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Dysregulated immune system networks in war veterans with PTSD is an outcome of altered miRNA expression and DNA methylation

机译:患有PTSD的退伍军人的免疫系统网络失调是miRNA表达和DNA甲基化改变的结果

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摘要

Post-traumatic stress disorder patients experience chronic systemic inflammation. However, the molecular pathways involved and mechanisms regulating the expression of genes involved in inflammatory pathways in PTSD are reported inadequately. Through RNA sequencing and miRNA microarray, we identified 326 genes and 190 miRNAs that were significantly different in their expression levels in the PBMCs of PTSD patients. Expression pairing of the differentially expressed genes and miRNAs indicated an inverse relationship in their expression. Functional analysis of the differentially expressed genes indicated their involvement in the canonical pathways specific to immune system biology. DNA methylation analysis of differentially expressed genes also showed a gradual trend towards differences between control and PTSD patients, again indicating a possible role of this epigenetic mechanism in PTSD inflammation. Overall, combining data from the three techniques provided a holistic view of several pathways in which the differentially expressed genes were impacted through epigenetic mechanisms, in PTSD. Thus, analysis combining data from RNA-Seq, miRNA array and DNA methylation, can provide key evidence about dysregulated pathways and the controlling mechanism in PTSD. Most importantly, the present study provides further evidence that inflammation in PTSD could be epigenetically regulated.
机译:创伤后应激障碍患者会经历慢性全身性炎症。然而,关于PTSD中炎症途径所涉及的分子途径和调控基因表达的机制的报道不足。通过RNA测序和miRNA芯片,我们鉴定了326个基因和190个miRNA,它们在PTSD患者的PBMC中的表达水平显着不同。差异表达的基因和miRNA的表达配对表明它们的表达呈反比关系。差异表达基因的功能分析表明它们参与了免疫系统生物学特有的经典途径。差异表达基因的DNA甲基化分析也显示了对照和PTSD患者之间差异的逐渐趋势,再次表明这种表观遗传机制在PTSD炎症中的可能作用。总体而言,将来自这三种技术的数据结合起来,可以全面了解PTSD中差异表达基因通过表观遗传机制受到影响的几种途径。因此,将来自RNA-Seq,miRNA阵列和DNA甲基化的数据相结合的分析可以提供有关PTSD通路失调和控制机制的关键证据。最重要的是,本研究提供了进一步的证据表明,PTSD中的炎症可以通过表观遗传调控。

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