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肌痛性脑脊髓炎/慢性疲劳综合征的表观遗传学成分揭示了潜在的转座元件激活。

Epigenetic Components of Myalgic Encephalomyelitis/Chronic Fatigue Syndrome Uncover Potential Transposable Element Activation.

机构信息

Escuela de Doctorado, Universidad Católica de Valencia San Vicente Mártir, Valencia, Spain.

School of Medicine, Universidad Católica de Valencia San Vicente Mártir, Valencia, Spain.

出版信息

Clin Ther. 2019 Apr;41(4):675-698. doi: 10.1016/j.clinthera.2019.02.012. Epub 2019 Mar 23.

Abstract

PURPOSE

Studies to determine epigenetic changes associated with myalgic encephalomyelitis/chronic fatigue syndrome (ME/CFS) remain scarce; however, current evidence clearly shows that methylation patterns of genomic DNA and noncoding RNA profiles of immune cells differ between patients and healthy subjects, suggesting an active role of these epigenetic mechanisms in the disease. The present study compares and contrasts the available ME/CFS epigenetic data in an effort to evidence overlapping pathways capable of explaining at least some of the dysfunctional immune parameters linked to this disease.

METHODS

A systematic search of the literature evaluating the ME/CFS epigenome landscape was performed following the Preferred Reporting Items for Systematic Reviews and Meta-Analyses criteria. Differential DNA methylation and noncoding RNA differential expression patterns associated with ME/CFS were used to screen for the presence of transposable elements using the Dfam browser, a search program nurtured with the Repbase repetitive sequence database and the RepeatMasker annotation tool.

FINDINGS

Unexpectedly, particular associations of transposable elements and ME/CFS epigenetic hallmarks were uncovered. A model for the disease emerged involving transcriptional induction of endogenous dormant transposons and structured cellular RNA interactions, triggering the activation of the innate immune system without a concomitant active infection.

IMPLICATIONS

Repetitive sequence filters (ie, RepeatMasker) should be avoided when analyzing transcriptomic data to assess the potential participation of repetitive sequences ("junk repetitive DNA"), representing >45% of the human genome, in the onset and evolution of ME/CFS. In addition, transposable element screenings aimed at designing cost-effective, focused empirical assays that can confirm or disprove the suspected involvement of transposon transcriptional activation in this disease, following the pilot strategy presented here, will require databases gathering large ME/CFS epigenetic datasets.

摘要

目的

与肌痛性脑脊髓炎/慢性疲劳综合征(ME/CFS)相关的表观遗传变化的研究仍然很少;然而,目前的证据清楚地表明,免疫细胞基因组 DNA 的甲基化模式和非编码 RNA 谱在患者和健康受试者之间存在差异,这表明这些表观遗传机制在疾病中具有积极作用。本研究比较和对比了现有的 ME/CFS 表观遗传数据,努力证明重叠的途径能够解释至少一些与这种疾病相关的功能失调的免疫参数。

方法

根据系统评价和荟萃分析的首选报告项目标准,对评估 ME/CFS 表观基因组景观的文献进行了系统搜索。使用 Dfam 浏览器筛选与 ME/CFS 相关的差异 DNA 甲基化和非编码 RNA 差异表达模式,该浏览器是一个使用 Repbase 重复序列数据库和 RepeatMasker 注释工具培育的搜索程序。

结果

出乎意料的是,发现了转座元件与 ME/CFS 表观遗传特征的特定关联。出现了一种疾病模型,涉及内源性休眠转座子的转录诱导和结构细胞 RNA 相互作用,触发固有免疫系统的激活,而没有伴随的活跃感染。

意义

在分析转录组数据以评估重复序列(即重复Masker)在评估重复序列(代表人类基因组的>45%)在 ME/CFS 的发生和发展中的潜在参与时,应避免使用重复序列过滤器。此外,为了设计具有成本效益的、有针对性的经验性检测,以证实或反驳这里提出的试点策略中推测的转座子转录激活在这种疾病中的可疑参与,需要收集大量 ME/CFS 表观遗传数据集的数据库。

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