Nonlinear DNA methylation trajectories in aging male mice

Author:

Olecka MajaORCID,van Bömmel AlenaORCID,Best LenaORCID,Haase Madlen,Foerste Silke,Riege Konstantin,Dost ThomasORCID,Flor StefanoORCID,Witte Otto W.,Franzenburg SörenORCID,Groth MarcoORCID,von Eyss BjörnORCID,Kaleta ChristophORCID,Frahm Christiane,Hoffmann SteveORCID

Abstract

AbstractAlthough DNA methylation data yields highly accurate age predictors, little is known about the dynamics of this quintessential epigenomic biomarker during lifespan. To narrow the gap, we investigate the methylation trajectories of male mouse colon at five different time points of aging. Our study indicates the existence of sudden hypermethylation events at specific stages of life. Precisely, we identify two epigenomic switches during early-to-midlife (3-9 months) and mid-to-late-life (15-24 months) transitions, separating the rodents’ life into three stages. These nonlinear methylation dynamics predominantly affect genes associated with the nervous system and enrich in bivalently marked chromatin regions. Based on groups of nonlinearly modified loci, we construct a clock-like classifier STageR (STage of aging estimatoR) that accurately predicts murine epigenetic stage. We demonstrate the universality of our clock in an independent mouse cohort and with publicly available datasets.

Funder

Deutsche Forschungsgemeinschaft

Carl-Zeiss-Stiftung

Leibniz-Gemeinschaft

EC | Horizon 2020 Framework Programme

Publisher

Springer Science and Business Media LLC

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