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Tumour and host cell PD-L1 is required to mediate suppression of anti-tumour immunity in mice

Author

Listed:
  • Janet Lau

    (Genentech, Inc.)

  • Jeanne Cheung

    (Genentech, Inc.)

  • Armando Navarro

    (Genentech, Inc.)

  • Steve Lianoglou

    (Genentech, Inc.)

  • Benjamin Haley

    (Genentech, Inc.)

  • Klara Totpal

    (Genentech, Inc.)

  • Laura Sanders

    (Genentech, Inc.)

  • Hartmut Koeppen

    (Genentech, Inc.)

  • Patrick Caplazi

    (Genentech, Inc.)

  • Jacqueline McBride

    (Genentech, Inc.)

  • Henry Chiu

    (Genentech, Inc.)

  • Rebecca Hong

    (Genentech, Inc.)

  • Jane Grogan

    (Genentech, Inc.)

  • Vincent Javinal

    (Genentech, Inc.)

  • Robert Yauch

    (Genentech, Inc. 1 DNA Way)

  • Bryan Irving

    (Genentech, Inc.
    Present address: CytomX Therapeutics, Inc. 151 Oyster Point Blvd, Suite 400, South San Francisco, California 94080, USA.)

  • Marcia Belvin

    (Genentech, Inc.)

  • Ira Mellman

    (Genentech, Inc.)

  • Jeong M. Kim

    (Genentech, Inc.)

  • Maike Schmidt

    (Genentech, Inc.)

Abstract

Expression of PD-L1, the ligand for T-cell inhibitory receptor PD-1, is one key immunosuppressive mechanism by which cancer avoids eradication by the immune system. Therapeutic use of blocking antibodies to PD-L1 or its receptor PD-1 has produced unparalleled, durable clinical responses, with highest likelihood of response seen in patients whose tumour or immune cells express PD-L1 before therapy. The significance of PD-L1 expression in each cell type has emerged as a central and controversial unknown in the clinical development of immunotherapeutics. Using genetic deletion in preclinical mouse models, here we show that PD-L1 from disparate cellular sources, including tumour cells, myeloid or other immune cells can similarly modulate the degree of cytotoxic T-cell function and activity in the tumour microenvironment. PD-L1 expression in both the host and tumour compartment contribute to immune suppression in a non-redundant fashion, suggesting that both sources could be predictive of sensitivity to therapeutic agents targeting the PD-L1/PD-1 axis.

Suggested Citation

  • Janet Lau & Jeanne Cheung & Armando Navarro & Steve Lianoglou & Benjamin Haley & Klara Totpal & Laura Sanders & Hartmut Koeppen & Patrick Caplazi & Jacqueline McBride & Henry Chiu & Rebecca Hong & Jan, 2017. "Tumour and host cell PD-L1 is required to mediate suppression of anti-tumour immunity in mice," Nature Communications, Nature, vol. 8(1), pages 1-11, April.
    • Handle: RePEc:nat:natcom:v:8:y:2017:i:1:d:10.1038_ncomms14572
    DOI: 10.1038/ncomms14572
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    Cited by:

    1. Lin-Zhou Zhang & Jie-Gang Yang & Gai-Li Chen & Qi-Hui Xie & Qiu-Yun Fu & Hou-Fu Xia & Yi-Cun Li & Jue Huang & Ye Li & Min Wu & Hai-Ming Liu & Fu-Bing Wang & Ke-Zhen Yi & Huan-Gang Jiang & Fu-Xiang Zho, 2024. "PD-1/CD80+ small extracellular vesicles from immunocytes induce cold tumours featured with enhanced adaptive immunosuppression," Nature Communications, Nature, vol. 15(1), pages 1-18, December.

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