N7-methylguanosine methylation of tRNAs regulates survival to stress in cancer

Author:

García-Vílchez Raquel,Añazco-Guenkova Ana M.ORCID,López Judith,Dietmann Sabine,Tomé Mercedes,Jimeno Sonia,Azkargorta Mikel,Elortza Félix,Bárcena Laura,Gonzalez-Lopez Monika,Aransay Ana M.ORCID,Sánchez-Martín Manuel A.ORCID,Huertas PabloORCID,Durán Raúl V.ORCID,Blanco SandraORCID

Abstract

AbstractTumour progression and therapy tolerance are highly regulated and complex processes largely dependent on the plasticity of cancer cells and their capacity to respond to stress. The higher plasticity of cancer cells highlights the need for identifying targetable molecular pathways that challenge cancer cell survival. Here, we show that N7-guanosine methylation (m7G) of tRNAs, mediated by METTL1, regulates survival to stress conditions in cancer cells. Mechanistically, we find that m7G in tRNAs protects them from stress-induced cleavage and processing into 5’ tRNA fragments. Our analyses reveal that the loss of tRNA m7G methylation activates stress response pathways, sensitising cancer cells to stress. Furthermore, we find that the loss of METTL1 reduces tumour growth and increases cytotoxic stress in vivo. Our study uncovers the role of m7G methylation of tRNAs in stress responses and highlights the potential of targeting METTL1 to sensitise cancer cells to chemotherapy.

Publisher

Springer Science and Business Media LLC

Subject

Cancer Research,Genetics,Molecular Biology

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