Glioblastoma cell motility depends on enhanced oxidative stress coupled with mobilization of a sulfurtransferase

Author:

Saurty-Seerunghen Mirca S.,Daubon ThomasORCID,Bellenger Léa,Delaunay Virgile,Castro Gloria,Guyon JorisORCID,Rezk Ahmed,Fabrega Sylvie,Idbaih Ahmed,Almairac Fabien,Burel-Vandenbos Fanny,Turchi Laurent,Duplus Eric,Virolle ThierryORCID,Peyrin Jean-Michel,Antoniewski Christophe,Chneiweiss HervéORCID,El-Habr Elias A.ORCID,Junier Marie-PierreORCID

Abstract

AbstractCell motility is critical for tumor malignancy. Metabolism being an obligatory step in shaping cell behavior, we looked for metabolic weaknesses shared by motile cells across the diverse genetic contexts of patients’ glioblastoma. Computational analyses of single-cell transcriptomes from thirty patients’ tumors isolated cells with high motile potential and highlighted their metabolic specificities. These cells were characterized by enhanced mitochondrial load and oxidative stress coupled with mobilization of the cysteine metabolism enzyme 3-Mercaptopyruvate sulfurtransferase (MPST). Functional assays with patients’ tumor-derived cells and -tissue organoids, and genetic and pharmacological manipulations confirmed that the cells depend on enhanced ROS production and MPST activity for their motility. MPST action involved protection of protein cysteine residues from damaging hyperoxidation. Its knockdown translated in reduced tumor burden, and a robust increase in mice survival. Starting from cell-by-cell analyses of the patients’ tumors, our work unravels metabolic dependencies of cell malignancy maintained across heterogeneous genomic landscapes.

Publisher

Springer Science and Business Media LLC

Subject

Cancer Research,Cell Biology,Cellular and Molecular Neuroscience,Immunology

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