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Transcriptomic analyses and leukocyte telomere length measurement in subjects exposed to severe recent stressful life events

机译:暴露于严重近期应激生活事件的受试者的转录组学分析和白细胞端粒长度测量

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摘要

Stressful life events occurring in adulthood have been found able to affect mood and behavior, thus increasing the vulnerability for several stress-related psychiatric disorders. However, although there is plenty of clinical data supporting an association between stressful life events in adulthood and an enhanced vulnerability for psychopathology, the underlying molecular mechanisms are still poorly investigated. Thus, in this study we performed peripheral/whole-genome transcriptomic analyses in blood samples obtained from 53 adult subjects characterized for recent stressful life events occurred within the previous 6 months. Transcriptomic data were analyzed using Partek Genomics Suite; pathway and network analyses were performed using Ingenuity Pathway Analysis and GeneMANIA Software. We found 207 genes significantly differentially expressed in adult subjects who reported recent stressful life experiences ( n =21) compared with those without such experiences ( n =32). Moreover, the same subjects exposed to such stressful experiences showed a reduction in leukocyte telomere length. A correlation analyses between telomere length and transcriptomic data indicated an association between the exposures to recent stressful life events and the modulation of several pathways, mainly involved in immune-inflammatory-related processes and oxidative stress, such as natural killer cell signaling, interleukin-1 (IL-1) signaling, MIF regulation of innate immunity and IL-6 signaling. Our data suggest an association between exposures to recent stressful life events in adulthood and alterations in the immune, inflammatory and oxidative stress pathways, which could be also involved in the negative effect of stressful life events on leukocyte telomere length. The modulation of these mechanisms may underlie the clinical association between the exposure to recent Stressful life events in adulthood and an enhanced vulnerability to develop psychiatric diseases in adulthood.
机译:已经发现,成年后发生的应激性生活事件能够影响情绪和行为,从而增加了几种与压力有关的精神病的脆弱性。然而,尽管有大量的临床数据支持成年后的应激性生活事件与心理病理学易感性之间的关联,但对潜在分子机制的研究仍很少。因此,在这项研究中,我们对53名成年受试者的血液样本进行了外周/全基因组转录组学分析,这些样本的特征是最近6个月内发生了近期的应激性生活事件。使用Partek Genomics Suite分析转录组数据。使用Ingenuity Pathway Analysis和GeneMANIA Software进行通路和网络分析。我们发现207个基因在报告了最近的生活经历(n = 21)的成年人中显着差异表达,而没有经历的经历(n = 32)。而且,暴露于这种压力经历的相同受试者显示白细胞端粒长度的减少。端粒长度与转录组数据之间的相关性分析表明,近期应激性生活事件的暴露与几种途径的调节之间存在关联,这些途径主要参与免疫炎症相关过程和氧化应激,例如自然杀伤细胞信号传导,白介素-1 (IL-1)信号传导,MIF调节先天免疫和IL-6信号传导。我们的数据表明,成年期最近的应激性生活事件的暴露与免疫,炎症和氧化应激途径的改变之间可能存在关联,这也可能与应激性生活事件对白细胞端粒长度的负面影响有关。这些机制的调节可能是成年后暴露于近期应激生活事件与成年后发展为精神疾病的易感性增强之间的临床联系的基础。

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