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Differential DNA Methylation of MicroRNA Genes in Temporal Cortex from Alzheimers Disease Individuals

机译:阿尔茨海默氏病患者颞皮质中MicroRNA基因的差异DNA甲基化

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摘要

This study investigated for the first time the genomewide DNA methylation changes of noncoding RNA genes in the temporal cortex samples from individuals with Alzheimer's disease (AD). The methylome of 10 AD individuals and 10 age-matched controls were obtained using Illumina 450 K methylation array. A total of 2,095 among the 15,258 interrogated noncoding RNA CpG sites presented differential methylation, 161 of which were associated with miRNA genes. In particular, 10 miRNA CpG sites that were found to be hypermethylated in AD compared to control brains represent transcripts that have been previously associated with the disease. This miRNA set is predicted to target 33 coding genes from the neuregulin receptor complex (ErbB) signaling pathway, which is required for the neurons myelination process. For 6 of these miRNA genes (MIR9-1, MIR9-3, MIR181C, MIR124-1, MIR146B, and MIR451), the hypermethylation pattern is in agreement with previous results from literature that shows downregulation of miR-9, miR-181c, miR-124, miR-146b, and miR-451 in the AD brain. Our data implicate dysregulation of miRNA methylation as contributor to the pathogenesis of AD.
机译:这项研究首次调查了患有阿尔茨海默氏病(AD)的个体颞叶皮层样本中非编码RNA基因的全基因组DNA甲基化变化。使用Illumina 450 K甲基化阵列获得10位AD个体和10位年龄匹配的对照的甲基化组。在15258个被询问的非编码RNA CpG位点中,共有2,095个出现了甲基化差异,其中161个与miRNA基因相关。特别是,与对照大脑相比,在AD中被发现甲基化程度较高的10个miRNA CpG位点代表以前与疾病相关的转录本。预测该miRNA集可靶向神经调节蛋白复合物(ErbB)信号传导途径中的33个编码基因,这是神经元髓鞘形成过程所必需的。对于这些miRNA基因中的6个(MIR9-1,MIR9-3,MIR181C,MIR124-1,MIR146B和MIR451),超甲基化模式与文献中先前的结果一致,后者表明miR-9,miR-181c, AD脑中的miR-124,miR-146b和miR-451。我们的数据暗示miRNA甲基化失调是导致AD发病的原因。

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