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Transcriptional control of pancreatic cancer immunosuppression by metabolic enzyme CD73 in a tumor-autonomous and -autocrine manner

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  • Tianyu Tang

    (Zhejiang University School of Medicine
    Zhejiang University School of Medicine
    Zhejiang Clinical Research Center of Hepatobiliary and Pancreatic Diseases
    The Innovation Center for the Study of Pancreatic Diseases of Zhejiang Province)

  • Xing Huang

    (Zhejiang University School of Medicine
    Zhejiang University School of Medicine
    Zhejiang Clinical Research Center of Hepatobiliary and Pancreatic Diseases
    The Innovation Center for the Study of Pancreatic Diseases of Zhejiang Province)

  • Minghao Lu

    (Zhejiang University School of Medicine
    Zhejiang University School of Medicine
    Zhejiang Clinical Research Center of Hepatobiliary and Pancreatic Diseases
    The Innovation Center for the Study of Pancreatic Diseases of Zhejiang Province)

  • Gang Zhang

    (Zhejiang University School of Medicine
    Zhejiang University School of Medicine
    Zhejiang Clinical Research Center of Hepatobiliary and Pancreatic Diseases
    The Innovation Center for the Study of Pancreatic Diseases of Zhejiang Province)

  • Xu Han

    (Zhejiang University School of Medicine
    Zhejiang University School of Medicine
    Zhejiang Clinical Research Center of Hepatobiliary and Pancreatic Diseases
    The Innovation Center for the Study of Pancreatic Diseases of Zhejiang Province)

  • Tingbo Liang

    (Zhejiang University School of Medicine
    Zhejiang University School of Medicine
    Zhejiang Clinical Research Center of Hepatobiliary and Pancreatic Diseases
    The Innovation Center for the Study of Pancreatic Diseases of Zhejiang Province)

Abstract

Cancer cell metabolism contributes to the establishment of an immunosuppressive tumor microenvironment. Aberrant expression of CD73, a critical enzyme in ATP metabolism, on the cell surface results in the extracellular accumulation of adenosine, which exhibits direct inhibitory effects on tumor-infiltrating lymphocytes. However, little is known about the influence of CD73 on negative immune regulation-associated signaling molecules and transduction pathways inside tumor cells. This study aims to demonstrate the moonlighting functions of CD73 in immunosuppression in pancreatic cancer, an ideal model characterized by complex crosstalk among cancer metabolism, immune microenvironment, and immunotherapeutic resistance. The synergistic effect of CD73-specific drugs in combination with immune checkpoint blockade is observed in multiple pancreatic cancer models. Cytometry by time-of-flight analysis shows that CD73 inhibition reduces tumor-infiltrating Tregs in pancreatic cancer. Tumor cell-autonomous CD73 is found to facilitate Treg recruitment, in which CCL5 is identified as a significant downstream effector of CD73 using integrated proteomic and transcriptomic analyses. CD73 transcriptionally upregulates CCL5 through tumor cell-autocrine adenosine–Adora2a signaling-mediated activation of the p38–STAT1 axis, recruiting Tregs to pancreatic tumors and causing an immunosuppressive microenvironment. Together, this study highlights that CD73–adenosine metabolism transcriptionally controls pancreatic cancer immunosuppression in a tumor-autonomous and -autocrine manner.

Suggested Citation

  • Tianyu Tang & Xing Huang & Minghao Lu & Gang Zhang & Xu Han & Tingbo Liang, 2023. "Transcriptional control of pancreatic cancer immunosuppression by metabolic enzyme CD73 in a tumor-autonomous and -autocrine manner," Nature Communications, Nature, vol. 14(1), pages 1-18, December.
    • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-38578-3
    DOI: 10.1038/s41467-023-38578-3
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    References listed on IDEAS

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    1. Luis Felipe Campesato & Sadna Budhu & Jeremy Tchaicha & Chien-Huan Weng & Mathieu Gigoux & Ivan Jose Cohen & David Redmond & Levi Mangarin & Stephane Pourpe & Cailian Liu & Roberta Zappasodi & Dmitriy, 2020. "Blockade of the AHR restricts a Treg-macrophage suppressive axis induced by L-Kynurenine," Nature Communications, Nature, vol. 11(1), pages 1-11, December.
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