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

被引:0
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作者
Sylwia Kabacik
Donna Lowe
Leonie Fransen
Martin Leonard
Siew-Lan Ang
Christopher Whiteman
Sarah Corsi
Howard Cohen
Sarah Felton
Radhika Bali
Steve Horvath
Ken Raj
机构
[1] Public Health England,Radiation Effects Department, Centre for Radiation, Chemical and Environmental Hazards
[2] Chilton,Toxicology Department, Centre for Radiation, Chemical and Environmental Hazards
[3] Public Health England,Department of Dermatology
[4] Chilton,Department of Human Genetics, David Geffen School of Medicine
[5] The Francis Crick Institute,Department of Biostatistics, Fielding School of Public Health
[6] Elizabeth House Surgery,undefined
[7] Churchill Hospital,undefined
[8] University of California,undefined
[9] Los Angeles,undefined
[10] University of California,undefined
[11] Los Angeles,undefined
[12] Altos Labs,undefined
[13] Cambridge Institute of Science,undefined
[14] Altos Labs,undefined
[15] Cambridge Institute of Science,undefined
来源
Nature Aging | 2022年 / 2卷
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摘要
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 cells1,2. 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 factors2, 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 identified3. 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.
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页码:484 / 493
页数:9
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