# Epigenetic Dysregulation as a Driver of Skeletal Muscle Aging

> **NIH NIH F32** · HARVARD MEDICAL SCHOOL · 2020 · $64,926

## Abstract

ABSTRACT
 The “relocalization of chromatin modifiers” theory of aging postulates that the degenerative process of
aging is the result of a lifetime accumulation of epigenetic noise, which transcriptionally dysregulates cellular
signaling pathways, triggering symptoms of tissue dysfunction and health deterioration. Evidence suggests that
DNA methylation, in particular, may set the pace of the aging clock in several mammalian tissues, yet it is
unclear whether these changes are reversible. Skeletal muscle is a particular tissue of interest because of its
high metabolic load, biomass, and susceptibility to age-related dysfunction, termed sarcopenia.
 My approach is to first survey of the epigenomic landscape of individual nuclei isolated from young and
old mouse muscle using snATAC-seq and integrate snRNA-seq data to test whether regions of chromatin
accessibility in each discreet cell type correlate with gene expression from those regions. I will integrate whole
genome bisulfite sequencing with 5hmC capture data, to find CpG sites that are hydroxymethylated in young
muscle but remain methylated in old and see if these correlate with gene expression. To test the hypothesis
that age-associated muscle dysfunction is the result of changes in the epigenetic landscape that lead
to a TET2-driven loss of cellular identity, I will use the single nucleus and 5hmC data to determine if age-
associated changes to the epigenome are correlated with a loss of cellular identity, as measured by significant
changes to the transcriptomes of old muscle cells. Next, I will focus on the role of TET2 dioxygenase in adult
skeletal muscle from young and old animals. I will perform CHiP-seq to locate TET2 in healthy young muscle
and then determine if this localization is altered in old skeletal muscle. I will also test TET2 activity, including
5mC oxidation, and stability in culture and in vivo in old and young muscle, using AMPK and electrical
stimulation to increase TET2 activation. Finally, I will determine if age-associated muscle dysfunction is
reversible in vivo using epigenetic reprogramming. Our preliminary results show that OSK epigenetic
reprogramming dramatically enhances regeneration of terminally differentiated somatic cells (neurons) and
improves visual acuity in aged mice in a TET-dependent manner. Because epigenetic aging is seen broadly in
all tissues, I predict that the TET-dependent mechanism of OSK reprogramming is not limited to a single tissue
type, and that it may benefit aged skeletal muscle. I will treat young and old muscle cells in culture and muscle
tissue with OSK-AAV and measure myogenicity, repair after acute injury, muscle force and other hallmarks of
muscle aging. If my aims are achieved the field will benefit from my newly developed methods and integrative
analyses of single nucleus-based transcriptomic and epigenomic data. Moreover, the proposed experiments
will define the role of TET2 demethylation dynamics in aging muscle and determine if...

## Key facts

- **NIH application ID:** 10067089
- **Project number:** 1F32AG069363-01
- **Recipient organization:** HARVARD MEDICAL SCHOOL
- **Principal Investigator:** Amber Levell Mueller
- **Activity code:** F32 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $64,926
- **Award type:** 1
- **Project period:** 2020-09-01 → 2023-08-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10067089

## Citation

> US National Institutes of Health, RePORTER application 10067089, Epigenetic Dysregulation as a Driver of Skeletal Muscle Aging (1F32AG069363-01). Retrieved via AI Analytics 2026-05-23 from https://api.ai-analytics.org/grant/nih/10067089. Licensed CC0.

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