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Triamterene induces autophagic degradation of lysosome by exacerbating lysosomal integrity

Na Yeon Park, Doo Sin Jo, Yong Hwan Kim, Ji-Eun Bae, Joon Bum Kim, Hyun Jun Park, Ji Yeon Choi, Ha Jung Lee, Jeong Ho Chang, Heeyoun Bunch, Hong Bae Jeon, Yong‐Keun Jung, Dong‐Hyung Cho

2021Archives of Pharmacal Research10 citationsDOIOpen Access PDF

Abstract

The maintenance of lysosomal integrity is essential for lysosome function and cell fate. Damaged lysosomes are degraded by lysosomal autophagy, lysophagy. The mechanism underlying lysophagy remains largely unknown; this study aimed to contribute to the understanding of this topic. A cell-based screening system was used to identify novel lysophagy modulators. Triamterene (6-phenylpteridine-2,4,7-triamine) was identified as one of the most potent lysophagy inducers from the screening process. We found that triamterene causes lysosomal rupture without affecting other cellular organelles and increases autophagy flux in HepG2 cells. Damaged lysosomes in triamterene-treated cells were removed by autophagy-mediated pathway, which was inhibited by depletion of the autophagy regulator, ATG5 or SQSTM1. In addition, treatment of triamterene decreased the integrity of lysosome and cell viability, which were rescued by removing the triamterene treatment in HepG2 cells. Hence, our data suggest that triamterene is a novel lysophagy inducer through the disruption of lysosomal integrity.

Topics & Concepts

AutophagyLysosomeTriamtereneCell biologyChemistryOrganelleInducerViability assayATG5CellBiochemistryBiologyEndocrinologyEnzymeApoptosisHydrochlorothiazideGeneBlood pressureAutophagy in Disease and TherapyCalcium signaling and nucleotide metabolismPlant Parasitism and Resistance
Triamterene induces autophagic degradation of lysosome by exacerbating lysosomal integrity | Litcius