Targeting aldolase A in hepatocellular carcinoma leads to imbalanced glycolysis and energy stress due to uncontrolled FBP accumulation

Abstract:
        Abstract
        Increased glycolytic flux is a hallmark of cancer; however, an increasing body of evidence indicates that glycolytic ATP production may be dispensable in cancer, as metabolic plasticity allows cancer cells to readily adapt to disruption of glycolysis by increasing ATP production via oxidative phosphorylation. Using functional genomic screening, we show here that liver cancer cells show a unique sensitivity toward aldolase A (ALDOA) depletion. Targeting glycolysis by disrupting the catalytic activity of ALDOA led to severe energy stress and cell cycle arrest in murine and human hepatocellular carcinoma cell lines. With a combination of metabolic flux analysis, metabolomics, stable-isotope tracing and mathematical modelling, we demonstrate that inhibiting ALDOA induced a state of imbalanced glycolysis in which the investment phase outpaced the payoff phase. Targeting ALDOA effectively converted glycolysis from an energy producing into an energy-consuming process. Moreover, we found that depletion of ALDOA extended survival and reduced cancer cell proliferation in an animal model of hepatocellular carcinoma. Thus, our findings indicate that induction of imbalanced glycolysis by targeting ALDOA presents a unique opportunity to overcome the inherent metabolic plasticity of cancer cells.

SEEK ID: https://seek.lisym.org/publications/443

DOI: 10.1038/s42255-024-01201-w

Projects: Forschungsnetzwerk LiSyM-Krebs, SMART-NAFLD

Publication type: Journal

Journal: Nature Metabolism

Citation: Nat Metab 7(2):348-366

Date Published: 1st Feb 2025

Registered Mode: by DOI

Authors: Marteinn T. Snaebjornsson, Philipp Poeller, Daria Komkova, Florian Röhrig, Lisa Schlicker, Alina M. Winkelkotte, Adriano B. Chaves-Filho, Kamal M. Al-Shami, Carolina Dehesa Caballero, Ioanna Koltsaki, Felix C. E. Vogel, Roberto Carlos Frias-Soler, Ramona Rudalska, Jessica D. Schwarz, Elmar Wolf, Daniel Dauch, Ralf Steuer, Almut Schulze

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Snaebjornsson, M. T., Poeller, P., Komkova, D., Röhrig, F., Schlicker, L., Winkelkotte, A. M., Chaves-Filho, A. B., Al-Shami, K. M., Caballero, C. D., Koltsaki, I., Vogel, F. C. E., Frias-Soler, R. C., Rudalska, R., Schwarz, J. D., Wolf, E., Dauch, D., Steuer, R., & Schulze, A. (2025). Targeting aldolase A in hepatocellular carcinoma leads to imbalanced glycolysis and energy stress due to uncontrolled FBP accumulation. In Nature Metabolism (Vol. 7, Issue 2, pp. 348–366). Springer Science and Business Media LLC. https://doi.org/10.1038/s42255-024-01201-w
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Created: 2nd Apr 2025 at 12:06

Last updated: 2nd Apr 2025 at 12:08

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