Blood Cancer Journal (May 2024)

Patient-derived follicular lymphoma spheroids recapitulate lymph node signaling and immune profile uncovering galectin-9 as a novel immunotherapeutic target

  • Cèlia Dobaño-López,
  • Juan García Valero,
  • Ferran Araujo-Ayala,
  • Ferran Nadeu,
  • Fabien Gava,
  • Carla Faria,
  • Marine Norlund,
  • Renaud Morin,
  • Pascale Bernes-Lasserre,
  • Fabian Arenas,
  • Marta Grau,
  • Cristina López,
  • Irene López-Oreja,
  • Neus Serrat,
  • Ares Martínez-Farran,
  • Lluís Hernández,
  • Heribert Playa-Albinyana,
  • Rubén Giménez,
  • Silvia Beà,
  • Elías Campo,
  • Jean-Michel Lagarde,
  • Armando López-Guillermo,
  • Laura Magnano,
  • Dolors Colomer,
  • Christine Bezombes,
  • Patricia Pérez-Galán

DOI
https://doi.org/10.1038/s41408-024-01041-7
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 14

Abstract

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Abstract Follicular lymphoma (FL), the most common indolent non-Hodgkin lymphoma, constitutes a paradigm of immune tumor microenvironment (TME) contribution to disease onset, progression, and heterogenous clinical outcome. Here we present the first FL-Patient Derived Lymphoma Spheroid (FL-PDLS), including fundamental immune actors and features of TME in FL lymph nodes (LNs). FL-PDLS is organized in disc-shaped 3D structures composed of proliferating B and T cells, together with macrophages with an intermediate M1/M2 phenotype. FL-PDLS recapitulates the most relevant B-cell transcriptional pathways present in FL-LN (proliferation, epigenetic regulation, mTOR, adaptive immune system, among others). The T cell compartment in the FL-PDLS preserves CD4 subsets (follicular helper, regulatory, and follicular regulatory), also encompassing the spectrum of activation/exhaustion phenotypes in CD4 and CD8 populations. Moreover, this system is suitable for chemo and immunotherapy testing, recapitulating results obtained in the clinic. FL-PDLS allowed uncovering that soluble galectin-9 limits rituximab, rituximab, plus nivolumab/TIM-3 antitumoral activities. Blocking galectin-9 improves rituximab efficacy, highlighting galectin-9 as a novel immunotherapeutic target in FL. In conclusion, FL-PDLS maintains the crosstalk between malignant B cells and the immune LN-TME and constitutes a robust and multiplexed pre-clinical tool to perform drug screening in a patient-derived system, advancing toward personalized therapeutic approaches.