Author
Listed:
- Francesca Rapino
(University of Liège
GIGA-institute, University of Liège)
- Sylvain Delaunay
(University of Liège
GIGA-institute, University of Liège)
- Florian Rambow
(KU Leuven
VIB)
- Zhaoli Zhou
(University of Liège
GIGA-institute, University of Liège)
- Lars Tharun
(University Hospital Cologne)
- Pascal Tullio
(University of Liège)
- Olga Sin
(Max Planck Institute for Molecular Biomedicine
University of Münster
University of Münster)
- Kateryna Shostak
(GIGA-institute, University of Liège
University of Liège)
- Sebastian Schmitz
(University of Liège
GIGA-institute, University of Liège)
- Jolanda Piepers
(Maastricht University)
- Bart Ghesquière
(VIB)
- Latifa Karim
(GIGA-institute, University of Liège
University of Liège)
- Benoit Charloteaux
(GIGA-institute, University of Liège
University of Liège)
- Diane Jamart
(University of Liège
GIGA-institute, University of Liège)
- Alexandra Florin
(University Hospital Cologne)
- Charles Lambert
(GIGA-institute, University of Liège)
- Andrée Rorive
(University of Liège)
- Guy Jerusalem
(University of Liège)
- Eleonora Leucci
(KU Leuven
VIB)
- Michael Dewaele
(KU Leuven
VIB)
- Marc Vooijs
(Maastricht University)
- Sebastian A. Leidel
(Max Planck Institute for Molecular Biomedicine
University of Münster
University of Münster)
- Michel Georges
(GIGA-institute, University of Liège
University of Liège)
- Marianne Voz
(GIGA-institute, University of Liège)
- Bernard Peers
(GIGA-institute, University of Liège)
- Reinhard Büttner
(University Hospital Cologne)
- Jean-Christophe Marine
(KU Leuven
VIB)
- Alain Chariot
(GIGA-institute, University of Liège
University of Liège
WELBIO, University of Liège)
- Pierre Close
(University of Liège
GIGA-institute, University of Liège
WELBIO, University of Liège)
Abstract
Reprogramming of mRNA translation has a key role in cancer development and drug resistance1. However, the molecular mechanisms that are involved in this process remain poorly understood. Wobble tRNA modifications are required for specific codon decoding during translation2,3. Here we show, in humans, that the enzymes that catalyse modifications of wobble uridine 34 (U34) tRNA (U34 enzymes) are key players of the protein synthesis rewiring that is induced by the transformation driven by the BRAFV600E oncogene and by resistance to targeted therapy in melanoma. We show that BRAFV600E-expressing melanoma cells are dependent on U34 enzymes for survival, and that concurrent inhibition of MAPK signalling and ELP3 or CTU1 and/or CTU2 synergizes to kill melanoma cells. Activation of the PI3K signalling pathway, one of the most common mechanisms of acquired resistance to MAPK therapeutic agents, markedly increases the expression of U34 enzymes. Mechanistically, U34 enzymes promote glycolysis in melanoma cells through the direct, codon-dependent, regulation of the translation of HIF1A mRNA and the maintenance of high levels of HIF1α protein. Therefore, the acquired resistance to anti-BRAF therapy is associated with high levels of U34 enzymes and HIF1α. Together, these results demonstrate that U34 enzymes promote the survival and resistance to therapy of melanoma cells by regulating specific mRNA translation.
Suggested Citation
Francesca Rapino & Sylvain Delaunay & Florian Rambow & Zhaoli Zhou & Lars Tharun & Pascal Tullio & Olga Sin & Kateryna Shostak & Sebastian Schmitz & Jolanda Piepers & Bart Ghesquière & Latifa Karim & , 2018.
"Codon-specific translation reprogramming promotes resistance to targeted therapy,"
Nature, Nature, vol. 558(7711), pages 605-609, June.
Handle:
RePEc:nat:nature:v:558:y:2018:i:7711:d:10.1038_s41586-018-0243-7
DOI: 10.1038/s41586-018-0243-7
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