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Priming a vascular-selective cytokine response permits CD8+ T-cell entry into tumors

Author

Listed:
  • Dae Joong Kim

    (The University of Virginia)

  • Swetha Anandh

    (The University of Virginia)

  • Jamie L. Null

    (The University of Virginia)

  • Piotr Przanowski

    (The University of Virginia)

  • Sanchita Bhatnagar

    (School of Medicine)

  • Pankaj Kumar

    (The University of Virginia)

  • Sarah E. Shelton

    (Massachusetts Institute of Technology
    Dana-Farber Cancer Institute)

  • Erin E. Grundy

    (The George Washington University Cancer Center, The George Washington University School of Medicine and Health Sciences)

  • Katherine B. Chiappinelli

    (The George Washington University Cancer Center, The George Washington University School of Medicine and Health Sciences)

  • Roger D. Kamm

    (Massachusetts Institute of Technology
    Massachusetts Institute of Technology)

  • David A. Barbie

    (Dana-Farber Cancer Institute
    Dana-Farber Cancer Institute)

  • Andrew C. Dudley

    (The University of Virginia
    The University of Virginia)

Abstract

Targeting DNA methyltransferase 1 (DNMT1) has immunomodulatory and anti-neoplastic activity, especially when paired with cancer immunotherapies. Here we explore the immunoregulatory functions of DNMT1 in the tumor vasculature of female mice. Dnmt1 deletion in endothelial cells (ECs) impairs tumor growth while priming expression of cytokine-driven cell adhesion molecules and chemokines important for CD8+ T-cell trafficking across the vasculature; consequently, the efficacy of immune checkpoint blockade (ICB) is enhanced. We find that the proangiogenic factor FGF2 promotes ERK-mediated DNMT1 phosphorylation and nuclear translocation to repress transcription of the chemokines Cxcl9/Cxcl10 in ECs. Targeting Dnmt1 in ECs reduces proliferation but augments Th1 chemokine production and extravasation of CD8+ T-cells, suggesting DNMT1 programs immunologically anergic tumor vasculature. Our study is in good accord with preclinical observations that pharmacologically disrupting DNMT1 enhances the activity of ICB but suggests an epigenetic pathway presumed to be targeted in cancer cells is also operative in the tumor vasculature.

Suggested Citation

  • Dae Joong Kim & Swetha Anandh & Jamie L. Null & Piotr Przanowski & Sanchita Bhatnagar & Pankaj Kumar & Sarah E. Shelton & Erin E. Grundy & Katherine B. Chiappinelli & Roger D. Kamm & David A. Barbie &, 2023. "Priming a vascular-selective cytokine response permits CD8+ T-cell entry into tumors," Nature Communications, Nature, vol. 14(1), pages 1-16, December.
  • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-37807-z
    DOI: 10.1038/s41467-023-37807-z
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    References listed on IDEAS

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