Journal of Translational Medicine (Jan 2025)

PD-L1 and IFN-γ modulate Non-Small Cell Lung Cancer (NSCLC) cell plasticity associated to immune checkpoint inhibitor (ICI)-mediated hyperprogressive disease (HPD)

  • Stefania Angelicola,
  • Francesca Giunchi,
  • Francesca Ruzzi,
  • Mariateresa Frascino,
  • Mary Pitzalis,
  • Laura Scalambra,
  • Maria Sofia Semprini,
  • Olga Maria Pittino,
  • Chiara Cappello,
  • Irene Siracusa,
  • Ilaria Candida Chillico,
  • Martina Di Noia,
  • Cristian Turato,
  • Silvia De Siervi,
  • Francesco Lescai,
  • Teresa Ciavattini,
  • Giulia Lopatriello,
  • Luca Bertoli,
  • Hugo De Jonge,
  • Luisa Iamele,
  • Annalisa Altimari,
  • Elisa Gruppioni,
  • Andrea Ardizzoni,
  • Marzia Rossato,
  • Francesco Gelsomino,
  • Pier-Luigi Lollini,
  • Arianna Palladini

DOI
https://doi.org/10.1186/s12967-024-06023-8
Journal volume & issue
Vol. 23, no. 1
pp. 1 – 20

Abstract

Read online

Abstract Background Non-Small Cell Lung Cancer (NSCLC) is the leading cause of cancer death worldwide. Although immune checkpoint inhibitors (ICIs) have shown remarkable clinical efficacy, they can also induce a paradoxical cancer acceleration, known as hyperprogressive disease (HPD), whose causative mechanisms are still unclear. Methods This study investigated the mechanisms of ICI resistance in an HPD-NSCLC model. Two primary cell cultures were established from samples of a NSCLC patient, before ICI initiation (“baseline”, NSCLC-B) and during HPD (“hyperprogression”, NSCLC-H). The cell lines were phenotypically and molecularly characterized through immunofluorescence, Western Blotting and RNA-Seq analysis. To assess cell plasticity and aggressiveness, cellular growth patterns were evaluated both in vitro and in vivo through 2D and 3D cell growth assays and patient-derived xenografts establishment. In vitro investigations, including the evaluation of cell sensitivity to interferon-gamma (IFN-γ) and cell response to PD-L1 modulation, were conducted to explore the influence of these factors on cell plasticity regulation. Results NSCLC-H exhibited increased expression of specific CD44 isoforms and a more aggressive phenotype, including organoid formation ability, compared to NSCLC-B. Plastic changes in NSCLC-H were well described by a deep transcriptome shift, that also affected IFN-γ–related genes, including PD-L1. IFN-γ–mediated cell growth inhibition was compromised in both 2D-cultured NSCLC-B and NSCLC-H cells. Further, the cytokine induced a partial activation of both type I and type II IFN-pathway mediators, together with a striking increase in NSCLC-B growth in 3D cell culture systems. Finally, low IFN-γ doses and PD-L1 modulation both promoted plastic changes in NSCLC-B, increasing CD44 expression and its ability to produce spheres. Conclusions Our findings identified plasticity as a relevant hallmark of ICI-mediated HPD by demonstrating that ICIs can modulate the IFN-γ and PD-L1 pathways, driving tumor cell plasticity and fueling HPD development.

Keywords