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Constitutive inflammation and epithelial-mesenchymal transition dictate sensitivity to nivolumab in CONFIRM: a placebo-controlled, randomised phase III trial

Author

Listed:
  • Dean A. Fennell

    (UK Robert Kilpatrick Clinical Sciences Building
    University Hospitals of Leicester NHS Trust)

  • Kayleigh Hill

    (University of Southampton)

  • Min Zhang

    (UK Robert Kilpatrick Clinical Sciences Building
    Novogene Co. Limited)

  • Charlotte Poile

    (UK Robert Kilpatrick Clinical Sciences Building)

  • Sean Ewings

    (University of Southampton)

  • Essa Y. Baitei

    (UK Robert Kilpatrick Clinical Sciences Building
    King Faisal Specialist Hospital & Research Centre)

  • Joanna Dzialo

    (UK Robert Kilpatrick Clinical Sciences Building)

  • Nada Nusrat

    (UK Robert Kilpatrick Clinical Sciences Building
    University of Tripoli)

  • Jan Rogel

    (UK Robert Kilpatrick Clinical Sciences Building)

  • Daniel Faulkner

    (UK Robert Kilpatrick Clinical Sciences Building)

  • Christian Ottensmeier

    (University of Liverpool)

  • Raffaele Califano

    (Wythenshawe Hospital)

  • Gerard G. Hanna

    (Queens University Belfast)

  • Sarah Danson

    (Sheffield Teaching Hospitals NHS Foundation)

  • Nicola Steele

    (Beatson West of Scotland Cancer Centre)

  • Mavis Nye

    (c/o University of Southampton)

  • Lucy Johnson

    (University of Southampton)

  • Kim Mallard

    (University of Southampton)

  • Joanne Lord

    (University of Southampton)

  • Calley Middleton

    (University of Southampton)

  • Peter Szlosarek

    (Queen Mary University of London)

  • Sam Chan

    (York Teaching Hospital NHS Foundation Trust)

  • Liz Darlison

    (Mesothelioma UK)

  • Peter Wells-Jordan

    (UK Robert Kilpatrick Clinical Sciences Building
    University Hospitals of Leicester NHS Trust)

  • Cathy Richards

    (University Hospitals of Leicester NHS Trust)

  • James Harber

    (UWA Centre for Medical Research & Harry Perkins Institute of Medical Research)

  • Aleksandra Bzura

    (UK Robert Kilpatrick Clinical Sciences Building)

  • Jake Spicer

    (UK Robert Kilpatrick Clinical Sciences Building)

  • Catrin Pritchard

    (UK Robert Kilpatrick Clinical Sciences Building)

  • Tamihiro Kamata

    (Tennis Court Road)

  • Jens C. Hahne

    (UK Robert Kilpatrick Clinical Sciences Building)

  • Maymun Jama

    (UK Robert Kilpatrick Clinical Sciences Building)

  • Edward J. Hollox

    (University of Leicester)

  • Jason F. Lester

    (Singleton & Morrison Hospitals)

  • Jin-Li Luo

    (University of Leicester)

  • Zisen Zhou

    (University of Leicester)

  • Hongji Yang

    (University of Leicester)

  • Huiyu Zhou

    (University of Leicester)

  • Astero Klampatsa

    (The Institute of Cancer Research)

  • Gareth O. Griffiths

    (University of Southampton)

Abstract

Leveraging adaptive tumour immunity to control mesothelioma via immune checkpoint blockade is now a standard therapeutic approach. However, the determinants of sensitivity remain elusive. Low non-synonymous mutation burden and programmed death-ligand 1 expression, an abundance of immunosuppressive immune cell infiltration, and 9p21 deletion should all mitigate responses to therapy. To address this knowledge gap, we conducted a double blind, placebo-controlled, randomized phase III trial of the PD1 inhibitor, nivolumab (ClinicalTrial.gov registration: NCT03063450). After 37.2 months of follow-up, the primary endpoint of progression free-survival, but not overall survival was met. The nivolumab response rate was 10.3%, and related grade 3 or above adverse events occurred in 20.4% versus 7.2% for placebo. Progression-free and overall survival were longer in nivolumab-treated responders versus non-responders. In an exploratory multiomic analysis, blinded whole exome, transcriptome and multiplex immune profiling were used to interrogate R- versus NR-subgroups. Non-synonymous and neoantigen mutation burden were no different between groups, however R-mesotheliomas were infiltrated with activated CD8+ T- and CD19+ B-lymphocytes, organised into tertiary lymphoid structures. B-cell infiltration correlated with pro-inflammatory chemokines including IL24 and CCL19. Conversely, epithelial-mesenchymal transition and mitosis were associated with resistance to nivolumab. These findings illuminate features which can be leveraged to advance precision immunotherapy in this rare cancer setting.

Suggested Citation

  • Dean A. Fennell & Kayleigh Hill & Min Zhang & Charlotte Poile & Sean Ewings & Essa Y. Baitei & Joanna Dzialo & Nada Nusrat & Jan Rogel & Daniel Faulkner & Christian Ottensmeier & Raffaele Califano & G, 2025. "Constitutive inflammation and epithelial-mesenchymal transition dictate sensitivity to nivolumab in CONFIRM: a placebo-controlled, randomised phase III trial," Nature Communications, Nature, vol. 16(1), pages 1-13, December.
  • Handle: RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-61691-4
    DOI: 10.1038/s41467-025-61691-4
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    References listed on IDEAS

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