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表观遗传年龄与人类细胞衰老特征之间的关系。

The relationship between epigenetic age and the hallmarks of aging in human cells.

机构信息

Radiation Effects Department, Centre for Radiation, Chemical and Environmental Hazards, Public Health England, Chilton, Didcot, UK.

Present address: Altos Labs, Cambridge Institute of Science, Cambridge, UK.

出版信息

Nat Aging. 2022 Jun;2(6):484-493. doi: 10.1038/s43587-022-00220-0. Epub 2022 May 16.

Abstract

Epigenetic clocks are mathematically derived age estimators that are based on combinations of methylation values that change with age at specific CpGs in the genome. These clocks are widely used to measure the age of tissues and cells. The discrepancy between epigenetic age (EpiAge), as estimated by these clocks, and chronological age is referred to as EpiAge acceleration. Epidemiological studies have linked EpiAge acceleration to a wide variety of pathologies, health states, lifestyle, mental state and environmental factors, indicating that epigenetic clocks tap into critical biological processes that are involved in aging. Despite the importance of this inference, the mechanisms underpinning these clocks remained largely uncharacterized and unelucidated. Here, using primary human cells, we set out to investigate whether epigenetic aging is the manifestation of one or more of the aging hallmarks previously identified. We show that although epigenetic aging is distinct from cellular senescence, telomere attrition and genomic instability, it is associated with nutrient sensing, mitochondrial activity and stem cell composition.

摘要

表观遗传时钟是基于基因组中特定 CpG 位点的甲基化值随年龄变化的组合而得出的数学年龄估算器。这些时钟被广泛用于测量组织和细胞的年龄。这些时钟估算的表观遗传年龄(EpiAge)与实际年龄之间的差异被称为表观遗传年龄加速。流行病学研究将表观遗传年龄加速与多种病理、健康状况、生活方式、精神状态和环境因素联系起来,表明表观遗传时钟揭示了与衰老相关的关键生物学过程。尽管这种推断很重要,但这些时钟的潜在机制在很大程度上仍未被描述和阐明。在这里,我们使用原代人类细胞,着手研究表观遗传衰老是否是先前确定的一个或多个衰老标志的表现。我们表明,尽管表观遗传衰老与细胞衰老、端粒磨损和基因组不稳定性不同,但它与营养感应、线粒体活性和干细胞组成有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0dfa/10077971/42f410898c12/nihms-1877992-f0005.jpg

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