Brusati Alberto, Peverelli Silvia, Calzari Luciano, Tiloca Cinzia, Casiraghi Valeria, Sorce Marta Nice, Invernizzi Sabrina, Carbone Erika, Cavagnola Rebecca, Verde Federico, Silani Vincenzo, Ticozzi Nicola, Ratti Antonia, Gentilini Davide
Department of Brain and Behavioral Sciences, University of Pavia, Pavia, Italy.
Department of Neurology and Laboratory of Neuroscience, IRCCS Istituto Auxologico Italiano, Milan, Italy.
Front Aging Neurosci. 2023 Nov 27;15:1272135. doi: 10.3389/fnagi.2023.1272135. eCollection 2023.
During the last decades, our knowledge about the genetic architecture of sporadic amyotrophic lateral sclerosis (sALS) has significantly increased. However, besides the recognized genetic risk factors, also the environment is supposed to have a role in disease pathogenesis. Epigenetic modifications reflect the results of the interaction between environmental factors and genes and may play a role in the development and progression of ALS. A recent epigenome-wide association study (EWAS) in blood identified differentially methylated positions mapping to 42 genes involved in cholesterol biosynthesis and immune-related pathways. Here we performed a genome-wide DNA methylation analysis in the blood of an Italian cohort of 61 sALS patients and 61 healthy controls. Initially, a conventional genome-wide association analysis was performed, and results were subsequently integrated with the findings from the previous EWAS using a meta-analytical approach. To delve deeper into the significant outcomes, over-representation analysis (ORA) was employed. Moreover, the epigenetic signature obtained from the meta-analysis was examined to determine potential associations with chemical compounds, utilizing the Toxicogenomic Database. Expanding the scope of the epigenetic analysis, we explored both epigenetic drift and rare epivariations. Notably, we observed an elevated epigenetic drift in sALS patients compared to controls, both at a global and single gene level. Interestingly, epigenetic drift at a single gene level revealed an enrichment of genes related to the neurotrophin signaling pathway. Moreover, for the first time, we identified rare epivariations exclusively enriched in sALS cases associated with 153 genes, 88 of whom with a strong expression in cerebral areas. Overall, our study reinforces the evidence that epigenetics may contribute to the pathogenesis of ALS and that epigenetic drift may be a useful diagnostic marker. Moreover, this study suggests the potential role of epivariations in ALS.
在过去几十年中,我们对散发性肌萎缩侧索硬化症(sALS)遗传结构的了解显著增加。然而,除了已确认的遗传风险因素外,环境因素在疾病发病机制中也被认为起到一定作用。表观遗传修饰反映了环境因素与基因之间相互作用的结果,可能在肌萎缩侧索硬化症的发生和发展中发挥作用。最近一项针对血液的全表观基因组关联研究(EWAS)确定了与42个参与胆固醇生物合成和免疫相关途径的基因映射的差异甲基化位点。在此,我们对61例sALS患者和61例健康对照组成的意大利队列的血液进行了全基因组DNA甲基化分析。首先,进行了常规的全基因组关联分析,随后使用荟萃分析方法将结果与先前EWAS的结果进行整合。为了更深入地研究显著结果,采用了过度表达分析(ORA)。此外,利用毒理基因组数据库检查了荟萃分析获得的表观遗传特征,以确定与化学化合物的潜在关联。为了扩大表观遗传分析的范围,我们探索了表观遗传漂移和罕见的表观变异。值得注意的是,我们观察到与对照组相比,sALS患者在整体和单基因水平上的表观遗传漂移都有所增加。有趣的是,单基因水平的表观遗传漂移显示出与神经营养因子信号通路相关的基因富集。此外,我们首次确定了仅在sALS病例中富集的与153个基因相关的罕见表观变异,其中88个在脑区有强烈表达。总体而言,我们的研究强化了表观遗传学可能有助于肌萎缩侧索硬化症发病机制的证据,并且表观遗传漂移可能是一个有用的诊断标志物。此外,这项研究表明表观变异在肌萎缩侧索硬化症中的潜在作用。
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