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伏隔核投射的扣带回下皮质神经元的化学遗传刺激可阻断甲苯诱导的条件性位置偏爱。

Chemogenetic Excitation of Accumbens-Projecting Infralimbic Cortical Neurons Blocks Toluene-Induced Conditioned Place Preference.

机构信息

Department of Neuroscience and.

Department of Neuroscience and

出版信息

J Neurosci. 2018 Feb 7;38(6):1462-1471. doi: 10.1523/JNEUROSCI.2503-17.2018. Epub 2018 Jan 9.

Abstract

Abuse rates for inhalants among adolescents continue to be high, yet preclinical models for studying mechanisms underlying inhalant abuse remain limited. Our laboratory has previously shown that, in male rats, an acute binge-like exposure to toluene vapor that mimics human solvent abuse modifies the intrinsic excitability of mPFC pyramidal neurons projecting to the NAc. These changes showed region (infralimbic; IL vs prelimbic; PRL), layer (shallow; 2/3 vs deep; 5/6), target (core vs shell), and age (adolescent vs adult) dependent differences (Wayman and Woodward, 2017). To expand these findings using reward-based models that may better mimic human drug abuse, we used whole-cell electrophysiology and drug receptors exclusively activated by designer drugs to examine changes in neuronal function and behavior in rats showing a conditioned place preference (CPP) to toluene. Repeated pairings of adolescent rats to binge concentrations of toluene vapor previously shown to enhance dopamine release in reward-sensitive areas of the brain produced CPP that persisted for 7 but not 30 d. Toluene-induced CPP was associated with increased excitability of IL5/6 mPFC neurons projecting to the core of the NAc and reduced excitability of those projecting to the NAc shell. No changes in PRL-NAc-projecting neurons were found in toluene-CPP rats. Chemogenetic reversal of the toluene-induced decrease in IL5/6-NAc shell neurons blocked the expression of toluene-induced CPP while manipulating IL5/6-NAc core neuron activity had no effect. These data reveal that alterations in selective mPFC-NAc pathways are required for expression of toluene-induced CPP. Disturbed physiology of pyramidal neurons projecting from the mPFC to the NAc has been shown to have different roles in drug-seeking behaviors for a number of drugs (e.g., methamphetamine, cocaine, ecstasy, alcohol, heroin). Here, we report that rats repeatedly exposed to the volatile organic solvent toluene, a member of the class of abused inhalants often used for intoxicating purposes by adolescents, induces a preference for the drug-paired environment that is accompanied by altered physiology of a specific population of NAc-projecting mPFC neurons. Chemogenetic correction of this deficit before testing prevented expression of drug preference. Overall, these findings highlight the importance of corticolimbic circuitry in mediating the rewarding properties of abused inhalants.

摘要

青少年滥用吸入剂的比率仍然很高,然而,用于研究吸入剂滥用基础机制的临床前模型仍然有限。我们的实验室之前曾表明,在雄性大鼠中,急性 binge 样暴露于甲苯蒸气(模拟人类溶剂滥用)会改变投射到 NAc 的 mPFC 锥体神经元的固有兴奋性。这些变化表现出区域(边缘下;IL 与边缘前;PRL)、层(浅层;2/3 与深层;5/6)、靶区(核心与壳)和年龄(青少年与成年)依赖性差异(Wayman 和 Woodward,2017 年)。为了使用可能更好地模拟人类药物滥用的基于奖励的模型扩展这些发现,我们使用全细胞电生理学和仅被设计药物激活的药物受体来检查对甲苯烷显示条件性位置偏好(CPP)的大鼠的神经元功能和行为变化。在之前显示增强大脑奖励敏感区域多巴胺释放的 binge 浓度下,将青少年大鼠重复配对到甲苯蒸气中,产生了持续 7 天但不是 30 天的 CPP。甲苯诱导的 CPP 与投射到 NAc 核心的 IL5/6 mPFC 神经元的兴奋性增加以及投射到 NAc 壳的神经元的兴奋性降低有关。在甲苯-CPP 大鼠中未发现 PRL-NAc 投射神经元的变化。甲苯诱导的 IL5/6-NAc 壳神经元兴奋性降低的化学遗传逆转阻止了甲苯诱导的 CPP 的表达,而操纵 IL5/6-NAc 核心神经元活动则没有影响。这些数据表明,选择性 mPFC-NAc 途径的改变对于甲苯诱导的 CPP 的表达是必需的。已经表明,投射从 mPFC 到 NAc 的锥体神经元的生理学紊乱在许多药物(例如,甲基苯丙胺,可卡因,摇头丸,酒精,海洛因)的觅药行为中具有不同的作用。在这里,我们报告说,反复暴露于挥发性有机溶剂甲苯(一种经常被青少年用于陶醉目的的滥用吸入剂)的大鼠会诱导对药物配对环境的偏好,同时伴随着投射到 NAc 的特定 mPFC 神经元群体的生理学改变。在测试之前,通过化学遗传方法纠正这种缺陷可防止药物偏好的表达。总体而言,这些发现强调了皮质边缘电路在介导滥用吸入剂的奖赏特性中的重要性。

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