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Blood DNA Methylation and Aging: A Cross-Sectional Analysis and Longitudinal Validation in the InCHIANTI Study

机译:血液DNA甲基化和老化:春馨学研究中的横截面分析和纵向验证

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Changes in DNA methylation have been found to be highly correlated with aging in humans, but causes or consequences of these changes are not understood. We characterized the DNA methylomes of several hundred people in the Invecchiare in Chianti study to identify DNA sites in which percent methylation was systematically different with age. Then, we tested the hypothesis that changes of percent methylation in the same DNA sites occur longitudinally for the same DNA sites in the same subjects. We identified six differentially methylated regions in which percent methylation showed robust longitudinal changes in the same direction. We then describe functions of the genes near these differentially methylated regions and their potential relationship with aging, noting that the genes appear to regulate metabolism or cell type specificity. The nature of transcription factor binding sites in the vicinity of these differentially methylated regions suggest that these age-associated methylation changes reflect modulation of two biological mechanisms: the polycomb repressive complex 2, a protein complex that trimethylates histone H3 on lysine 27, and the transcriptional repressor CCCTC-binding factor or CTCF, both of which are regulators of chromatin architecture. These findings are consistent with the idea that changes in methylation with aging are of adaptive nature.
机译:DNA甲基化的变化已被发现与人类的衰老高度相关,但这些变化的原因或后果尚不清楚。我们在基安蒂的因维奇亚研究中对数百人的DNA甲基组进行了表征,以确定甲基化百分比随年龄系统性不同的DNA位点。然后,我们检验了同一受试者同一DNA位点的甲基化百分比发生纵向变化的假设。我们确定了六个差异甲基化区域,其中甲基化百分比在同一方向上表现出强烈的纵向变化。然后,我们描述了这些差异甲基化区域附近的基因的功能及其与衰老的潜在关系,并指出这些基因似乎可以调节代谢或细胞类型特异性。这些差异甲基化区域附近的转录因子结合位点的性质表明,这些年龄相关的甲基化变化反映了两种生物学机制的调节:多梳抑制复合物2,一种使赖氨酸27上的组蛋白H3三甲基化的蛋白质复合物,以及转录抑制物CCCTC结合因子或CTCF,它们都是染色质结构的调节器。这些发现与甲基化随年龄增长的变化具有适应性的观点是一致的。

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