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Loss of vacuolar acidity results in iron-sulfur cluster defects and divergent homeostatic responses during aging in Saccharomyces cerevisiae

Authors :
Chen, Kenneth L.
Ven, Toby N.
Crane, Matthew M.
Brunner, Matthew L. C.
Pun, Adrian K.
Helget, Kathleen L.
Brower, Katherine
Chen, Dexter E.
Doan, Ha
Dillard-Telm, Justin D.
Huynh, Ellen
Feng, Yen-Chi
Yan, Zili
Golubeva, Alexandra
Hsu, Roy A.
Knight, Raheem
Levin, Jessie
Mobasher, Vesal
Muir, Michael
Omokehinde, Victor
Screws, Corey
Tunali, Esin
Tran, Rachael K.
Valdez, Luz
Yang, Edward
Kennedy, Scott R.
Herr, Alan J.
Kaeberlein, Matt
Wasko, Brian M.
Source :
GeroScience; 20240101, Issue: Preprints p1-16, 16p
Publication Year :
2024

Abstract

The loss of vacuolar/lysosomal acidity is an early event during aging that has been linked to mitochondrial dysfunction. However, it is unclear how loss of vacuolar acidity results in age-related dysfunction. Through unbiased genetic screens, we determined that increased iron uptake can suppress the mitochondrial respiratory deficiency phenotype of yeast vmamutants, which have lost vacuolar acidity due to genetic disruption of the vacuolar ATPase proton pump. Yeast vmamutants exhibited nuclear localization of Aft1, which turns on the iron regulon in response to iron-sulfur cluster (ISC) deficiency. This led us to find that loss of vacuolar acidity with age in wild-type yeast causes ISC defects and a DNA damage response. Using microfluidics to investigate aging at the single-cell level, we observe grossly divergent trajectories of iron homeostasis within an isogenic and environmentally homogeneous population. One subpopulation of cells fails to mount the expected compensatory iron regulon gene expression program, and suffers progressively severe ISC deficiency with little to no activation of the iron regulon. In contrast, other cells show robust iron regulon activity with limited ISC deficiency, which allows extended passage and survival through a period of genomic instability during aging. These divergent trajectories suggest that iron regulation and ISC homeostasis represent a possible target for aging interventions.

Details

Language :
English
ISSN :
25092715 and 25092723
Issue :
Preprints
Database :
Supplemental Index
Journal :
GeroScience
Publication Type :
Periodical
Accession number :
ejs52231765
Full Text :
https://doi.org/10.1007/s11357-020-00159-3