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间歇性接触尼古丁自我给药后出现类似复发的行为和烟碱型乙酰胆碱受体敏化。

Relapse-like behavior and nAChR sensitization following intermittent access nicotine self-administration.

机构信息

Department of Physiology & Pharmacology, Wake Forest University School of Medicine, Winston-Salem, NC, USA.

Department of Pharmacology & Cancer Biology, Duke University School of Medicine, Durham, NC, USA.

出版信息

Neuropharmacology. 2022 Jul 1;212:109066. doi: 10.1016/j.neuropharm.2022.109066. Epub 2022 Apr 21.

Abstract

Many tobacco smokers consume nicotine intermittently, but the underlying mechanisms and neurobiological changes associated with intermittent nicotine intake are unclear. Understanding intermittent nicotine intake is a high priority, as it could promote therapeutic strategies to attenuate tobacco consumption. We examined nicotine intake behavior and neurobiological changes in male rats that were trained to self-administer nicotine during brief (5 min) trials interspersed with longer (15 min) drug-free periods. Rats readily adapted to intermittent access (IntA) SA following acquisition on a continuous access (ContA) schedule. Probabilistic analysis of IntA nicotine SA suggested reduced nicotine loading behavior compared to ContA, and nicotine pharmacokinetic modeling revealed that rats taking nicotine intermittently may have increased intake to maintain blood levels of nicotine that are comparable to ContA SA. After IntA nicotine SA, rats exhibited an increase in unreinforced responses for nicotine-associated cues (incubation of craving) and specific alterations in the striatal proteome after 7 days without nicotine. IntA nicotine SA also induced nAChR functional upregulation in the interpeduncular nucleus (IPN), and it enhanced nicotine binding in the brain as determined via [C]nicotine positron emission tomography. Reducing the saliency of the cue conditions during the 5 min access periods attenuated nicotine intake, but incubation of craving was preserved. Together, these results indicate that IntA conditions promote nicotine SA and nicotine seeking after a nicotine-free period.

摘要

许多烟民间歇性地摄入尼古丁,但间歇性摄入尼古丁相关的潜在机制和神经生物学变化尚不清楚。理解间歇性摄入尼古丁是当务之急,因为它可能促进治疗策略来减轻烟草消费。我们在雄性大鼠中检查了尼古丁摄入行为和神经生物学变化,这些大鼠在短暂(5 分钟)试验中接受自我管理尼古丁,同时间隔更长的(15 分钟)无药物期。大鼠在连续摄入(ContA)方案上获得适应性后,很容易适应间歇性摄入(IntA)SA。IntA 尼古丁 SA 的概率分析表明,与 ContA 相比,尼古丁加载行为减少,尼古丁药代动力学建模表明,间歇性摄入尼古丁的大鼠可能会增加摄入量,以维持与 ContA SA 相当的血液尼古丁水平。在 IntA 尼古丁 SA 后,大鼠在没有尼古丁的 7 天后表现出对尼古丁相关线索(渴望的潜伏期)的无强化反应增加,以及纹状体蛋白质组的特定改变。IntA 尼古丁 SA 还诱导了中脑导水管周围灰质(IPN)中的 nAChR 功能上调,并通过 [C]尼古丁正电子发射断层扫描确定增强了大脑中的尼古丁结合。在 5 分钟的访问期间降低线索条件的显著性可减轻尼古丁的摄入量,但渴望的潜伏期仍然存在。总之,这些结果表明,IntA 条件促进了尼古丁 SA 和尼古丁寻求,在无尼古丁期之后。

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