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Functional Genomic and Proteomic Analysis Reveals Disruption of Myelin-Related Genes and Translation in a Mouse Model of Early Life Neglect

机译:功能基因组和蛋白质组学分析揭示了髓鞘相关基因的破坏和早期忽视的小鼠模型中的翻译。

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摘要

Early life neglect is an important public health problem which can lead to lasting psychological dysfunction. Good animal models are necessary to understand the mechanisms responsible for the behavioral and anatomical pathology that results. We recently described a novel model of early life neglect, maternal separation with early weaning (MSEW), that produces behavioral changes in the mouse that persist into adulthood. To begin to understand the mechanism by which MSEW leads to these changes we applied cDNA microarray, next-generation RNA-sequencing (RNA-seq), label-free proteomics, multiple reaction monitoring (MRM) proteomics, and methylation analysis to tissue samples obtained from medial prefrontal cortex to determine the molecular changes induced by MSEW that persist into adulthood. The results show that MSEW leads to dysregulation of markers of mature oligodendrocytes and genes involved in protein translation and other categories, an apparent downward biasing of translation, and methylation changes in the promoter regions of selected dysregulated genes. These findings are likely to prove useful in understanding the mechanism by which early life neglect affects brain structure, cognition, and behavior.
机译:忽视早期生活是一个重要的公共卫生问题,可能导致持久的心理功能障碍。良好的动物模型对于理解导致行为和解剖病理学的机制必不可少。我们最近描述了一种早期忽略生命的新模型,即早期断奶的母婴分离(MSEW),该模型会在小鼠中产生行为变化,并持续到成年期。为了开始了解MSEW导致这些变化的机制,我们对获得的组织样品应用了cDNA微阵列,下一代RNA测序(RNA-seq),无标记蛋白质组学,多反应监测(MRM)蛋白质组学和甲基化分析从内侧前额叶皮层确定持续到成年的MSEW诱导的分子变化。结果表明,MSEW导致成熟的少突胶质细胞和参与蛋白质翻译及其他类别的基因的标记失调,翻译的明显向下偏向以及所选失调基因的启动子区域的甲基化变化。这些发现可能被证明有助于理解早期忽视生命影响大脑结构,认知和行为的机制。

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