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Analysis of Nonlinear Gene Expression Progression Reveals Extensive Pathway and Age-Specific Transitions in Aging Human Brains

机译:非线性基因表达过程的分析揭示了衰老的人类大脑中广泛的途径和特定年龄的转变

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摘要

Several recent gene expression studies identified hundreds of genes that are correlated with age in brain and other tissues in human. However, these studies used linear models of age correlation, which are not well equipped to model abrupt changes associated with particular ages. We developed a computational algorithm for age estimation in which the expression of each gene is treated as a dichotomized biomarker for whether the subject is older or younger than a particular age. In addition, for each age-informative gene our algorithm identifies the age threshold with the most drastic change in expression level, which allows us to associate genes with particular age periods. Analysis of human aging brain expression datasets from three frontal cortex regions showed that different pathways undergo transitions at different ages, and the distribution of pathways and age thresholds varies across brain regions. Our study reveals age-correlated expression changes at particular age points and allows one to estimate the age of an individual with better accuracy than previously published methods.
机译:最近的几项基因表达研究确定了数百种与人类大脑和其他组织的年龄相关的基因。但是,这些研究使用了年龄相关性的线性模型,这些模型不能很好地模拟与特定年龄相关的突变。我们开发了一种用于年龄估算的计算算法,该算法将每个基因的表达视为受试者年龄大于或小于特定年龄的二分生物标记。此外,对于每个年龄信息基因,我们的算法都可以识别出表达水平发生最剧烈变化的年龄阈值,从而使我们能够将基因与特定年龄段相关联。对来自三个额叶皮层区域的人类衰老大脑表达数据集的分析表明,不同的路径在不同的年龄经历转变,并且路径的分布和年龄阈值在整个大脑区域之间变化。我们的研究揭示了在特定年龄点的与年龄相关的表达变化,并使人们能够以比以前发表的方法更高的准确性估算一个人的年龄。

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