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Genetics and genomics of human ageing

机译:人类衰老的遗传学和基因组学

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摘要

Ageing in humans is typified by the decline of physiological functions in various organs and tissues leading to an increased probability of death. Some individuals delay, escape or survive much of this age-related decline and live past age 100. Studies comparing centenarians to average-aged individuals have found polymorphisms in genes that are associated with long life, including APOE and FOXOA3, which have been replicated many times. However, the associations found in humans account for small percentages of the variance in lifespan and many other gene associations have not been replicated in additional populations. Therefore, ageing is probably a highly polygenic trait. In humans, it is important to also consider differences in age-related decline that occur within and among tissues. Longitudinal data of age-related traits can be used in association studies to test for polymorphisms that predict how an individual will change over time. Transcriptional and genetic association studies of different tissues have revealed common and unique pathways involved in human ageing. Genomic convergence is a method that combines multiple types of functional genomic information such as transcriptional profiling, expression quantitative trait mapping and gene association. The genomic convergence approach has been used to implicate the gene MMP20 in human kidney ageing. New human genetics technologies are continually in development and may lead to additional breakthroughs in human ageing in the near future.
机译:人类衰老的典型特征是各种器官和组织的生理功能下降,导致死亡的可能性增加。一些个体在这种与年龄有关的下降中大部分都延迟,逃避或生存,并且活到100岁以上。将百岁老人与平均年龄的个体进行比较的研究发现,与长寿相关的基因(包括APOE和FOXOA3)具有多态性,这些基因已被复制很多。次。然而,人类中发现的关联仅占寿命变异的很小百分比,许多其他基因关联尚未在其他人群中复制。因此,衰老可能是高度多基因性状。在人类中,重要的是还要考虑在组织内部和组织之间发生的与年龄相关的衰老的差异。年龄相关性状的纵向数据可用于关联研究中,以测试预测个体随时间变化的多态性。不同组织的转录和遗传关联研究已经揭示了人类衰老的共同和独特途径。基因组融合是一种结合多种类型的功能基因组信息的方法,例如转录谱,表达定量性状图谱和基因关联。基因组收敛方法已被用来暗示人类肾脏衰老中的基因MMP20。新的人类遗传学技术正在不断发展,并可能在不久的将来导致人类衰老的其他突破。

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