齿状回的新神经元促进甲基苯丙胺寻找的恢复。

Journal of Experimental Neuroscience Pub Date : 2018-06-04 eCollection Date: 2018-01-01 DOI:10.1177/1179069518779625
Chitra D Mandyam, Sucharita S Somkuwar, Robert J Oliver, Yoshio Takashima
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引用次数: 3

摘要

成瘾性药物通过改变控制回路的神经元的功能可塑性来影响大脑奖赏回路。复发是成瘾者的固有问题,与包括海马体在内的几个大脑区域的神经可塑性变化有关。最近的研究已经开始确定海马齿状回成体神经发生的功能意义,在那里颗粒细胞层中不断产生新的神经元来取代死亡或患病的细胞。在啮齿类动物和非人类灵长类动物模型中,慢性甲基苯丙胺(冰毒)滥用和冰毒成瘾的许多负面后果之一是在冰毒暴露期间齿状回神经祖细胞减少,颗粒细胞层神经发生减少。然而,最近Galinato等人研究了戒断和戒断期间祖细胞数量的反弹,以及戒断期间祖细胞存活率提高对复发倾向的功能意义。冰毒成瘾的大鼠模型与消融神经祖细胞的药物遗传学方法一致表明,戒断期间的神经发生促进了寻求冰毒行为的复发。生化和电生理学研究表明,戒断期间神经发生的增加与齿状回中与学习和记忆相关的可塑性相关蛋白的增加以及颗粒细胞神经元自发活动的增强和神经元兴奋性的降低相关。基于这些发现,我们讨论了可能导致戒断期间异常神经发生的分子机制。我们还指出,在冰毒成瘾的动物中,前脑-齿状回回路可能有助于异常的神经发生,并导致寻求冰毒行为的复发。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

New Neurons in the Dentate Gyrus Promote Reinstatement of Methamphetamine Seeking.

New Neurons in the Dentate Gyrus Promote Reinstatement of Methamphetamine Seeking.

Addictive drugs effect the brain reward circuitry by altering functional plasticity of neurons governing the circuits. Relapse is an inherent problem in addicted subjects and is associated with neuroplasticity changes in several brain regions including the hippocampus. Recent studies have begun to determine the functional significance of adult neurogenesis in the dentate gyrus of the hippocampus, where new neurons in the granule cell layer are continuously generated to replace dying or diseased cells. One of the many negative consequences of chronic methamphetamine (METH) abuse and METH addiction in rodent and nonhuman primate models is a decrease in neural progenitor cells in the dentate gyrus and reduced neurogenesis in the granule cell layer during METH exposure. However, the number of progenitors rebound during withdrawal and abstinence from METH and the functional significance of enhanced survival of the progenitors during abstinence on the propensity for relapse was recently investigated by Galinato et al. A rat model of METH addiction in concert with a pharmacogenetic approach of ablating neural progenitor cells revealed that neurogenesis during abstinence promoted a relapse to METH-seeking behavior. Biochemical and electrophysiology studies demonstrated that an increase in neurogenesis during abstinence correlated with increases in plasticity-related proteins associated with learning and memory in the dentate gyrus and enhanced spontaneous activity and reduced neuronal excitability of granule cell neurons. Based on these findings, we discuss the putative molecular mechanisms that could drive aberrant neurogenesis during abstinence. We also indicate forebrain-dentate gyrus circuits that could assist with aberrant neurogenesis and drive a relapse into METH-seeking behavior in METH-addicted animals.

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