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. 2020 May 28;181(5):1176-1187.e16.
doi: 10.1016/j.cell.2020.04.025. Epub 2020 May 20.

Visualizing and Modulating Mitophagy for Therapeutic Studies of Neurodegeneration

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Visualizing and Modulating Mitophagy for Therapeutic Studies of Neurodegeneration

Hiroyuki Katayama et al. Cell. .

Abstract

Dysfunctional mitochondria accumulate in many human diseases. Accordingly, mitophagy, which removes these mitochondria through lysosomal degradation, is attracting broad attention. Due to uncertainties in the operational principles of conventional mitophagy probes, however, the specificity and quantitativeness of their readouts are disputable. Thorough investigation of the behaviors and fates of fluorescent proteins inside and outside lysosomes enabled us to develop an indicator for mitophagy, mito-SRAI. Through strict control of its mitochondrial targeting, we were able to monitor mitophagy in fixed biological samples more reproducibly than before. Large-scale image-based high-throughput screening led to the discovery of a hit compound that induces selective mitophagy of damaged mitochondria. In a mouse model of Parkinsons disease, we found that dopaminergic neurons selectively failed to execute mitophagy that promoted their survival within lesions. These results show that mito-SRAI is an essential tool for quantitative studies of mitochondrial quality control.

Keywords: FRET; Parkinsons disease; autophagy; fluorescent protein; high-throughput screening; lysosome; mitochondria; mitophagy.

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Conflict of interest statement

Declaration of Interests H. Katayama and A.M. are inventors on patent application PCT/JP2016/068189 submitted by RIKEN that covers the creation and use of SRAI/mito-SRAI.

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