# A novel approach to understand a mechanism of proteostatic decline with aging

> **NIH NIH R56** · OKLAHOMA MEDICAL RESEARCH FOUNDATION · 2020 · $767,685

## Abstract

SUMMARY
Proteostatic quality control mechanisms fail with advancing age, resulting in the accumulation of damaged and
dysfunctional proteins. Protein breakdown and replacement with synthesis of new proteins (collectively referred
to as protein turnover) is the primary mechanism to mitigate accumulation of damaged proteins over time, and
is thus a critical proteostatic mechanism. As proteostatic mechanisms are highly relevant to the biology of ag-
ing and interventions targeted to increase healthspan, a more accurate assessment of the components of pro-
teostasis will provide important insights into their mechanisms. The overall goal of this project is to use a novel
approach to overcome barriers to progress in understanding protein turnover with aging and to reveal mecha-
nisms of cell-specific proteostatic processes. For the last decade we have developed stable isotope approach-
es to understand the mechanistic underpinnings of protein turnover in proteostasis. This proposal identifies
three physiological mechanisms that are often unaccounted for when designing studies of protein turnover and
aging: 1) content and half-lives of individual proteins vary by orders of magnitude, 2) the proliferative capacity
of a cell type impacts protein turnover measurements, and 3) that proteins can become resistant to breakdown
(e.g. aggregation or cross bridging), which changes the size of the dynamic protein pool. Technological ad-
vancements allow us to overcome these previous limitations and definitively address protein turnover with ag-
ing and treatments (rapamycin and caloric restriction (CR)) that increase health- lifespan. The proposed project
will use the newly described Nuclear tagging and Translating Ribosome Affinity Purification (NuTRAP) mouse,
targeted proteomics, and novel deuterium oxide (D2O) labeling to examine cell-type-specific individual protein
turnover and replication. This study leverages the cell-type specificity of NuTRAP x Cre mice to examine three
cell types in brain and three cell types in skeletal muscle. Examination of a mix of proliferative and non-
proliferative cell types within each tissue will help determine how changes in protein turnover contribute to de-
clining proteostasis with age, and if treatments that slow aging (rapamycin and CR) maintain proteostasis
through improved protein turnover. The hypotheses are that: 1) with aging, heterogeneous changes in protein
turnover by protein, cell, and tissue cause a loss of proteostasis and decreased dynamic protein pool size, and
2) in brain and skeletal muscle, rapamycin and CR will increase, not decrease, turnover of key aging-related
proteins, decrease replication of proliferative cell types, and maintain a larger dynamic protein pool. By using
approaches designed to specifically address mechanisms that are traditionally unaccounted for, as well as a
predictive bioinformatics approach, it is expected that the completion of this project will overcome a significant
barrier in ...

## Key facts

- **NIH application ID:** 10229298
- **Project number:** 1R56AG067754-01A1
- **Recipient organization:** OKLAHOMA MEDICAL RESEARCH FOUNDATION
- **Principal Investigator:** Benjamin Francis Miller
- **Activity code:** R56 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $767,685
- **Award type:** 1
- **Project period:** 2020-09-30 → 2022-04-30

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10229298

## Citation

> US National Institutes of Health, RePORTER application 10229298, A novel approach to understand a mechanism of proteostatic decline with aging (1R56AG067754-01A1). Retrieved via AI Analytics 2026-05-27 from https://api.ai-analytics.org/grant/nih/10229298. Licensed CC0.

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