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Suh, Pann-Ghill
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Resveratrol induces autophagy by directly inhibiting mTOR through ATP competition

Author(s)
Park, DohyunJeong, HeeyoonLee, Mi NamKoh, AraKwon, OhmanYang, Yong RyoulNoh, JungeunSuh, Pann-GhillPark, HwangseoRyu, Sung Ho
Issued Date
2016-02
DOI
10.1038/srep21772
URI
https://scholarworks.unist.ac.kr/handle/201301/18827
Fulltext
http://www.nature.com/articles/srep21772
Citation
SCIENTIFIC REPORTS, v.6, pp.21772
Abstract
Resveratrol (RSV) is a natural polyphenol that has a beneficial effect on health, and resveratrol-induced autophagy has been suggested to be a key process in mediating many beneficial effects of resveratrol, such as reduction of inflammation and induction of cancer cell death. Although various resveratrol targets have been suggested, the molecule that mediates resveratrol-induced autophagy remains unknown. Here, we demonstrate that resveratrol induces autophagy by directly inhibiting the mTOR-ULK1 pathway. We found that inhibition of mTOR activity and presence of ULK1 are required for autophagy induction by resveratrol. In line with this mTOR dependency, we found that resveratrol suppresses the viability of MCF7 cells but not of SW620 cells, which are mTOR inhibitor sensitive and insensitive cancer cells, respectively. We also found that resveratrol-induced cancer cell suppression occurred ULK1 dependently. For the mechanism of action of resveratrol on mTOR inhibition, we demonstrate that resveratrol directly inhibits mTOR. We found that resveratrol inhibits mTOR by docking onto the ATP-binding pocket of mTOR (i.e., it competes with ATP). We propose mTOR as a novel direct target of resveratrol, and inhibition of mTOR is necessary for autophagy induction
Publisher
NATURE PUBLISHING GROUP
ISSN
2045-2322
Keyword
ACTIVATED PROTEIN-KINASECELL-DEATHMAMMALIAN TARGETSKELETAL-MUSCLEAMPK ACTIVATIONPHOSPHORYLATIONSIRT1MECHANISMSIRTUINSCANCER

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