Mifepristone and rapamycin have non-additive benefits for life span in mated female .

Fly (Austin)

Molecular and Computational Biology Section, Department of Biological Sciences, University of Southern California, Los Angeles, CA, USA.

Published: December 2024

AI Article Synopsis

  • Mifepristone and rapamycin were tested for their ability to extend the life span of mated female subjects, with rapamycin showing an optimal concentration of 50 μM increasing life span by 81%, while mifepristone at 466 μM increased life span by 114%.
  • Combining the two drugs did not enhance life span further and, in fact, decreased it relative to using either drug alone.
  • Both drugs were effective at reducing mating-induced midgut hypertrophy and activated a mitophagy reporter, suggesting they may work through a similar mechanism to promote longevity by enhancing mitophagy and reducing midgut enlargement.

Article Abstract

The drugs mifepristone and rapamycin were compared for their relative ability to increase the life span of mated female . Titration of rapamycin indicated an optimal concentration of approximately 50 μM, which increased median life span here by average +81%. Meta-analysis of previous mifepristone titrations indicated an optimal concentration of approximately 466 μM, which increased median life span here by average +114%. Combining mifepristone with various concentrations of rapamycin did not produce further increases in life span, and instead reduced life span relative to either drug alone. Assay of maximum midgut diameter indicated that rapamycin was equally efficacious as mifepristone in reducing mating-induced midgut hypertrophy. The mito-QC mitophagy reporter is a previously described green fluorescent protein (GFP)-mCherry fusion protein targeted to the outer mitochondrial membrane. Inhibition of GFP fluorescence by the acidic environment of the autophagolysosome yields an increased red/green fluorescence ratio indicative of increased mitophagy. Creation of a multi-copy mito-QC reporter strain facilitated assay in live adult flies, as well as in dissected midgut tissue. Mifepristone was equally efficacious as rapamycin in activating the mito-QC mitophagy reporter in the adult female fat-body and midgut. The data suggest that mifepristone and rapamycin act through a common pathway to increase mated female life span, and implicate increased mitophagy and decreased midgut hypertrophy in that pathway.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11514543PMC
http://dx.doi.org/10.1080/19336934.2024.2419151DOI Listing

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