Cellular aging in vitro recapitulates multi-tissue epigenetic aging in vivo

Minteer, Christopher J.; Morselli, Marco; Meer, Margarita; Cao, Jian; Higgins‐Chen, Albert; Lang, Sabine M.; Pellegrini, Matteo; Yan, Qin; Levine, Morgan E.

doi:10.1101/2020.09.02.280073

Cited by 2 publications

(4 citation statements)

References 100 publications

(123 reference statements)

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“…Consistent with other recent developments in aging clocks, we find that dimensionality reduction by PCA prior to regression functions well in constructing aging clocks ( Minteer et al, 2020 ). One drawback of PCA and linear regression methods is that they can only capture linear dependencies.…”

Section: Discussionsupporting

confidence: 90%

“…Fig S1]. When analyzing data from aging cohorts, age is expected to be the major source of biological aging within each cohort (genotype, treatment condition) ( Tarkhov et al, 2019 ; Minteer et al, 2020 ). Following transformation of all samples into principal component space, we therefore determined the linear correlation of each PC coordinate with age in both WT and mutant cohorts ( Figure 1 ).…”

Section: Resultsmentioning

confidence: 99%

“…Aging is therefore expected to be a major source of variance when analyzing data describing a biological system across its lifespan. PCA is a technique to identify correlated features or “directions” in feature space along which covariance is large and this can be exploited in the construction of clocks and classifiers ( Tarkhov et al, 2019 ; Minteer et al, 2020 ).…”

Section: Discussionmentioning

confidence: 99%

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LipidClock: A Lipid-Based Predictor of Biological Age

Unfried

Cazenave-Gassiot

et al. 2022

Front. Aging

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Complexity is a fundamental feature of biological systems. Omics techniques like lipidomics can simultaneously quantify many thousands of molecules, thereby directly capturing the underlying biological complexity. However, this approach transfers the original biological complexity to the resulting datasets, posing challenges in data reduction and analysis. Aging is a prime example of a process that exhibits complex behaviour across multiple scales of biological organisation. The aging process is characterised by slow, cumulative and detrimental changes that are driven by intrinsic biological stochasticity and mediated through non-linear interactions and feedback within and between these levels of organization (ranging from metabolites, macromolecules, organelles and cells to tissue and organs). Only collectively and over long timeframes do these changes manifest as the exponential increases in morbidity and mortality that define biological aging, making aging a problem more difficult to study than the aetiologies of specific diseases. But aging’s time dependence can also be exploited to extract key insights into its underlying biology. Here we explore this idea by using data on changes in lipid composition across the lifespan of an organism to construct and test a LipidClock to predict biological age in the nematode Caenorhabdits elegans. The LipidClock consist of a feature transformation via Principal Component Analysis followed by Elastic Net regression and yields and Mean Absolute Error of 1.45 days for wild type animals and 4.13 days when applied to mutant strains with lifespans that are substantially different from that of wild type. Gompertz aging rates predicted by the LipidClock can be used to simulate survival curves that are in agreement with those from lifespan experiments.

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Section: Discussionsupporting

confidence: 90%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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LipidClock: A Lipid-Based Predictor of Biological Age

Unfried

Cazenave-Gassiot

et al. 2022

Front. Aging

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“…It was particularly important to address the question of the relationship between epigenetic aging and cellular senescence, as previous reports were equivocal in their conclusions 31 , 33 , 34 . Here, using primary cells from many individual donors, the results are clear that cellular senescence, although undoubtedly a major contributor to the aging phenotype, is not associated with epigenetic aging, as measured by the Skin&blood clock.…”

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confidence: 99%

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

et al. 2022

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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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Cellular aging in vitro recapitulates multi-tissue epigenetic aging in vivo

Cited by 2 publications

References 100 publications

LipidClock: A Lipid-Based Predictor of Biological Age

LipidClock: A Lipid-Based Predictor of Biological Age

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

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