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通过雷帕霉素对mTOR激酶进行全身抑制来破坏重新巩固可减少觅可卡因行为。

Disrupting Reconsolidation by Systemic Inhibition of mTOR Kinase via Rapamycin Reduces Cocaine-Seeking Behavior.

作者信息

Zhang Fushen, Huang Shihao, Bu Haiyan, Zhou Yu, Chen Lixiang, Kang Ziliu, Chen Liangpei, Yan He, Yang Chang, Yan Jie, Jian Xiaohong, Luo Yixiao

机构信息

Key Laboratory of Molecular Epidemiology of Hunan Province, School of Medicine, Hunan Normal University, Changsha, China.

Yiyang Medical College, Yiyang, China.

出版信息

Front Pharmacol. 2021 Apr 9;12:652865. doi: 10.3389/fphar.2021.652865. eCollection 2021.

Abstract

Drug addiction is considered maladaptive learning, and drug-related memories aroused by the presence of drug related stimuli (drug context or drug-associated cues) promote recurring craving and reinstatement of drug seeking. The mammalian target of rapamycin signaling pathway is involved in reconsolidation of drug memories in conditioned place preference and alcohol self-administration (SA) paradigms. Here, we explored the effect of mTOR inhibition on reconsolidation of addiction memory using cocaine self-administration paradigm. Rats received intravenous cocaine self-administration training for 10 consecutive days, during which a light/tone conditioned stimulus was paired with each cocaine infusion. After acquisition of the stable cocaine self-administration behaviors, rats were subjected to nosepoke extinction (11 days) to extinguish their behaviors, and then received a 15 min retrieval trial with or without the cocaine-paired tone/light cue delivery or without. Immediately or 6 h after the retrieval trial, rapamycin (10 mg/kg) was administered intraperitoneally. Finally, cue-induced reinstatement, cocaine-priming-induced reinstatement and spontaneous recovery of cocaine-seeking behaviors were assessed in rapamycin previously treated animals, respectively. We found that rapamycin treatment immediately after a retrieval trial decreased subsequent reinstatement of cocaine seeking induced by cues or cocaine itself, and these effects lasted at least for 28 days. In contrast, delayed intraperitoneal injection of rapamycin 6 h after retrieval or rapamycin injection without retrieval had no effects on cocaine-seeking behaviors. These findings indicated that mTOR inhibition within the reconsolidation time-window impairs the reconsolidation of cocaine associated memory, reduces cocaine-seeking behavior and prevents relapse, and these effects are retrieval-dependent and temporal-specific.

摘要

药物成瘾被认为是一种适应不良的学习行为,与药物相关的刺激(药物环境或与药物相关的线索)引发的与药物相关的记忆会促使复发性渴望和恢复觅药行为。雷帕霉素信号通路的哺乳动物靶点参与了条件性位置偏爱和酒精自我给药(SA)范式中药物记忆的重新巩固。在此,我们使用可卡因自我给药范式探究了mTOR抑制对成瘾记忆重新巩固的影响。大鼠连续10天接受静脉注射可卡因自我给药训练,在此期间,每次注射可卡因时都伴有光/音条件刺激。在获得稳定的可卡因自我给药行为后,对大鼠进行鼻触消退训练(11天)以消除其行为,然后进行15分钟的恢复试验,试验过程中伴有或不伴有与可卡因配对的音/光线索呈现,或两者都不呈现。在恢复试验后立即或6小时后,腹腔注射雷帕霉素(10mg/kg)。最后,分别在先前接受雷帕霉素治疗的动物中评估线索诱导的复吸、可卡因激发诱导的复吸以及可卡因觅药行为的自发恢复情况。我们发现,在恢复试验后立即给予雷帕霉素治疗可减少随后由线索或可卡因本身诱导的可卡因觅药行为的复吸,且这些作用至少持续28天。相比之下,在恢复试验6小时后延迟腹腔注射雷帕霉素或在未进行恢复试验的情况下注射雷帕霉素对可卡因觅药行为没有影响。这些发现表明,在重新巩固时间窗口内抑制mTOR会损害可卡因相关记忆的重新巩固,减少可卡因觅药行为并预防复发,且这些作用依赖于恢复试验且具有时间特异性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d657/8064688/395753c779e5/fphar-12-652865-g001.jpg

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