Frontiers in Immunology (Nov 2022)

Vanadyl sulfate-enhanced oncolytic virus immunotherapy mediates the antitumor immune response by upregulating the secretion of pro-inflammatory cytokines and chemokines

  • Nouf Alluqmani,
  • Nouf Alluqmani,
  • Nouf Alluqmani,
  • Anna Jirovec,
  • Anna Jirovec,
  • Zaid Taha,
  • Zaid Taha,
  • Oliver Varette,
  • Andrew Chen,
  • Daniel Serrano,
  • Glib Maznyi,
  • Sarwat Khan,
  • Nicole E. Forbes,
  • Rozanne Arulanandam,
  • Rebecca C. Auer,
  • Rebecca C. Auer,
  • Jean-Simon Diallo,
  • Jean-Simon Diallo

DOI
https://doi.org/10.3389/fimmu.2022.1032356
Journal volume & issue
Vol. 13

Abstract

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Oncolytic viruses (OVs) are promising anticancer treatments that specifically replicate in and kill cancer cells and have profound immunostimulatory effects. We previously reported the potential of vanadium-based compounds such as vanadyl sulfate (VS) as immunostimulatory enhancers of OV immunotherapy. These compounds, in conjunction with RNA-based OVs such as oncolytic vesicular stomatitis virus (VSVΔ51), improve viral spread and oncolysis, leading to long-term antitumor immunity and prolonged survival in resistant tumor models. This effect is associated with a virus-induced antiviral type I IFN response shifting towards a type II IFN response in the presence of vanadium. Here, we investigated the systemic impact of VS+VSVΔ51 combination therapy to understand the immunological mechanism of action leading to improved antitumor responses. VS+VSVΔ51 combination therapy significantly increased the levels of IFN-γ and IL-6, and improved tumor antigen-specific T-cell responses. Supported by immunological profiling and as a proof of concept for the design of more effective therapeutic regimens, we found that local delivery of IL-12 using VSVΔ51 in combination with VS further improved therapeutic outcomes in a syngeneic CT26WT colon cancer model.

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