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Longitudinal epigenetic and gene expression profiles analyzed by three-component analysis reveal down-regulation of genes involved in protein translation in human aging

机译:通过三成分分析法分析的纵向表观遗传和基因表达谱揭示了人类衰老过程中参与蛋白质翻译的基因的下调

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Data on biological mechanisms of aging are mostly obtained from cross-sectional study designs. An inherent disadvantage of this design is that inter-individual differences can mask small but biologically significant age-dependent changes. A serially sampled design (same individual at different time points) would overcome this problem but is often limited by the relatively small numbers of available paired samples and the statistics being used. To overcome these limitations, we have developed a new vector-based approach, termed three-component analysis, which incorporates temporal distance, signal intensity and variance into one single score for gene ranking and is combined with gene set enrichment analysis. We tested our method on a unique age-based sample set of human skin fibroblasts and combined genome-wide transcription, DNA methylation and histone methylation (H3K4me3 and H3K27me3) data. Importantly, our method can now for the first time demonstrate a clear age-dependent decrease in expression of genes coding for proteins involved in translation and ribosome function. Using analogies with data from lower organisms, we propose a model where age-dependent down-regulation of protein translation-related components contributes to extend human lifespan.
机译:关于衰老的生物学机制的数据主要来自横断面研究设计。这种设计的固有缺点是,个体间的差异可能掩盖了细微但生物学上重要的年龄依赖性变化。串行采样设计(在不同时间点使用相同的个体)可以解决此问题,但通常会受到可用配对样本和使用的统计数据相对较少的限制。为了克服这些局限性,我们开发了一种新的基于矢量的方法,称为三成分分析,该方法将时间距离,信号强度和方差合并到一个单一分数中进行基因排名,并与基因集富集分析相结合。我们在一组基于年龄的人类皮肤成纤维细胞样本上测试了我们的方法,并结合了全基因组转录,DNA甲基化和组蛋白甲基化(H3K4me3和H3K27me3)数据。重要的是,我们的方法现在可以首次证明与翻译和核糖体功能有关的蛋白质的编码基因的年龄明显下降。使用来自下层生物的数据的类比,我们提出了一个模型,其中依赖年龄的蛋白质翻译相关成分的下调有助于延长人类寿命。

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