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PURPL represses autophagic cell death to promote cutaneous melanoma by modulating ULK1 phosphorylation

Shuo Han, Xue Li, Ke Wang, Dingheng Zhu, Bingyao Meng, Jieyu Liu, Xiaoting Liang, Yi Jin, Xingyuan Liu, Qian Wen, Liang Zhou

2021Cell Death and Disease45 citationsDOIOpen Access PDF

Abstract

Uncontrolled overactivation of autophagy may lead to autophagic cell death, suppression of which is a pro-survival strategy for tumors. However, mechanisms involving key regulators in modulating autophagic cell death remain poorly defined. Here, we report a novel long noncoding RNA, p53 upregulated regulator of p53 levels (PURPL), functions as an oncogene to promote cell proliferation, colony formation, migration, invasiveness, and inhibits cell death in melanoma cells. Mechanistic studies showed that PURPL promoted mTOR-mediated ULK1 phosphorylation at Ser757 by physical interacting with mTOR and ULK1 to constrain autophagic response to avoid cell death. Loss of PURPL led to AMPK-mediated phosphorylation of ULK1 at Ser555 and Ser317 to over-activate autophagy and induce autophagic cell death. Our results identify PURPL as a key regulator to modulate the activity of autophagy initiation factor ULK1 to repress autophagic cell death in melanoma and may represent a potential intervention target for melanoma therapy.

Topics & Concepts

AutophagyProgrammed cell deathPI3K/AKT/mTOR pathwayCell biologyULK1Cancer researchRegulatorMelanomaBiologyPhosphorylationCell growthAMPKCellMechanistic target of rapamycinSignal transductionProtein kinase AApoptosisGeneticsGeneAutophagy in Disease and TherapyCancer-related molecular mechanisms researchToxoplasma gondii Research Studies