AMPK promotes survival of c-Myc-positive melanoma cells by suppressing oxidative stress

Alain Kfoury; Marzia Armaro; Caterina Collodet; Jessica Sordet-Dessimoz; Maria Pilar Giner; Stefan Christen; Sofia Moco; Marion Leleu; Laurence de Leval; Ute Koch; Andreas Trumpp; Kei Sakamoto; Friedrich Beermann; Freddy Radtke

doi:10.15252/embj.201797673

AMPK promotes survival of c-Myc-positive melanoma cells by suppressing oxidative stress

Alain Kfoury, Marzia Armaro, Caterina Collodet, Jessica Sordet-Dessimoz, Maria Pilar Giner, Stefan Christen, Sofia Moco, Marion Leleu, Laurence de Leval, Ute Koch, Andreas Trumpp, Kei Sakamoto, Friedrich Beermann, Freddy Radtke^*

^*Corresponding author af dette arbejde

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

36 Citationer (Scopus)

Abstract

Although c-Myc is essential for melanocyte development, its role in cutaneous melanoma, the most aggressive skin cancer, is only partly understood. Here we used the Nras^Q61KINK4a^−/− mouse melanoma model to show that c-Myc is essential for tumor initiation, maintenance, and metastasis. c-Myc-expressing melanoma cells were preferentially found at metastatic sites, correlated with increased tumor aggressiveness and high tumor initiation potential. Abrogation of c-Myc caused apoptosis in primary murine and human melanoma cells. Mechanistically, c-Myc-positive melanoma cells activated and became dependent on the metabolic energy sensor AMP-activated protein kinase (AMPK), a metabolic checkpoint kinase that plays an important role in energy and redox homeostasis under stress conditions. AMPK pathway inhibition caused apoptosis of c-Myc-expressing melanoma cells, while AMPK activation protected against cell death of c-Myc-depleted melanoma cells through suppression of oxidative stress. Furthermore, TCGA database analysis of early-stage human melanoma samples revealed an inverse correlation between C-MYC and patient survival, suggesting that C-MYC expression levels could serve as a prognostic marker for early-stage disease.

Originalsprog	Engelsk
Artikelnummer	e97673
Tidsskrift	EMBO Journal
Vol/bind	37
Udgave nummer	5
ISSN	0261-4189
DOI	https://doi.org/10.15252/embj.201797673
Status	Udgivet - 1 mar. 2018
Udgivet eksternt	Ja

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10.15252/embj.201797673

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Citationsformater

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title = "AMPK promotes survival of c-Myc-positive melanoma cells by suppressing oxidative stress",

abstract = "Although c-Myc is essential for melanocyte development, its role in cutaneous melanoma, the most aggressive skin cancer, is only partly understood. Here we used the NrasQ61KINK4a−/− mouse melanoma model to show that c-Myc is essential for tumor initiation, maintenance, and metastasis. c-Myc-expressing melanoma cells were preferentially found at metastatic sites, correlated with increased tumor aggressiveness and high tumor initiation potential. Abrogation of c-Myc caused apoptosis in primary murine and human melanoma cells. Mechanistically, c-Myc-positive melanoma cells activated and became dependent on the metabolic energy sensor AMP-activated protein kinase (AMPK), a metabolic checkpoint kinase that plays an important role in energy and redox homeostasis under stress conditions. AMPK pathway inhibition caused apoptosis of c-Myc-expressing melanoma cells, while AMPK activation protected against cell death of c-Myc-depleted melanoma cells through suppression of oxidative stress. Furthermore, TCGA database analysis of early-stage human melanoma samples revealed an inverse correlation between C-MYC and patient survival, suggesting that C-MYC expression levels could serve as a prognostic marker for early-stage disease.",

keywords = "AMPK, c-Myc, gene targeting, melanoma, oxidative stress",

author = "Alain Kfoury and Marzia Armaro and Caterina Collodet and Jessica Sordet-Dessimoz and Giner, {Maria Pilar} and Stefan Christen and Sofia Moco and Marion Leleu and {de Leval}, Laurence and Ute Koch and Andreas Trumpp and Kei Sakamoto and Friedrich Beermann and Freddy Radtke",

year = "2018",

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doi = "10.15252/embj.201797673",

language = "English",

volume = "37",

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issn = "0261-4189",

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TY - JOUR

T1 - AMPK promotes survival of c-Myc-positive melanoma cells by suppressing oxidative stress

AU - Kfoury, Alain

AU - Armaro, Marzia

AU - Collodet, Caterina

AU - Sordet-Dessimoz, Jessica

AU - Giner, Maria Pilar

AU - Christen, Stefan

AU - Moco, Sofia

AU - Leleu, Marion

AU - de Leval, Laurence

AU - Koch, Ute

AU - Trumpp, Andreas

AU - Sakamoto, Kei

AU - Beermann, Friedrich

AU - Radtke, Freddy

PY - 2018/3/1

Y1 - 2018/3/1

N2 - Although c-Myc is essential for melanocyte development, its role in cutaneous melanoma, the most aggressive skin cancer, is only partly understood. Here we used the NrasQ61KINK4a−/− mouse melanoma model to show that c-Myc is essential for tumor initiation, maintenance, and metastasis. c-Myc-expressing melanoma cells were preferentially found at metastatic sites, correlated with increased tumor aggressiveness and high tumor initiation potential. Abrogation of c-Myc caused apoptosis in primary murine and human melanoma cells. Mechanistically, c-Myc-positive melanoma cells activated and became dependent on the metabolic energy sensor AMP-activated protein kinase (AMPK), a metabolic checkpoint kinase that plays an important role in energy and redox homeostasis under stress conditions. AMPK pathway inhibition caused apoptosis of c-Myc-expressing melanoma cells, while AMPK activation protected against cell death of c-Myc-depleted melanoma cells through suppression of oxidative stress. Furthermore, TCGA database analysis of early-stage human melanoma samples revealed an inverse correlation between C-MYC and patient survival, suggesting that C-MYC expression levels could serve as a prognostic marker for early-stage disease.

AB - Although c-Myc is essential for melanocyte development, its role in cutaneous melanoma, the most aggressive skin cancer, is only partly understood. Here we used the NrasQ61KINK4a−/− mouse melanoma model to show that c-Myc is essential for tumor initiation, maintenance, and metastasis. c-Myc-expressing melanoma cells were preferentially found at metastatic sites, correlated with increased tumor aggressiveness and high tumor initiation potential. Abrogation of c-Myc caused apoptosis in primary murine and human melanoma cells. Mechanistically, c-Myc-positive melanoma cells activated and became dependent on the metabolic energy sensor AMP-activated protein kinase (AMPK), a metabolic checkpoint kinase that plays an important role in energy and redox homeostasis under stress conditions. AMPK pathway inhibition caused apoptosis of c-Myc-expressing melanoma cells, while AMPK activation protected against cell death of c-Myc-depleted melanoma cells through suppression of oxidative stress. Furthermore, TCGA database analysis of early-stage human melanoma samples revealed an inverse correlation between C-MYC and patient survival, suggesting that C-MYC expression levels could serve as a prognostic marker for early-stage disease.

KW - AMPK

KW - c-Myc

KW - gene targeting

KW - melanoma

KW - oxidative stress

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U2 - 10.15252/embj.201797673

DO - 10.15252/embj.201797673

M3 - Journal article

C2 - 29440228

AN - SCOPUS:85041919285

SN - 0261-4189

VL - 37

JO - EMBO Journal

JF - EMBO Journal

IS - 5

M1 - e97673

ER -