| Literature DB >> 33562682 |
Viraj R Sanghvi1,2, Prathibha Mohan1, Kamini Singh1, Linlin Cao1,3, Marjan Berishaj1, Andrew L Wolfe1,4, Jonathan H Schatz1,5, Nathalie Lailler6, Elisa de Stanchina7, Agnes Viale6, Hans-Guido Wendel1.
Abstract
Inhibition of the eIF4A RNA helicase with silvestrol and related compounds is emerging as a powerful anti-cancer strategy. We find that a synthetic silvestrol analogue (CR-1-31 B) has nanomolar activity across many cancer cell lines. It is especially active against aggressive MYC+/BCL2+ B cell lymphomas and this likely reflects the eIF4A-dependent translation of both MYC and BCL2. We performed a genome-wide CRISPR/Cas9 screen and identified mechanisms of resistance to this new class of therapeutics. We identify three negative NRF2 regulators (KEAP1, CUL3, CAND1) whose inactivation is sufficient to cause CR1-31-B resistance. NRF2 is known to alter the oxidation state of translation factors and cause a broad increase in protein production. We find that NRF2 activation particularly increases the translation of some eIF4A-dependent mRNAs and restores MYC and BCL2 production. We know that NRF2 functions depend on removal of sugar adducts by the frutosamine-3-kinase (FN3K). Accordingly, loss of FN3K results in NRF2 hyper-glycation and inactivation and resensitizes cancer cells to eIF4A inhibition. Together, our findings implicate NRF2 in the translation of eIF4A-dependent mRNAs and point to FN3K inhibition as a new strategy to block NRF2 functions in cancer.Entities:
Keywords: G-quadruplex; KEAP1; NRF2; drug resistance; eIF4A; lymphoma; silvestrol
Year: 2021 PMID: 33562682 PMCID: PMC7915661 DOI: 10.3390/cancers13040639
Source DB: PubMed Journal: Cancers (Basel) ISSN: 2072-6694 Impact factor: 6.639