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首页> 外文期刊>European neuropsychopharmacology: the journal of the European College of Neuropsychopharmacology >A mouse model of anxiety molecularly characterized by altered protein networks in the brain proteome.
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A mouse model of anxiety molecularly characterized by altered protein networks in the brain proteome.

机译:小鼠焦虑症分子模型的特征是大脑蛋白质组中蛋白质网络的改变。

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Recently, several attempts have been made to describe changes related to certain anxiety states in the proteome of experimental animal models. However, these studies are restricted by limitations regarding the number and correct identification of separated proteins. Moreover, the application of a systems biology approach to discover the molecular mechanisms of anxiety requires genetically homogenous inbred animal models. Therefore, we developed a novel mouse model of anxiety using a combination of crossbreeding (inbred for 35 generations) and behavioral selection. We found significant changes in 82 proteins in the total brain proteome compared to the control proteome. Thirty-four of these proteins had been previously identified in other anxiety, depression or repeated psychosocial stress studies. The identified proteins are associated with different cellular functions, including synaptic transmission, metabolism, proteolysis, protein biosynthesis and folding, cytoskeletal proteins, brain development and neurogenesis, oxidative stress, signal transduction. Our proteomics data suggest that alterations in serotonin receptor-associated proteins, in the carbohydrate metabolism, in the cellular redox system and in synaptic docking are all involved in anxiety.
机译:近来,已经进行了几种尝试来描述与实验动物模型的蛋白质组中的某些焦虑状态有关的变化。但是,这些研究受到有关分离蛋白质的数量和正确鉴定的限制。此外,应用系统生物学方法发现焦虑的分子机制需要遗传上同质的近交动物模型。因此,我们结合杂交(近交35代)和行为选择开发了一种新型的焦虑症小鼠模型。与对照蛋白质组相比,我们发现总脑蛋白质组中82种蛋白质发生了显着变化。这些蛋白质中的34种先前已在其他焦虑症,抑郁症或反复的社会心理压力研究中得到鉴定。鉴定出的蛋白质与不同的细胞功能有关,包括突触传递,代谢,蛋白水解,蛋白质生物合成和折叠,细胞骨架蛋白质,大脑发育和神经发生,氧化应激,信号转导。我们的蛋白质组学数据表明,血清素受体相关蛋白,碳水化合物代谢,细胞氧化还原系统和突触对接的改变均与焦虑有关。

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