Journal
CELL REPORTS
Volume 35, Issue 13, Pages -Publisher
CELL PRESS
DOI: 10.1016/j.celrep.2021.109321
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Funding
- EMBO long-term fellowship [ALTF 1005-2015]
- Human Frontier Science Program long-term fellowship [LT000711/2016-L]
- University of California, Berkeley
- Tata Consultancy Services
- NIH [DP2 CA239597, R35CA242986]
- Goldberg-Benioff Endowed Professorship
- American Cancer Society [RP-19-181-01-RMC]
- American Cancer Society Research Professor Award
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eIF4E controls the translation of Tfeb, a key executor of the autophagy response; eIF4E has a functional interaction with Bcl-xL in tumor growth; eIF4E interacts with the exon-junction complex (EJC) to control the migratory properties of cancer cells.
The major cap-binding protein eukaryotic translation initiation factor 4E (eIF4E), an ancient protein required for translation of all eukaryotic genomes, is a surprising yet potent oncogenic driver. The genetic interactions that maintain the oncogenic activity of this key translation factor remain unknown. In this study, we carry out a genome-wide CRISPRi screen wherein we identify more than 600 genetic interactions that sustain eIF4E oncogenic activity. Our data show that eIF4E controls the translation of Tfeb, a key executer of the autophagy response. This autophagy survival response is triggered by mitochondrial proteotoxic stress, which allows cancer cell survival. Our screen also reveals a functional interaction between eIF4E and a single anti-apoptotic factor, Bcl-xL, in tumor growth. Furthermore, we show that eIF4E and the exon-junction complex (EJC), which is involved in many steps of RNA metabolism, interact to control the migratory properties of cancer cells. Overall, we uncover several cancer-specific vulnerabilities that provide further resolution of the cancer translatome.
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