Mitochondrial heterogeneity and crosstalk in aging: Time for a paradigm shift?

Author:

Hinton Antentor O.1ORCID,Vue Zer1,Scudese Estevão1,Neikirk Kit1,Kirabo Annet2345,Montano Monty6ORCID

Affiliation:

1. Department of Molecular Physiology and Biophysics Vanderbilt University Nashville Tennessee USA

2. Department of Medicine Vanderbilt University Medical Center Nashville Tennessee USA

3. Vanderbilt Center for Immunobiology Nashville Tennessee USA

4. Immunology and Inflammation Vanderbilt Institute for Infection Nashville Tennessee USA

5. Vanderbilt Institute for Global Health Nashville Tennessee USA

6. Department of Medicine Harvard Medical School Boston Massachusetts USA

Abstract

AbstractThe hallmarks of aging have been influential in guiding the biology of aging research, with more recent and growing recognition of the interdependence of these hallmarks on age‐related health outcomes. However, a current challenge is personalizing aging trajectories to promote healthy aging, given the diversity of genotypes and lived experience. We suggest that incorporating heterogeneity—including intrinsic (e.g., genetic and structural) and extrinsic (e.g., environmental and exposome) factors and their interdependence of hallmarks—may move the dial. This editorial perspective will focus on one hallmark, namely mitochondrial dysfunction, to exemplify how consideration of heterogeneity and interdependence or crosstalk may reveal new perspectives and opportunities for personalizing aging research. To this end, we highlight heterogeneity within mitochondria as a model.

Funder

Vanderbilt Diabetes Research and Training Center, Vanderbilt University Medical Center

Clinical Center

United Negro College Fund

Chan Zuckerberg Initiative

Burroughs Wellcome Fund

Publisher

Wiley

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