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IL-7 receptor blockade blunts antigen-specific memory T cell responses and chronic inflammation in primates

Author

Listed:
  • Lyssia Belarif

    (Université de Nantes
    OSE Immunotherapeutics)

  • Caroline Mary

    (Université de Nantes
    OSE Immunotherapeutics)

  • Lola Jacquemont

    (Université de Nantes)

  • Hoa Le Mai

    (Université de Nantes)

  • Richard Danger

    (Université de Nantes)

  • Jeremy Hervouet

    (Université de Nantes)

  • David Minault

    (Université de Nantes)

  • Virginie Thepenier

    (Université de Nantes
    OSE Immunotherapeutics)

  • Veronique Nerrière-Daguin

    (Université de Nantes)

  • Elisabeth Nguyen

    (Université de Nantes)

  • Sabrina Pengam

    (Université de Nantes
    OSE Immunotherapeutics)

  • Eric Largy

    (Quality Assistance
    Université de Bordeaux, INSERM U1212, CNRS UMR5320, IECB)

  • Arnaud Delobel

    (Quality Assistance)

  • Bernard Martinet

    (Université de Nantes)

  • Stéphanie Bas-Bernardet

    (Université de Nantes
    CHU Nantes)

  • Sophie Brouard

    (Université de Nantes
    CHU Nantes)

  • Jean-Paul Soulillou

    (Université de Nantes)

  • Nicolas Degauque

    (Université de Nantes
    CHU Nantes)

  • Gilles Blancho

    (Université de Nantes
    CHU Nantes)

  • Bernard Vanhove

    (Université de Nantes
    OSE Immunotherapeutics)

  • Nicolas Poirier

    (Université de Nantes
    OSE Immunotherapeutics)

Abstract

Targeting the expansion of pathogenic memory immune cells is a promising therapeutic strategy to prevent chronic autoimmune attacks. Here we investigate the therapeutic efficacy and mechanism of new anti-human IL-7Rα monoclonal antibodies (mAb) in non-human primates and show that, depending on the target epitope, a single injection of antagonistic anti-IL-7Rα mAbs induces a long-term control of skin inflammation despite repeated antigen challenges in presensitized monkeys. No modification in T cell numbers, phenotype, function or metabolism is observed in the peripheral blood or in response to polyclonal stimulation ex vivo. However, long-term in vivo hyporesponsiveness is associated with a significant decrease in the frequency of antigen-specific T cells producing IFN-γ upon antigen restimulation ex vivo. These findings indicate that chronic antigen-specific memory T cell responses can be controlled by anti-IL-7Rα mAbs, promoting and maintaining remission in T-cell mediated chronic inflammatory diseases.

Suggested Citation

  • Lyssia Belarif & Caroline Mary & Lola Jacquemont & Hoa Le Mai & Richard Danger & Jeremy Hervouet & David Minault & Virginie Thepenier & Veronique Nerrière-Daguin & Elisabeth Nguyen & Sabrina Pengam & , 2018. "IL-7 receptor blockade blunts antigen-specific memory T cell responses and chronic inflammation in primates," Nature Communications, Nature, vol. 9(1), pages 1-13, December.
  • Handle: RePEc:nat:natcom:v:9:y:2018:i:1:d:10.1038_s41467-018-06804-y
    DOI: 10.1038/s41467-018-06804-y
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