Targeting serine/glycine metabolism improves radiotherapy response in non-small cell lung cancer

Anais Sanchez-Castillo, Elien Heylen, Judith Hounjet, Kim G. Savelkouls, Natasja G. Lieuwes, Rianne Biemans, Ludwig J. Dubois, Kobe Reynders, Kasper M. Rouschop, Rianne D. W. Vaes, Kim De Keersmaecker, Maarten Lambrecht, Lizza E. L. Hendriks, Dirk K. M. De Ruysscher, Marc Vooijs, Kim R. Kampen*

*Corresponding author for this work

Research output: Contribution to journalArticleAcademicpeer-review

Abstract

BackgroundLung cancer is the most lethal cancer, and 85% of cases are classified as non-small cell lung cancer (NSCLC). Metabolic rewiring is a cancer hallmark that causes treatment resistance, and lacks insights into serine/glycine pathway adaptations upon radiotherapy.MethodsWe analyzed radiotherapy responses using mass-spectrometry-based metabolomics in NSCLC patient's plasma and cell lines. Efficacy of serine/glycine conversion inhibitor sertraline with radiotherapy was investigated by proliferation, clonogenic and spheroid assays, and in vivo using a serine/glycine dependent NSCLC mouse model by assessment of tumor growth, metabolite and cytokine levels, and immune signatures.ResultsSerine/glycine pathway metabolites were significantly consumed in response to radiotherapy in NSCLC patients and cell models. Combining sertraline with radiotherapy impaired NSCLC proliferation, clonogenicity and stem cell self-renewal capacity. In vivo, NSCLC tumor growth was reduced solely in the sertraline plus radiotherapy combination treatment group. Tumor weights linked to systemic serine/glycine pathway metabolite levels, and were inhibited in the combination therapy group. Interestingly, combination therapy reshaped the tumor microenvironment via cytokines associated with natural killer cells, supported by eradication of immune checkpoint galectin-1 and elevated granzyme B levels.ConclusionOur findings highlight that targeting serine/glycine metabolism using sertraline restricts cancer cell recovery from radiotherapy and provides tumor control through immunomodulation in NSCLC.
Original languageEnglish
Pages (from-to)568-584
Number of pages17
JournalBritish Journal of Cancer
Volume130
Issue number4
Early online date1 Dec 2023
DOIs
Publication statusPublished - 9 Mar 2024

Keywords

  • SERINE HYDROXYMETHYLTRANSFERASE SHMT
  • PERSISTENT OXIDATIVE STRESS
  • IONIZING-RADIATION
  • IN-VIVO
  • PATHWAY
  • DNA
  • PHARMACOKINETICS
  • MICROENVIRONMENT
  • IDENTIFICATION
  • BIOSYNTHESIS

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