Abstract

There is a growing body of evidence that epigenetic changes may not simply be a symptom of aging but an underlying cause (Brunet & Berger, 2014). In budding yeast, the reorganization of chromatin and resulting alterations in gene expression are known contributors to aging. In mammals, similar processes appear to be associated with aging but whether they truly cause aging is not yet known. In the last round of this grant, we provided evidence that chromatin factors such as Sir2 in yeast and SIRT1 in mammals, are key players in a process that suppresses epigenetic change and aging in eukaryotes. To provide a direct test of whether epigenetic change can actually cause aging in a mammal, we have generated a new mouse model called ?ICE?, for inducible changes in the epigenome. This mouse carries a tamoxifen- inducible endonuclease that induces non-mutagenic, site-specific DNA breaks (DSBs) at a few sites in the mammalian genome, thereby stimulating epigenetic change. We can induce change in any tissue at any time in a mouse's lifespan, then switch the system off, and monitor the effects on aging. Results to date are consistent with alterations to the epigenome being a fundamental cause of aging in mammals. This study is important, because it may explain long-standing questions about aging, such as why DNA repair defects and nuclear Lamin mutations both result in diseases that resemble premature aging. It will also address whether aging is uni-directional or reversible, and provide tools to screen for potent longevity interventions and to ?humanize? mouse models of disease.
In Aim 1, we utilize fibroblasts from ICE mice to elucidate the mechanisms that drive epigenetic changes and the effects they have on the resilience of cells to DNA damage and senescence. Advanced genomic technologies will allow us to map protein-binding, histone modifications, transcription profiles, DNA methylation patterns, and the evolution of nuclear architectures in 3D during aging.
In Aim 2, we test cause and effect in a living mammal by inducing epigenetic change in young mice and observing the effects on nuclear organization and the aging process.
In Aim 3, we test if epigenetic decay can be prevented or reversed using the latest genetic or pharmacological approaches. Together, this work will provide new information about whether alterations in chromatin structure promote aging in eukaryotes and explore ways that this knowledge can be exploited to improve the human condition.

Public Health Relevance

The increasing health burden of the world's aging population underscores the need to understand the biological mechanisms of aging and develop therapies to prolong our healthspan. There is emerging evidence that aging is due, in part, to a progressive disruption in how our DNA is packaged within the nucleus as a result of having to repair broken DNA. To test this hypothesis, we have generated a mouse called ?ICE? (for inducible changes in epigenetics) that allows us to disrupt DNA packaging and study its effects on cell senescence and aging, providing clues to why we age and a tool to discover interventions that may extend healthspan in humans.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
5R01AG019719-12
Application #
9519660
Study Section
Cellular Mechanisms in Aging and Development Study Section (CMAD)
Program Officer
Guo, Max
Project Start
2001-09-30
Project End
2022-05-31
Budget Start
2018-07-15
Budget End
2019-05-31
Support Year
12
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Harvard Medical School
Department
Pathology
Type
Schools of Medicine
DUNS #
047006379
City
Boston
State
MA
Country
United States
Zip Code

  Publications

Rajman, Luis; Chwalek, Karolina; Sinclair, David A (2018) Therapeutic Potential of NAD-Boosting Molecules: The In Vivo Evidence. Cell Metab 27:529-547
Das, Abhirup; Huang, George X; Bonkowski, Michael S et al. (2018) Impairment of an Endothelial NAD+-H2S Signaling Network Is a Reversible Cause of Vascular Aging. Cell 173:74-89.e20
Schultz, Michael B; Lu, Yuancheng; Braidy, Nady et al. (2018) Assays for NAD+-Dependent Reactions and NAD+ Metabolites. Methods Mol Biol 1813:77-90
Costford, Sheila R; Brouwers, Bram; Hopf, Meghan E et al. (2018) Skeletal muscle overexpression of nicotinamide phosphoribosyl transferase in mice coupled with voluntary exercise augments exercise endurance. Mol Metab 7:1-11
Longchamp, Alban; Mirabella, Teodelinda; Arduini, Alessandro et al. (2018) Amino Acid Restriction Triggers Angiogenesis via GCN2/ATF4 Regulation of VEGF and H2S Production. Cell 173:117-129.e14
Dai, Han; Sinclair, David A; Ellis, James L et al. (2018) Sirtuin activators and inhibitors: Promises, achievements, and challenges. Pharmacol Ther 188:140-154
Mitchell, Sarah J; Bernier, Michel; Aon, Miguel A et al. (2018) Nicotinamide Improves Aspects of Healthspan, but Not Lifespan, in Mice. Cell Metab 27:667-676.e4
Uddin, Golam Mezbah; Youngson, Neil A; Doyle, Bronte M et al. (2017) Nicotinamide mononucleotide (NMN) supplementation ameliorates the impact of maternal obesity in mice: comparison with exercise. Sci Rep 7:15063
Pollack, Rena M; Barzilai, Nir; Anghel, Valentin et al. (2017) Resveratrol Improves Vascular Function and Mitochondrial Number but Not Glucose Metabolism in Older Adults. J Gerontol A Biol Sci Med Sci 72:1703-1709
Mohamad, Mashani; Mitchell, Sarah Jayne; Wu, Lindsay Edward et al. (2016) Ultrastructure of the liver microcirculation influences hepatic and systemic insulin activity and provides a mechanism for age-related insulin resistance. Aging Cell 15:706-15

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