OncoImmunology (Jan 2019)

IL-33 delays metastatic peritoneal cancer progression inducing an allergic microenvironment

  • Alfredo Perales-Puchalt,
  • Nikolaos Svoronos,
  • Daniel O. Villarreal,
  • Urvi Zankharia,
  • Emma Reuschel,
  • Krzysztof Wojtak,
  • Kyle K. Payne,
  • Elizabeth K. Duperret,
  • Kar Muthumani,
  • Jose R. Conejo-Garcia,
  • David B. Weiner

DOI
https://doi.org/10.1080/2162402X.2018.1515058
Journal volume & issue
Vol. 8, no. 1

Abstract

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Ovarian cancer is frequently diagnosed as peritoneal carcinomatosis. Unlike other tumor locations, the peritoneal cavity is commonly exposed to gut-breaching and ascending genital microorganisms and has a unique immune environment. IL-33 is a local cytokine that can activate innate and adaptive immunity. We studied the effectiveness of local IL-33 delivery in the treatment of cancer that has metastasized to the peritoneal cavity. Direct peritoneal administration of IL-33 delayed the progression of metastatic peritoneal cancer. Prolongation in survival was not associated with a direct effect of IL-33 on tumor cells, but with major changes in the immune microenvironment of the tumor. IL-33 promoted a significant increase in the leukocyte compartment of the tumor immunoenvironment and an allergic cytokine profile. We observed a substantial increase in the number of activated CD4+ T-cells accompanied by peritoneal eosinophil infiltration, B-cell activation and activation of peritoneal macrophages which displayed tumoricidal capacity. Depletion of CD4+ cells, eosinophils or macrophages reduced the anti-tumor effects of IL-33 but none of these alone were sufficient to completely abrogate its positive benefit. In conclusion, local administration of IL-33 generates an allergic tumor environment resulting in a novel approach for treatment of metastatic peritoneal malignancies, such as advanced ovarian cancer.

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