼠的口服阿片类药物觅药行为。
Addict Biol. 2020 Nov;25(6):e12828. doi: 10.1111/adb.12828. Epub 2019 Sep 5.
8
Sex Differences in Ethanol Reward Seeking Under Conflict in Mice.雄性和雌性小鼠在冲突条件下对乙醇奖赏寻求的性别差异。
Alcohol Clin Exp Res. 2019 Jul;43(7):1556-1566. doi: 10.1111/acer.14070. Epub 2019 May 18.
9
Opioid-like antinociceptive and locomotor effects of emerging fentanyl-related substances.新兴芬太尼相关物质的类阿片样镇痛和运动效应。
Neuropharmacology. 2019 Jun;151:171-179. doi: 10.1016/j.neuropharm.2019.03.023. Epub 2019 Mar 20.
10
Sex Differences in Aversion-Resistant Ethanol Intake in Mice.小鼠对乙醇摄入的抗拒性的性别差异。
Alcohol Alcohol. 2019 Jul 1;54(4):345-352. doi: 10.1093/alcalc/agz022.

耐阿片类药物的芬太尼自我给药在小鼠体内的研究

Aversion-resistant fentanyl self-administration in mice.

机构信息

Department of Psychology and Center for Neuroscience and Behavior, Miami University, 90 N Patterson Ave, Oxford, OH, 45056, USA.

出版信息

Psychopharmacology (Berl). 2021 Mar;238(3):699-710. doi: 10.1007/s00213-020-05722-6. Epub 2020 Nov 23.

DOI:10.1007/s00213-020-05722-6
PMID:33226446
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7914171/
Abstract

RATIONALE

Animal models of compulsive drug use that continues despite negative consequences can be used to investigate the neural mechanisms of addiction. However, models of punished or aversion-resistant opioid self-administration are notably lacking.

OBJECTIVES

We sought to develop an aversion-resistant, oral fentanyl self-administration paradigm.

METHODS

In Experiment 1, C57BL/6J male and female, adult mice consumed fentanyl (10 μg/mL) in a two-bottle drinking in the dark task and escalating concentrations of quinine were added to the bottles. In Experiment 2, mice were trained to administer oral fentanyl (10 μg/mL) in an operant response task. Quinine was next added to the fentanyl solution in escalating concentrations. In Experiment 3, mice were trained to respond for oral fentanyl or fentanyl adulterated with 500 μM quinine on every session. In Experiment 4, mice were trained to respond for a 1% sucrose solution before introduction of quinine.

RESULTS

Quinine reduced two-bottle choice consumption in males but not in females. Both sexes demonstrated the ability to detect the selected concentrations of quinine in fentanyl. In the operant chamber, mice responded robustly for oral fentanyl but introduction of quinine at any stage of training was insufficient to reduce responding. In contrast, quinine reduced responding for sucrose at concentrations above 250 μM.

CONCLUSIONS

Mice will respond for and consume oral fentanyl in both a two-bottle choice and an operant response task. Quinine is detectable in fentanyl but mice will continue to respond for and consume fentanyl with quinine in both paradigms. These data support the use of these models in behavioral studies of compulsive-like opioid use.

摘要

背景

尽管存在负面后果,但仍持续使用的强迫性药物使用的动物模型可用于研究成瘾的神经机制。然而,缺乏惩罚或抗厌恶的阿片类药物自我给药模型。

目的

我们试图开发一种抗厌恶的、口服芬太尼自我给药范式。

方法

在实验 1 中,C57BL/6J 雄性和雌性成年小鼠在黑暗中的两瓶饮用任务中消耗芬太尼(10μg/ml),并向瓶中添加递增浓度的奎宁。在实验 2 中,训练小鼠在操作性反应任务中给予口服芬太尼(10μg/ml)。接下来,向芬太尼溶液中添加递增浓度的奎宁。在实验 3 中,训练小鼠在每一次会议上对口服芬太尼或芬太尼与 500μM 奎宁混合的药物做出反应。在实验 4 中,在引入奎宁之前,训练小鼠对 1%蔗糖溶液做出反应。

结果

奎宁减少了雄性而不是雌性的两瓶选择消费。两性均能够检测到芬太尼中的选定浓度的奎宁。在操作室中,小鼠对口服芬太尼反应强烈,但在训练的任何阶段引入奎宁都不足以减少反应。相比之下,奎宁减少了对浓度高于 250μM 的蔗糖的反应。

结论

小鼠将在两瓶选择和操作性反应任务中对口服芬太尼做出反应并消耗。奎宁可在芬太尼中被检测到,但在这两种范式中,小鼠仍将继续对芬太尼与奎宁做出反应并消耗。这些数据支持在强迫性阿片类药物使用的行为研究中使用这些模型。