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接触滥用吸入剂甲苯会改变前额叶皮质的生理机能。

Exposure to the Abused Inhalant Toluene Alters Medial Prefrontal Cortex Physiology.

机构信息

Department of Neuroscience, Medical University of South Carolina, Charleston, SC, USA.

Department of Psychiatry & Behavioral Sciences, Medical University of South Carolina, Charleston, SC, USA.

出版信息

Neuropsychopharmacology. 2018 Mar;43(4):912-924. doi: 10.1038/npp.2017.117. Epub 2017 Jun 7.

Abstract

Inhalants, including toluene, target the addiction neurocircuitry and are often one of the first drugs of abuse tried by adolescents. The medial prefrontal cortex (mPFC) is involved in regulating goal-directed/reward-motivated behaviors and different mPFC sub-regions have been proposed to promote (prelimbic, PRL) or inhibit (infralimbic, IL) these behaviors. While this dichotomy has been studied in the context of other drugs of abuse, it is not known whether toluene exposure differentially affects neurons within PRL and IL regions. To address this question, we used whole-cell electrophysiology and determined the intrinsic excitability of PRL and IL pyramidal neurons in adolescent rats 24 h following a brief exposure to air or toluene vapor (10 500 p.p.m.). Prior to exposure, fluorescent retrobeads were injected into the NAc core (NAcc) or shell (NAcs) sub-regions to identify projection-specific mPFC neurons. In toluene treated adolescent rats, layer 5/6 NAcc projecting PRL (PRL5/6) neurons fired fewer action potentials and this was associated with increased rheobase, increased spike duration, and reductions in membrane resistance and amplitude of the I current. No changes in excitability were observed in layer 2/3 NAcc projecting PRL (PRL2/3) neurons. In contrast to PRL neurons, layer 5 IL (IL5) and layer 2/3 (IL2/3) NAcc projecting neurons showed enhanced firing in toluene-exposed animals and in IL5 neurons, this was associated with a reduction in rheobase and AHP. For NAcs projecting neurons, toluene exposure significantly decreased firing of IL5 neurons and this was accompanied by an increased rheobase, increased spike duration, and reduced I amplitude. The intrinsic excitability of PRL5, PRL2/3, and IL2/3 neurons projecting to the NAcs was not affected by exposure to toluene. The changes in excitability observed 24 h after toluene exposure were not observed when recordings were performed 7 days after the exposure. Finally, there were no changes in intrinsic excitability of any region in rats exposed to toluene as adults. These findings demonstrate that specific projections of the reward circuitry are uniquely susceptible to the effects of toluene during adolescence supporting the idea that adolescence is a critical period of the development that is vulnerable to drugs of abuse.

摘要

吸入剂,包括甲苯,靶向成瘾神经回路,并且经常是青少年尝试的第一种滥用药物之一。内侧前额叶皮层(mPFC)参与调节目标导向/奖励动机行为,并且已经提出不同的 mPFC 亚区来促进(边缘前皮质,PRL)或抑制(边缘下皮质,IL)这些行为。虽然这种二分法已经在其他滥用药物的背景下进行了研究,但尚不清楚甲苯暴露是否会对 PRL 和 IL 区域内的神经元产生不同的影响。为了解决这个问题,我们使用全细胞电生理学并确定了青少年大鼠在短暂暴露于空气或甲苯蒸气(10-5000 ppm)后 24 小时内 PRL 和 IL 锥体神经元的固有兴奋性。在暴露之前,将荧光逆行珠注射到 NAcc 核心(NAcc)或壳(NAcs)亚区中,以鉴定投射特异性 mPFC 神经元。在甲苯处理的青少年大鼠中,层 5/6 NAcc 投射的 PRL(PRL5/6)神经元发射的动作电位较少,这与增加基强度、增加峰持续时间以及降低膜电阻和 I 电流幅度有关。在层 2/3 NAcc 投射的 PRL(PRL2/3)神经元中未观察到兴奋性变化。与 PRL 神经元相反,层 5 IL(IL5)和层 2/3(IL2/3)NAcc 投射神经元在甲苯暴露的动物中表现出增强的放电,并且在 IL5 神经元中,这与基强度和 AHP 的降低有关。对于投射到 NAcs 的神经元,甲苯暴露显著降低了 IL5 神经元的放电,这伴随着基强度的增加、峰持续时间的增加和 I 幅度的降低。暴露于甲苯后 24 小时观察到的兴奋性变化在暴露后 7 天进行记录时并未观察到。最后,在成年时暴露于甲苯的大鼠中,任何区域的固有兴奋性都没有变化。这些发现表明,在青春期,奖励回路的特定投射对甲苯的作用具有独特的易感性,支持青春期是易受滥用药物影响的关键发育阶段的观点。

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