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ID 115922
Author
Hashimoto, Eiichi The University of Tokyo
Okuno, Shota The University of Tokyo
Hirayama, Shoshiro The University of Tokyo
Arata, Yoshiyuki The University of Tokyo
Goto, Tsuyoshi The University of Tokyo
Hamazaki, Jun The University of Tokyo
Murata, Shigeo The University of Tokyo
Content Type
Journal Article
Description
The proteasome is a therapeutic target in cancer, but resistance to proteasome inhibitors often develops owing to the induction of compensatory pathways. Through a genome-wide siRNA screen combined with RNA sequencing analysis, we identified hexokinase and downstream O-GlcNAcylation as cell survival factors under proteasome impairment. The inhibition of O-GlcNAcylation synergistically induced massive cell death in combination with proteasome inhibition. We further demonstrated that O-GlcNAcylation was indispensable for maintaining proteasome activity by enhancing biogenesis as well as proteasome degradation in a manner independent of Nrf1, a well-known compensatory transcription factor that upregulates proteasome gene expression. Our results identify a pathway that maintains proteasome function under proteasome impairment, providing potential targets for cancer therapy.
Journal Title
iScience
ISSN
25890042
Publisher
Elsevier
Volume
23
Issue
7
Start Page
101299
Published Date
2020-07-24
Rights
This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
EDB ID
DOI (Published Version)
URL ( Publisher's Version )
FullText File
language
eng
TextVersion
Publisher
departments
Institute of Advanced Medical Sciences