# Project 2: Chromatin, eigenome, and nuclear fidelity in senescence and aging

> **NIH NIH P01** · UNIVERSITY OF PENNSYLVANIA · 2020 · $383,573

## Abstract

Studies in animal models reveal that genetic differences and somatic mutations underlie longevity, but that 
non-genetic contributions also play a major role. Numerous observations, including our observations, suggest 
that epigenetic alterations occur as eukaryotes age. However, key questions remain, in particular, what are 
driving mechanisms and genomic changes that underlie the cellular phenotypes that characterize senescence 
and aging? Our hypothesis is that healthy aging involves homeostasis of the epigenomic landscape, which we 
refer to as chromostasis, and that chromostasis fails during aging, leading to tissue deterioration and to 
organismal death. Hence, genetic methods and pharmaco-therapeutics to enhance chromostasis are a 
prominent feature across all collaborative projects of this P01 application and in this Project 2. 
 During the previous funding period we showed a key functional role of chromatin alterations in yeast 
replicative aging and massive chromatin alterations in mammalian senescence. In the next funding period we 
will explore and elucidate new chromatin regulatory pathways that alter genomic function in senescence and 
aging, leading to loss of chromostasis. In preliminary studies, we newly identified chromatin regulators whose 
reduction extends replicative lifespan, leading to new pathways that maintain epigenome and transcriptome 
fidelity during aging. We also discovered that nuclear disruption and shedding of LADs/chromatin into the 
cytoplasm during senescence and aging is perceived by a canonical cytoplasmic DNA sensing pathway, 
cGAS-STING, which in turn triggers cellular immunity pathways and the SASP (the senescence associated 
secretory phenotype) leading eventually to tissue damage during aging. 
 To uncover the mechanisms and physiological importance of these new chromatin regulators and 
pathways in aging, we will carry out the following aims: 1. Investigate gene-internal cryptic transcriptional 
initiation during aging. We hypothesize that gene-internal transcriptional activation sites disrupt normal initiation 
at key longevity genes and lead to a global loss of transcriptional fidelity, contributing to reduction of 
chromostasis. (2) Investigate aging-associated upregulation of histone acetylation creating new enhancers. We 
hypothesize that dysregulated chromostasis licenses new enhancers during aging, leading to increased 
transcription of anti-longevity genes. (3) Investigate loss of chromatin integrity during aging triggering 
inflammation and autophagy of longevity chromatin regulators. Our preliminary findings show that 
LADs/chromatin in the cytoplasm triggers aging-promoting cellular immunity pathways via cGAS-STING. In the 
proposed studies, we will unravel the cGAS-STING pathway in promoting the SASP program in cellular 
senescence and the chronic inflammation associated with natural aging. 
 This research will yield novel epigenetic mechanisms altering longevity, with potential for new th...

## Key facts

- **NIH application ID:** 9950966
- **Project number:** 5P01AG031862-13
- **Recipient organization:** UNIVERSITY OF PENNSYLVANIA
- **Principal Investigator:** SHELLEY L BERGER
- **Activity code:** P01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $383,573
- **Award type:** 5
- **Project period:** — → —

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9950966

## Citation

> US National Institutes of Health, RePORTER application 9950966, Project 2: Chromatin, eigenome, and nuclear fidelity in senescence and aging (5P01AG031862-13). Retrieved via AI Analytics 2026-05-28 from https://api.ai-analytics.org/grant/nih/9950966. Licensed CC0.

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