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MitoTimer-based high-content screen identifies two chemically-related benzothiophene derivatives that enhance basal mitophagy

Authors :
Orian S. Shirihai
Eli C. Lewis
Haim Barr
Anton Petcherski
Guy Las
Essam A. Assali
Noga Kozer
Boris M. Baranovski
Roi Gazit
Dane M. Wolf
Fernanda M. Cerqueira
Yaelle Roth
Source :
Biochemical Journal. 477:461-475
Publication Year :
2020
Publisher :
Portland Press Ltd., 2020.

Abstract

Mitochondrial turnover is required for proper cellular function. Both mitochondrial biogenesis and mitophagy are impaired in several degenerative and age-related diseases. The search for mitophagy activators recently emerged as a new therapeutical approach; however, there is a lack in suitable tools to follow mitochondrial turnover in a high-throughput manner. We demonstrate that the fluorescent protein, MitoTimer, is a reliable and robust probe to follow mitochondrial turnover. The screening of 15 000 small molecules led us to two chemically-related benzothiophenes that stimulate basal mitophagy in the beta-cell line, INS1. Enhancing basal mitophagy was associated with improved mitochondrial function, higher Complex I activity and Complex II and III expressions in INS1 cells, as well as better insulin secretion performance in mouse islets. The possibility of further enhancing mitophagy in the absence of mitochondrial stressors points to the existence of a ‘basal mitophagy spare capacity'. To this end, we found two small molecules that can be used as models to better understand the physiological regulation of mitophagy.

Details

ISSN :
14708728 and 02646021
Volume :
477
Database :
OpenAIRE
Journal :
Biochemical Journal
Accession number :
edsair.doi.dedup.....382f432bf9c790682d69a09ecf3abfa9
Full Text :
https://doi.org/10.1042/bcj20190616