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Targeting the mTOR pathway uncouples the efficacy and toxicity of PD-1 blockade in renal transplantation

Author

Listed:
  • Khashayar Esfahani

    (McGill University
    Centre of Excellence in Translational Immunology (CETI)
    McGill University)

  • Tho-Alfakar Al-Aubodah

    (Centre of Excellence in Translational Immunology (CETI)
    McGill University
    Research Institute of the McGill University Health Centre)

  • Pamela Thebault

    (University of Montréal Hospital Research Centre
    Institut du cancer de Montréal
    Clinical Immuno-Monitoring Core Facility, CRCHUM
    University of Montréal)

  • Réjean Lapointe

    (University of Montréal Hospital Research Centre
    Institut du cancer de Montréal
    Clinical Immuno-Monitoring Core Facility, CRCHUM
    University of Montréal)

  • Marie Hudson

    (Centre of Excellence in Translational Immunology (CETI)
    McGill University)

  • Nathalie A. Johnson

    (Centre of Excellence in Translational Immunology (CETI)
    Lady Davis Institute, Jewish General Hospital, McGill University)

  • Dana Baran

    (McGill University)

  • Najwa Bhulaiga

    (McGill University)

  • Tomoko Takano

    (Centre of Excellence in Translational Immunology (CETI)
    McGill University)

  • Jean-François Cailhier

    (University of Montréal Hospital Research Centre
    Institut du cancer de Montréal
    Clinical Immuno-Monitoring Core Facility, CRCHUM
    University of Montréal)

  • Ciriaco A. Piccirillo

    (Centre of Excellence in Translational Immunology (CETI)
    McGill University
    Research Institute of the McGill University Health Centre)

  • Wilson H. Miller

    (McGill University
    Centre of Excellence in Translational Immunology (CETI)
    McGill University)

Abstract

Immune checkpoint inhibitor (ICI) use remains a challenge in patients with solid organ allografts as most would undergo rejection. In a melanoma patient in whom programmed-death 1 (PD-1) blockade resulted in organ rejection and colitis, the addition of the mTOR inhibitor sirolimus resulted in ongoing anti-tumor efficacy while promoting allograft tolerance. Strong granzyme B+, interferon (IFN)-γ+ CD8+ cytotoxic T cell and circulating regulatory T (Treg) cell responses were noted during allograft rejection, along with significant eosinophilia and elevated serum IL-5 and eotaxin levels. Co-treatment with sirolimus abated cytotoxic T cell numbers and eosinophilia, while elevated Treg cell numbers in the peripheral blood were maintained. Interestingly, numbers of IFN-γ+ CD4+ T cells and serum IFN-γ levels increased with the addition of sirolimus treatment likely promoting ongoing anti-PD-1 efficacy. Thus, our results indicate that sirolimus has the potential to uncouple anti-PD-1 therapy toxicity and efficacy.

Suggested Citation

  • Khashayar Esfahani & Tho-Alfakar Al-Aubodah & Pamela Thebault & Réjean Lapointe & Marie Hudson & Nathalie A. Johnson & Dana Baran & Najwa Bhulaiga & Tomoko Takano & Jean-François Cailhier & Ciriaco A., 2019. "Targeting the mTOR pathway uncouples the efficacy and toxicity of PD-1 blockade in renal transplantation," Nature Communications, Nature, vol. 10(1), pages 1-9, December.
  • Handle: RePEc:nat:natcom:v:10:y:2019:i:1:d:10.1038_s41467-019-12628-1
    DOI: 10.1038/s41467-019-12628-1
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    Cited by:

    1. Victor Joo & Karim Abdelhamid & Alessandra Noto & Sofiya Latifyan & Federica Martina & Douglas Daoudlarian & Rita De Micheli & Menno Pruijm & Solange Peters & Roger Hullin & Olivier Gaide & Giuseppe P, 2024. "Primary prophylaxis with mTOR inhibitor enhances T cell effector function and prevents heart transplant rejection during talimogene laherparepvec therapy of squamous cell carcinoma," Nature Communications, Nature, vol. 15(1), pages 1-12, December.

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