An epitranscriptomic mechanism underlies selective mRNA translation remodelling in melanoma persister cells

Shensi Shen; Sara Faouzi; Amandine Bastide; Sylvain Martineau; Hélène Malka-Mahieu; Yu Fu; Xiaoxiao Sun; Christine Mateus; Emilie Routier; Severine Roy; Laurent Desaubry; Fabrice André; Alexander Eggermont; Alexandre David; Jean Yves Scoazec; Stéphan Vagner; Caroline Robert

doi:10.1038/s41467-019-13360-6

An epitranscriptomic mechanism underlies selective mRNA translation remodelling in melanoma persister cells

Shensi Shen
, Sara Faouzi
, Amandine Bastide
, Sylvain Martineau
, Hélène Malka-Mahieu
, Yu Fu
, Xiaoxiao Sun
, Christine Mateus
, Emilie Routier
, Severine Roy
, Laurent Desaubry
, Fabrice André
, Alexander Eggermont
, Alexandre David
, Jean Yves Scoazec
, Stéphan Vagner
, Caroline Robert

Research output: Contribution to journal › Article › peer-review

79 Citations (Scopus)

Abstract

Cancer persister cells tolerate anticancer drugs and serve as the founders of acquired resistance and cancer relapse. Here we show that a subpopulation of BRAF^V600 mutant melanoma cells that tolerates exposure to BRAF and MEK inhibitors undergoes a reversible remodelling of mRNA translation that evolves in parallel with drug sensitivity. Although this process is associated with a global reduction in protein synthesis, a subset of mRNAs undergoes an increased efficiency in translation. Inhibiting the eIF4A RNA helicase, a component of the eIF4F translation initiation complex, abrogates this selectively increased translation and is lethal to persister cells. Translation remodelling in persister cells coincides with an increased N6-methyladenosine modification in the 5′-untranslated region of some highly translated mRNAs. Combination of eIF4A inhibitor with BRAF and MEK inhibitors effectively inhibits the emergence of persister cells and may represent a new therapeutic strategy to prevent acquired drug resistance.

Original language	English
Article number	5713
Journal	Nature communications
Volume	10
Issue number	1
DOIs	https://doi.org/10.1038/s41467-019-13360-6
Publication status	Published - 1 Dec 2019
Externally published	Yes

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Shen, S., Faouzi, S., Bastide, A., Martineau, S., Malka-Mahieu, H., Fu, Y., Sun, X., Mateus, C., Routier, E., Roy, S., Desaubry, L., André, F., Eggermont, A., David, A., Scoazec, J. Y., Vagner, S., & Robert, C. (2019). An epitranscriptomic mechanism underlies selective mRNA translation remodelling in melanoma persister cells. Nature communications, 10(1), Article 5713. https://doi.org/10.1038/s41467-019-13360-6

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title = "An epitranscriptomic mechanism underlies selective mRNA translation remodelling in melanoma persister cells",

abstract = "Cancer persister cells tolerate anticancer drugs and serve as the founders of acquired resistance and cancer relapse. Here we show that a subpopulation of BRAFV600 mutant melanoma cells that tolerates exposure to BRAF and MEK inhibitors undergoes a reversible remodelling of mRNA translation that evolves in parallel with drug sensitivity. Although this process is associated with a global reduction in protein synthesis, a subset of mRNAs undergoes an increased efficiency in translation. Inhibiting the eIF4A RNA helicase, a component of the eIF4F translation initiation complex, abrogates this selectively increased translation and is lethal to persister cells. Translation remodelling in persister cells coincides with an increased N6-methyladenosine modification in the 5′-untranslated region of some highly translated mRNAs. Combination of eIF4A inhibitor with BRAF and MEK inhibitors effectively inhibits the emergence of persister cells and may represent a new therapeutic strategy to prevent acquired drug resistance.",

author = "Shensi Shen and Sara Faouzi and Amandine Bastide and Sylvain Martineau and H{\'e}l{\`e}ne Malka-Mahieu and Yu Fu and Xiaoxiao Sun and Christine Mateus and Emilie Routier and Severine Roy and Laurent Desaubry and Fabrice Andr{\'e} and Alexander Eggermont and Alexandre David and Scoazec, \{Jean Yves\} and St{\'e}phan Vagner and Caroline Robert",

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doi = "10.1038/s41467-019-13360-6",

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Shen, S, Faouzi, S, Bastide, A, Martineau, S, Malka-Mahieu, H, Fu, Y, Sun, X, Mateus, C, Routier, E, Roy, S, Desaubry, L, André, F, Eggermont, A, David, A, Scoazec, JY, Vagner, S & Robert, C 2019, 'An epitranscriptomic mechanism underlies selective mRNA translation remodelling in melanoma persister cells', Nature communications, vol. 10, no. 1, 5713. https://doi.org/10.1038/s41467-019-13360-6

TY - JOUR

T1 - An epitranscriptomic mechanism underlies selective mRNA translation remodelling in melanoma persister cells

AU - Shen, Shensi

AU - Faouzi, Sara

AU - Bastide, Amandine

AU - Martineau, Sylvain

AU - Malka-Mahieu, Hélène

AU - Fu, Yu

AU - Sun, Xiaoxiao

AU - Mateus, Christine

AU - Routier, Emilie

AU - Roy, Severine

AU - Desaubry, Laurent

AU - André, Fabrice

AU - Eggermont, Alexander

AU - David, Alexandre

AU - Scoazec, Jean Yves

AU - Vagner, Stéphan

AU - Robert, Caroline

PY - 2019/12/1

Y1 - 2019/12/1

N2 - Cancer persister cells tolerate anticancer drugs and serve as the founders of acquired resistance and cancer relapse. Here we show that a subpopulation of BRAFV600 mutant melanoma cells that tolerates exposure to BRAF and MEK inhibitors undergoes a reversible remodelling of mRNA translation that evolves in parallel with drug sensitivity. Although this process is associated with a global reduction in protein synthesis, a subset of mRNAs undergoes an increased efficiency in translation. Inhibiting the eIF4A RNA helicase, a component of the eIF4F translation initiation complex, abrogates this selectively increased translation and is lethal to persister cells. Translation remodelling in persister cells coincides with an increased N6-methyladenosine modification in the 5′-untranslated region of some highly translated mRNAs. Combination of eIF4A inhibitor with BRAF and MEK inhibitors effectively inhibits the emergence of persister cells and may represent a new therapeutic strategy to prevent acquired drug resistance.

AB - Cancer persister cells tolerate anticancer drugs and serve as the founders of acquired resistance and cancer relapse. Here we show that a subpopulation of BRAFV600 mutant melanoma cells that tolerates exposure to BRAF and MEK inhibitors undergoes a reversible remodelling of mRNA translation that evolves in parallel with drug sensitivity. Although this process is associated with a global reduction in protein synthesis, a subset of mRNAs undergoes an increased efficiency in translation. Inhibiting the eIF4A RNA helicase, a component of the eIF4F translation initiation complex, abrogates this selectively increased translation and is lethal to persister cells. Translation remodelling in persister cells coincides with an increased N6-methyladenosine modification in the 5′-untranslated region of some highly translated mRNAs. Combination of eIF4A inhibitor with BRAF and MEK inhibitors effectively inhibits the emergence of persister cells and may represent a new therapeutic strategy to prevent acquired drug resistance.

UR - https://www.scopus.com/pages/publications/85076619587

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DO - 10.1038/s41467-019-13360-6

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SN - 2041-1723

VL - 10

JO - Nature communications

JF - Nature communications

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ER -

An epitranscriptomic mechanism underlies selective mRNA translation remodelling in melanoma persister cells

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