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PKM2 diverts glycolytic flux in dependence on mitochondrial one-carbon cycle

Authors :
Mohaned Benzarti
Anais Oudin
Elodie Viry
Ernesto Gargiulo
Maryse Schmoetten
Laura Neises
Coralie Pulido
Nadia I. Lorenz
Michael W. Ronellenfitsch
David Sumpton
Marc Warmoes
Christian Jaeger
Antoine Lesur
Etienne Moussay
Jerome Paggetti
Simone P. Niclou
Elisabeth Letellier
Johannes Meiser
Publication Year :
2023
Publisher :
Cold Spring Harbor Laboratory, 2023.

Abstract

Throughout the metastatic cascade, cancer cells are faced with harsh metabolic environments and nutritional stresses which apply selection pressure leaving only the most metabolically resilient cells to survive and form metastases. Metabolic characterisation of such cell populationsin vitrois currently challenging. Using galactose as a tool compound to mimic glycolytic limitation within the tumour microenvironment of primary and secondary neoplastic sites, we were able to uncover metabolic flexibility and plasticity of cancer cellsin vitro. In contrast to the established idea that high glycolytic flux and expression of dimeric PKM2 redirects carbons towards anabolic routes such as the pentose phosphate pathway and serine synthesis pathway (SSP), we have discovered by using stable-isotope tracing that also glycolytic limitation results in metabolic rewiring. Surprisingly, despite limited carbon availability and energetic stress, cells induce a near complete block of pyruvate kinase isozyme M2 (PKM2) to divert carbons towards SSP. Simultaneously, TCA cycle flux is sustained and oxygen consumption is increased, both supported by glutamine. Glutamine not only supports TCA cycle flux but also SSP via distinct mechanisms. Due to PKM2 block, malic enzyme exclusively supports TCA cycle flux while mitochondrial phosphoenolpyruvate carboxykinase supports SSP. Moreover, by using genetic modifications of different one-carbon (1C) cycle enzymes, we are able to reverse the PKM2 block suggesting a link between mitochondrial 1C cycle and pyruvate kinase. Thus we show that PKM2 inhibition acts as a branching point to direct glycolytic and glutamine carbons into distinct routes, overall supporting the metabolic plasticity and flexibility of cancer cells.

Details

Database :
OpenAIRE
Accession number :
edsair.doi...........1a522bab3a28454fca112d3efdad6bfe