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Adoptive cancer immunotherapy using DNA-demethylated T helper cells as antigen-presenting cells

Author

Listed:
  • Alexei F. Kirkin

    (Danish Cancer Society Research Center
    CytoVac A/S)

  • Karine N. Dzhandzhugazyan

    (Danish Cancer Society Research Center
    CytoVac A/S)

  • Per Guldberg

    (Danish Cancer Society Research Center)

  • Johnny Jon Fang

    (Danish Cancer Society Research Center
    CytoVac A/S)

  • Rikke S. Andersen

    (University of Southern Denmark)

  • Christina Dahl

    (Danish Cancer Society Research Center)

  • Jann Mortensen

    (Copenhagen University Hospital)

  • Tim Lundby

    (Copenhagen University Hospital)

  • Aase Wagner

    (Copenhagen University Hospital)

  • Ian Law

    (Copenhagen University Hospital)

  • Helle Broholm

    (Copenhagen University Hospital)

  • Line Madsen

    (Aarhus University Hospital)

  • Christer Lundell-Ek

    (CytoVac A/S)

  • Morten F. Gjerstorff

    (University of Southern Denmark)

  • Henrik J. Ditzel

    (University of Southern Denmark
    Odense University Hospital)

  • Martin R. Jensen

    (CytoVac A/S)

  • Walter Fischer

    (CytoVac A/S
    Copenhagen University Hospital)

Abstract

In cancer cells, cancer/testis (CT) antigens become epigenetically derepressed through DNA demethylation and constitute attractive targets for cancer immunotherapy. Here we report that activated CD4+ T helper cells treated with a DNA-demethylating agent express a broad repertoire of endogenous CT antigens and can be used as antigen-presenting cells to generate autologous cytotoxic T lymphocytes (CTLs) and natural killer cells. In vitro, activated CTLs induce HLA-restricted lysis of tumor cells of different histological types, as well as cells expressing single CT antigens. In a phase 1 trial of 25 patients with recurrent glioblastoma multiforme, cytotoxic lymphocytes homed to the tumor, with tumor regression ongoing in three patients for 14, 22, and 27 months, respectively. No treatment-related adverse effects were observed. This proof-of-principle study shows that tumor-reactive effector cells can be generated ex vivo by exposure to antigens induced by DNA demethylation, providing a novel, minimally invasive therapeutic strategy for treating cancer.

Suggested Citation

  • Alexei F. Kirkin & Karine N. Dzhandzhugazyan & Per Guldberg & Johnny Jon Fang & Rikke S. Andersen & Christina Dahl & Jann Mortensen & Tim Lundby & Aase Wagner & Ian Law & Helle Broholm & Line Madsen &, 2018. "Adoptive cancer immunotherapy using DNA-demethylated T helper cells as antigen-presenting cells," Nature Communications, Nature, vol. 9(1), pages 1-12, December.
  • Handle: RePEc:nat:natcom:v:9:y:2018:i:1:d:10.1038_s41467-018-03217-9
    DOI: 10.1038/s41467-018-03217-9
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