# Integrative Omics to enhance therapeutics development for healthy aging

> **NIH NIH UH3** · TRANSLATIONAL GENOMICS RESEARCH INST · 2023 · $878,314

## Abstract

ABSTRACT/SUMMARY
A number of drugs and interventions have been identified that curb morbidities associated with individual age-
related diseases, and a few compounds have been identified that increase longevity in mice and other non-
human species. However, few, if any, have been definitively shown to work by slowing the aging process and
thereby simultaneously delaying the onset of multiple diseases and ultimately extending human longevity.
Thus, current searches for drug and intervention targets that can lead to the development of longevity-
enhancing `geroprotectors,' i.e., interventions which stave off multiple age-related diseases and increase
longevity by slowing or disrupting aspects of the aging process, need to be improved. Only very integrated
approaches are likely to lead to successful searches given the need to reconcile complexities surrounding the
pathogenesis of age-related diseases with processes contributing to the synchronized decay of multiple
systems that defines aging. We believe that such integration can be achieved practically by: 1. pursuing
multiple human longitudinal studies focusing on the discovery of metabolites and proteins associated with a
biologically-compelling definition of slow and healthy human aging in different tissues; 2. exploiting novel cross-
species longevity studies involving multiple tissues to obtain insights into conserved pathways impacting
longevity whose elements may be consistent with factors discovered in human studies and hence validate
them as truly related to longevity and not just disease; and 3. aggregating data arising from items 1-2 along
with relevant available public domain data to generate/validate hypotheses, in addition to pursuing a GWAS to
identify protective factors for disease and using novel statistical and inferential methods. Our proposed studies
are some of the first to champion the notion that the `triangulation' of disparate scientific studies and
discoveries, i.e., the attempt to unify results from different study designs based on their biological coherence, is
the optimal way to advance identification of human targets for longevity-enhancing geroprotective drugs and
interventions. Importantly, although we believe that each of the individual studies we are proposing is itself
powerful enough to identify potential geroprotector targets, their collective and integrated use with novel
analytic methods will have unprecedented power and provide a paradigm for anti-aging drug discovery
research within the academic community. For example, we are proposing the first human longitudinal study to
search for druggable factors associated with the epigenetic clock and other validated measures of the aging
rate/healthy aging in thousands of individuals; the largest metabolomics and proteomic cross-species multi-
tissue study (N=60 species) of factors associated with lifespan; the largest human longitudinal comparative
tissue study of aging exploring blood, muscle, fat and skin samples; ...

## Key facts

- **NIH application ID:** 10693877
- **Project number:** 5UH3AG064706-05
- **Recipient organization:** TRANSLATIONAL GENOMICS RESEARCH INST
- **Principal Investigator:** RICHARD A MILLER
- **Activity code:** UH3 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2023
- **Award amount:** $878,314
- **Award type:** 5
- **Project period:** 2019-09-15 → 2025-08-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10693877

## Citation

> US National Institutes of Health, RePORTER application 10693877, Integrative Omics to enhance therapeutics development for healthy aging (5UH3AG064706-05). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/10693877. Licensed CC0.

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