Metabolic stress regulates ERK activity by controlling KSR-RAF heterodimerization

Amandine Verlande; Michaela Krafčíková; David Potěšil; Lukáš Trantírek; Zbyněk Zdráhal; Moustafa Elkalaf; Jan Trnka; Karel Souček; Nora Rauch; Jens Rauch; Walter Kolch; Stjepan Uldrijan

doi:10.15252/embr.201744524

Metabolic stress regulates ERK activity by controlling KSR-RAF heterodimerization

EMBO Rep. 2018 Feb;19(2):320-336. doi: 10.15252/embr.201744524. Epub 2017 Dec 20.

Authors

Amandine Verlande^{1

2}, Michaela Krafčíková³, David Potěšil³, Lukáš Trantírek³, Zbyněk Zdráhal³, Moustafa Elkalaf⁴, Jan Trnka⁴, Karel Souček^{1

5

6}, Nora Rauch^{7

8

9}, Jens Rauch^{7

8

9}, Walter Kolch^{7

8

9}, Stjepan Uldrijan^{10

2}

Affiliations

¹ International Clinical Research Center, St. Anne's University Hospital, Brno, Czech Republic.
² Department of Biology, Faculty of Medicine, Masaryk University, Brno, Czech Republic.
³ Central European Institute of Technology, Masaryk University, Brno, Czech Republic.
⁴ Laboratory for Metabolism and Bioenergetics, Third Faculty of Medicine, Charles University, Prague, Czech Republic.
⁵ Laboratory of Cytokinetics, Institute of Biophysics, Academy of Sciences, Brno, Czech Republic.
⁶ Department of Experimental Biology, Faculty of Science, Masaryk University, Brno, Czech Republic.
⁷ Systems Biology Ireland, University College Dublin, Dublin, Ireland.
⁸ Conway Institute, University College Dublin, Dublin, Ireland.
⁹ School of Medicine, University College Dublin, Dublin, Ireland.
¹⁰ International Clinical Research Center, St. Anne's University Hospital, Brno, Czech Republic uldrijan@med.muni.cz.

Abstract

Altered cell metabolism is a hallmark of cancer, and targeting specific metabolic nodes is considered an attractive strategy for cancer therapy. In this study, we evaluate the effects of metabolic stressors on the deregulated ERK pathway in melanoma cells bearing activating mutations of the NRAS or BRAF oncogenes. We report that metabolic stressors promote the dimerization of KSR proteins with CRAF in NRAS-mutant cells, and with oncogenic BRAF in BRAF^V600E-mutant cells, thereby enhancing ERK pathway activation. Despite this similarity, the two genomic subtypes react differently when a higher level of metabolic stress is induced. In NRAS-mutant cells, the ERK pathway is even more stimulated, while it is strongly downregulated in BRAF^V600E-mutant cells. We demonstrate that this is caused by the dissociation of mutant BRAF from KSR and is mediated by activated AMPK. Both types of ERK regulation nevertheless lead to cell cycle arrest. Besides studying the effects of the metabolic stressors on ERK pathway activity, we also present data suggesting that for efficient therapies of both genomic melanoma subtypes, specific metabolic targeting is necessary.

Keywords: RAF‐ERK signaling; cell cycle arrest; cell survival; melanoma; metabolic stress.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

14-3-3 Proteins / chemistry
14-3-3 Proteins / metabolism
Cell Cycle Checkpoints / genetics
Cell Line, Tumor
Enzyme Activation
Extracellular Signal-Regulated MAP Kinases / metabolism*
GTP Phosphohydrolases / genetics
GTP Phosphohydrolases / metabolism
Glucose / metabolism
Glycolysis
Humans
Melanoma / genetics
Melanoma / metabolism
Membrane Proteins / genetics
Membrane Proteins / metabolism
Mutation
Oxygen Consumption
Protein Kinases / chemistry
Protein Kinases / genetics
Protein Kinases / metabolism*
Protein Multimerization*
Recombinant Fusion Proteins
Stress, Physiological*
raf Kinases / chemistry
raf Kinases / genetics
raf Kinases / metabolism*

Substances

14-3-3 Proteins
Membrane Proteins
Recombinant Fusion Proteins
Protein Kinases
KSR-1 protein kinase
raf Kinases
Extracellular Signal-Regulated MAP Kinases
GTP Phosphohydrolases
NRAS protein, human
Glucose