AI Article Synopsis
- Oncolytic viruses, like bovine herpesvirus-1 (BoHV-1), are designed to selectively attack cancer cells while enhancing the body's immune response.
- Research shows that both live and UV-inactivated (non-replicating) BoHV-1 can effectively extend the survival of mice with tumors by promoting similar immune cell infiltration, excluding neutrophils.
- Additionally, transcriptomic analysis indicates that both forms of BoHV-1 activate similar biological pathways and gene expressions, challenging the idea that viral replication is essential for their therapeutic benefits.
Article Abstract
Oncolytic viruses are a promising approach for cancer treatment where viruses selectively target and kill cancer cells while also stimulating an immune response. Among viruses with this ability, bovine herpesvirus-1 (BoHV-1) has several advantages, including observations suggesting it may not require viral replication for its anti-cancer effects. We previously demonstrated that binding and penetration of enveloped virus particles are sufficient to trigger intrinsic and innate immune signaling in normal cells, while other groups have published the efficacy of non-replicating viruses as viable immunotherapies in different cancer models. In this work, we definitively show that live and UV-inactivated (UV) (non-replicating) BoHV-1-based regimens extend survival of tumor-bearing mice to similar degrees and induce infiltration of similar immune cell populations, with the exception of neutrophils. Transcriptomic analysis of tumors treated with either live or UV BoHV-1-based regimens revealed similar pathway enrichment and a subset of overlapping differentially regulated genes, suggesting live and UV BoHV-1 have similar mechanisms of activity. Last, we present a gene signature across our and models that could potentially be used to validate new BoHV-1 therapeutics. This work contributes to the growing body of literature showing that replication may not be necessary for therapeutic efficacy of viral immunotherapies.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11650296 | PMC |
| http://dx.doi.org/10.1016/j.omton.2024.200906 | DOI Listing |
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