PLoS Pathogens (Mar 2020)

Combination immunotherapy with anti-PD-L1 antibody and depletion of regulatory T cells during acute viral infections results in improved virus control but lethal immunopathology.

  • Paul David,
  • Malgorzata Drabczyk-Pluta,
  • Eva Pastille,
  • Torben Knuschke,
  • Tanja Werner,
  • Nadine Honke,
  • Dominik A Megger,
  • Ilseyar Akhmetzyanova,
  • Namir Shaabani,
  • Annette Eyking-Singer,
  • Elke Cario,
  • Olivia Kershaw,
  • Achim D Gruber,
  • Matthias Tenbusch,
  • Kirsten K Dietze,
  • Mirko Trilling,
  • Jia Liu,
  • Dirk Schadendorf,
  • Hendrik Streeck,
  • Karl S Lang,
  • Youhua Xie,
  • Lisa Zimmer,
  • Barbara Sitek,
  • Annette Paschen,
  • Astrid M Westendorf,
  • Ulf Dittmer,
  • Gennadiy Zelinskyy

DOI
https://doi.org/10.1371/journal.ppat.1008340
Journal volume & issue
Vol. 16, no. 3
p. e1008340

Abstract

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Combination immunotherapy (CIT) is currently applied as a treatment for different cancers and is proposed as a cure strategy for chronic viral infections. Whether such therapies are efficient during an acute infection remains elusive. To address this, inhibitory receptors were blocked and regulatory T cells depleted in acutely Friend retrovirus-infected mice. CIT resulted in a dramatic expansion of cytotoxic CD4+ and CD8+ T cells and a subsequent reduction in viral loads. Despite limited viral replication, mice developed fatal immunopathology after CIT. The pathology was most severe in the gastrointestinal tract and was mediated by granzyme B producing CD4+ and CD8+ T cells. A similar post-CIT pathology during acute Influenza virus infection of mice was observed, which could be prevented by vaccination. Melanoma patients who developed immune-related adverse events under immune checkpoint CIT also presented with expanded granzyme-expressing CD4+ and CD8+ T cell populations. Our data suggest that acute infections may induce immunopathology in patients treated with CIT, and that effective measures for infection prevention should be applied.