首页> 外文期刊>Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences >Protein expression profile in the amygdala of rats with methamphetamine-induced behavioral sensitization.
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Protein expression profile in the amygdala of rats with methamphetamine-induced behavioral sensitization.

机译:甲基苯丙胺诱导的行为敏化大鼠杏仁核中的蛋白表达谱。

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Repeated exposure to methamphetamine (MAP) results in a progressively enhanced and enduring behavioral response to the drug. This phenomenon is known as behavioral sensitization. MAP-induced sensitization has been suggested to underlie certain aspects of MAP psychosis and schizophrenia. The mesolimbic dopamine system including the ventral tegmental area, nucleus accumbens (NAc) and associated brain regions such as the amygdala (AMG) are proposed to be involved in the behavioral sensitization. However, the molecular mechanisms underlying this protracted alteration of behavior are almost unknown. Here we examined protein expression profiles in the AMG of acute MAP-treated and MAP-sensitized rats using 2-DE-based proteomics. Analysis revealed that 64 and 43 protein spots were differentially regulated in the AMG of acute MAP-treated and MAP-sensitized rats, respectively, when compared to control rats. A total of 48 and 34 proteins were identified in these two models, respectively using MALDI-ToF-MS. When the results were compared between acute and chronic MAP-treated groups, only 9 proteins were identified in common. These proteins could be related to acute MAP effects and/or non-specific effects. It is therefore suggested that AMG react differently to the acute and repeated administration of MAP at least at the protein expression level. A number of proteins in the categories of synaptic, cytoskeletal, oxidative stress, apoptosis, and mitochondria related proteins were differentially expressed in the AMG of sensitized animals. Changes of these protein expressions in the AMG could be associated with the mechanism underlying behavioral sensitization.
机译:反复接触甲基苯丙胺(MAP)会导致对该药物的行为反应逐渐增强和持久。这种现象被称为行为敏化。 MAP引起的致敏作用被认为是MAP精神病和精神分裂症某些方面的基础。包括腹侧被盖区,伏伏核(NAc)和相关的脑区域如杏仁核(AMG)在内的中脑边缘多巴胺系统被提议参与行为敏化。但是,这种长期改变行为的分子机制几乎是未知的。在这里,我们使用基于2-DE的蛋白质组学检查了急性MAP治疗和MAP致敏大鼠AMG中的蛋白表达谱。分析显示,与对照大鼠相比,急性MAP治疗和MAP致敏大鼠的AMG中分别有64和43个蛋白斑点受到差异调节。在这两个模型中,分别使用MALDI-ToF-MS鉴定出总共48和34种蛋白质。当比较急性和慢性MAP治疗组的结果时,仅鉴定出9种共同蛋白。这些蛋白质可能与急性MAP效应和/或非特异性效应有关。因此,建议AMG至少在蛋白质表达水平上对MAP的急性和重复给药反应不同。在致敏动物的AMG中,突触,细胞骨架,氧化应激,细胞凋亡和线粒体相关蛋白类别中的许多蛋白质差异表达。 AMG中这些蛋白质表达的变化可能与行为致敏的机制有关。

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