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Multi-modal Potentiation of Oncolytic Virotherapy by Vanadium Compounds.


ABSTRACT: Oncolytic viruses (OV) are an emerging class of anticancer bio-therapeutics that induce antitumor immunity through selective replication in tumor cells. However, the efficacy of OVs as single agents remains limited. We introduce a strategy that boosts the therapeutic efficacy of OVs by combining their activity with immuno-modulating, small molecule protein tyrosine phosphatase inhibitors. We report that vanadium-based phosphatase inhibitors enhance OV infection in vitro and ex vivo, in resistant tumor cell lines. Furthermore, vanadium compounds increase antitumor efficacy in combination with OV in several syngeneic tumor models, leading to systemic and durable responses, even in models otherwise refractory to OV and drug alone. Mechanistically, this involves subverting the antiviral type I IFN response toward a death-inducing and pro-inflammatory type II IFN response, leading to improved OV spread, increased bystander killing of cancer cells, and enhanced antitumor immune stimulation. Overall, we showcase a new ability of vanadium compounds to simultaneously maximize viral oncolysis and systemic anticancer immunity, offering new avenues for the development of improved immunotherapy strategies.

SUBMITTER: Selman M 

PROVIDER: S-EPMC5763159 | biostudies-literature | 2018 Jan

REPOSITORIES: biostudies-literature

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Multi-modal Potentiation of Oncolytic Virotherapy by Vanadium Compounds.

Selman Mohammed M   Rousso Christopher C   Bergeron Anabel A   Son Hwan Hee HH   Krishnan Ramya R   El-Sayes Nader A NA   Varette Oliver O   Chen Andrew A   Le Boeuf Fabrice F   Tzelepis Fanny F   Bell John C JC   Crans Debbie C DC   Diallo Jean-Simon JS  

Molecular therapy : the journal of the American Society of Gene Therapy 20171024 1


Oncolytic viruses (OV) are an emerging class of anticancer bio-therapeutics that induce antitumor immunity through selective replication in tumor cells. However, the efficacy of OVs as single agents remains limited. We introduce a strategy that boosts the therapeutic efficacy of OVs by combining their activity with immuno-modulating, small molecule protein tyrosine phosphatase inhibitors. We report that vanadium-based phosphatase inhibitors enhance OV infection in vitro and ex vivo, in resistant  ...[more]

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