4.6 Review

The Multifaceted Role of Macrophages in Oncolytic Virotherapy

Journal

VIRUSES-BASEL
Volume 13, Issue 8, Pages -

Publisher

MDPI
DOI: 10.3390/v13081570

Keywords

cancer immunotherapy; oncolytic virotherapy; tumour microenvironment; innate immune system; tumour-associated macrophages; M1; M2 phenotypic shift; anti-tumour immunity

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The role of macrophages in oncolytic virotherapy is multifaceted, with potential contributions to both anti-viral responses and anti-inflammatory, tumour-suppressive properties. Oncolytic viruses have been shown to induce a phenotypic shift in macrophages towards an anti-inflammatory state, mediating immune responses and inhibiting cancer immune evasion.
One of the cancer hallmarks is immune evasion mediated by the tumour microenvironment (TME). Oncolytic virotherapy is a form of immunotherapy based on the application of oncolytic viruses (OVs) that selectively replicate in and induce the death of tumour cells. Virotherapy confers reciprocal interaction with the host's immune system. The aim of this review is to explore the role of macrophage-mediated responses in oncolytic virotherapy efficacy. The approach was to study current scientific literature in this field in order to give a comprehensive overview of the interactions of OVs and macrophages and their effects on the TME. The innate immune system has a central influence on the TME; tumour-associated macrophages (TAMs) generally have immunosuppressive, tumour-supportive properties. In the context of oncolytic virotherapy, macrophages were initially thought to predominantly contribute to anti-viral responses, impeding viral spread. However, macrophages have now also been found to mediate transport of OV particles and, after TME infiltration, to be subjected to a phenotypic shift that renders them pro-inflammatory and tumour-suppressive. These TAMs can present tumour antigens leading to a systemic, durable, adaptive anti-tumour immune response. After phagocytosis, they can recirculate carrying tissue-derived proteins, which potentially enables the monitoring of OV replication in the TME. Their role in therapeutic efficacy is therefore multifaceted, but based on research applying relevant, immunocompetent tumour models, macrophages are considered to have a central function in anti-cancer activity. These novel insights hold important clinical implications. When optimised, oncolytic virotherapy, mediating multifactorial inhibition of cancer immune evasion, could contribute to improved patient survival.

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