Molecular Therapy: Oncolytics (Dec 2023)

miR-146a inhibits ovarian tumor growth in vivo via targeting immunosuppressive neutrophils and enhancing CD8+ T cell infiltration

  • Rui Chen,
  • Elaina Coleborn,
  • Chintan Bhavsar,
  • Yue Wang,
  • Louisa Alim,
  • Andrew N. Wilkinson,
  • Michelle A. Tran,
  • Gowri Irgam,
  • Sharat Atluri,
  • Kiefer Wong,
  • Jae-Jun Shim,
  • Siddharth Adityan,
  • Ju-Seog Lee,
  • Willem W. Overwijk,
  • Raymond Steptoe,
  • Da Yang,
  • Sherry Y. Wu

Journal volume & issue
Vol. 31
p. 100725

Abstract

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Immunotherapies have emerged as promising strategies for cancer treatment. However, existing immunotherapies have poor activity in high-grade serous ovarian cancer (HGSC) due to the immunosuppressive tumor microenvironment and the associated low tumoral CD8+ T cell (CTL) infiltration. Through multiple lines of evidence, including integrative analyses of human HGSC tumors, we have identified miR-146a as a master regulator of CTL infiltration in HGSC. Tumoral miR-146a expression is positively correlated with anti-cancer immune signatures in human HGSC tumors, and delivery of miR-146a to tumors resulted in significant reduction in tumor growth in both ID8-p53−/− and IG10 murine HGSC models. Increasing miR-146a expression in tumors improved anti-tumor immune responses by decreasing immune suppressive neutrophils and increasing CTL infiltration. Mechanistically, miR-146a targets IL-1 receptor-associated kinase 1 and tumor necrosis factor receptor-associated factor 6 adaptor molecules of the transcription factor nuclear factor κB signaling pathway in ID8-p53−/− cells and decreases production of the downstream neutrophil chemoattractant, C-X-C motif chemokine ligand 1. In addition to HGSC, tumoral miR-146a expression also correlates strongly with CTL infiltration in other cancer types including thyroid, prostate, breast, and adrenocortical cancers. Altogether, our findings highlight the ability of miR-146a to overcome immune suppression and improve CTL infiltration in tumors.

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