| Literature DB >> 34102109 |
Stéphanie Torrino1, Eloise M Grasset2, Stephane Audebert3, Ilyes Belhadj4, Caroline Lacoux4, Meagan Haynes2, Sabrina Pisano5, Sophie Abélanet4, Frederic Brau4, Stephen Y Chan6, Bernard Mari4, William M Oldham7, Andrew J Ewald2, Thomas Bertero8.
Abstract
Mechanical signals from the tumor microenvironment modulate cell mechanics and influence cell metabolism to promote cancer aggressiveness. Cells withstand external forces by adjusting the stiffness of their cytoskeleton. Microtubules (MTs) act as compression-bearing elements. Yet how cancer cells regulate MT dynamic in response to the locally constrained environment has remained unclear. Using breast cancer as a model of a disease in which mechanical signaling promotes disease progression, we show that matrix stiffening rewires glutamine metabolism to promote MT glutamylation and force MT stabilization, thereby promoting cell invasion. Pharmacologic inhibition of glutamine metabolism decreased MT glutamylation and affected their mechanical stabilization. Similarly, decreased MT glutamylation by overexpressing tubulin mutants lacking glutamylation site(s) decreased MT stability, thereby hampering cancer aggressiveness in vitro and in vivo. Together, our results decipher part of the enigmatic tubulin code that coordinates the fine-tunable properties of MT and link cell metabolism to MT dynamics and cancer aggressiveness.Entities:
Keywords: breast cancer; cancer cell metabolism; glutamine metabolism; glutamylation; mechanobiology; microtubules; posttranslational modifications
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Year: 2021 PMID: 34102109 DOI: 10.1016/j.cmet.2021.05.009
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287