Cell Death Discovery (Jun 2024)

Dependence on mitochondrial respiration of malignant T cells reveals a new therapeutic target for angioimmunoblastic T-cell lymphoma

  • Adrien Krug,
  • Rana Mhaidly,
  • Marie Tosolini,
  • Laura Mondragon,
  • Gamze Tari,
  • Adriana Martinez Turtos,
  • Rachel Paul-Bellon,
  • Vahid Asnafi,
  • Sandrine Marchetti,
  • Léa Di Mascio,
  • Marion Travert,
  • Frédéric Bost,
  • Emmanuel Bachy,
  • Rafael J. Argüello,
  • Jean-Jacques Fournié,
  • Philippe Gaulard,
  • François Lemonnier,
  • Jean-Ehrland Ricci,
  • Els Verhoeyen

DOI
https://doi.org/10.1038/s41420-024-02061-9
Journal volume & issue
Vol. 10, no. 1
pp. 1 – 14

Abstract

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Abstract Cancer metabolic reprogramming has been recognized as one of the cancer hallmarks that promote cell proliferation, survival, as well as therapeutic resistance. Up-to-date regulation of metabolism in T-cell lymphoma is poorly understood. In particular, for human angioimmunoblastic T-cell lymphoma (AITL) the metabolic profile is not known. Metabolic intervention could help identify new treatment options for this cancer with very poor outcomes and no effective medication. Transcriptomic analysis of AITL tumor cells, identified that these cells use preferentially mitochondrial metabolism. By using our preclinical AITL mouse model, mimicking closely human AITL features, we confirmed that T follicular helper (Tfh) tumor cells exhibit a strong enrichment of mitochondrial metabolic signatures. Consistent with these results, disruption of mitochondrial metabolism using metformin or a mitochondrial complex I inhibitor such as IACS improved the survival of AITL lymphoma-bearing mice. Additionally, we confirmed a selective elimination of the malignant human AITL T cells in patient biopsies upon mitochondrial respiration inhibition. Moreover, we confirmed that diabetic patients suffering from T-cell lymphoma, treated with metformin survived longer as compared to patients receiving alternative treatments. Taking together, our findings suggest that targeting the mitochondrial metabolic pathway could be a clinically efficient approach to inhibit aggressive cancers such as peripheral T-cell lymphoma.