Repeated dosing improves oncolytic rhabdovirus therapy in mice via interactions with intravascular monocytes

Author:

Naumenko VictorORCID,Rajwani Jahanara,Turk MadisonORCID,Zhang Chunfen,Tse Mandy,Davis Rachelle P.,Kim Daesun,Rakic Andrea,Dastidar Himika,Van Shinia,Mah Laura K.,Kaul Esha K.,Chekhonin Vladimir P.,Mahoney Douglas J.ORCID,Jenne Craig N.ORCID

Abstract

AbstractThere is debate in the field of oncolytic virus (OV) therapy, whether a single viral dose, or multiple administrations, is better for tumor control. Using intravital microscopy, we describe the fate of vesicular stomatitis virus (VSV) delivered systemically as a first or a second dose. Following primary administration, VSV binds to the endothelium, initiates tumor infection and activates a proinflammatory response. This initial OV dose induces neutrophil migration into the tumor and limits viral replication. OV administered as a second dose fails to infect the tumor and is captured by intravascular monocytes. Despite a lack of direct infection, this second viral dose, in a monocyte-dependent fashion, enhances and sustains infection by the first viral dose, promotes CD8 T cell recruitment, delays tumor growth and improves survival in multi-dosing OV therapy. Thus, repeated VSV dosing engages monocytes to post-condition the tumor microenvironment for improved infection and anticancer T cell responses. Understanding the complex interactions between the subsequent viral doses is crucial for improving the efficiency of OV therapy and virus-based vaccines.

Funder

Canadian Cancer Society Research Institute

Gouvernement du Canada | Instituts de Recherche en Santé du Canada | CIHR Skin Research Training Centre

Publisher

Springer Science and Business Media LLC

Subject

General Agricultural and Biological Sciences,General Biochemistry, Genetics and Molecular Biology,Medicine (miscellaneous)

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