Advances in cell-based delivery of oncolytic viruses as therapy for lung cancer
- PMID: 38596310
- PMCID: PMC10976516
- DOI: 10.1016/j.omton.2024.200788
Advances in cell-based delivery of oncolytic viruses as therapy for lung cancer
Erratum in
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Erratum: Advances in cell-based delivery of oncolytic viruses as therapy for lung cancer.Mol Ther Oncol. 2024 Jul 23;32(3):200848. doi: 10.1016/j.omton.2024.200848. eCollection 2024 Sep 19. Mol Ther Oncol. 2024. PMID: 39135745 Free PMC article.
Abstract
Lung cancer's intractability is enhanced by its frequent resistance to (chemo)therapy and often high relapse rates that make it the leading cause of cancer death worldwide. Improvement of therapy efficacy is a crucial issue that might lead to a significant advance in the treatment of lung cancer. Oncolytic viruses are desirable combination partners in the developing field of cancer immunotherapy due to their direct cytotoxic effects and ability to elicit an immune response. Systemic oncolytic virus administration through intravenous injection should ideally lead to the highest efficacy in oncolytic activity. However, this is often hampered by the prevalence of host-specific, anti-viral immune responses. One way to achieve more efficient systemic oncolytic virus delivery is through better protection against neutralization by several components of the host immune system. Carrier cells, which can even have innate tumor tropism, have shown their appropriateness as effective vehicles for systemic oncolytic virus infection through circumventing restrictive features of the immune system and can warrant oncolytic virus delivery to tumors. In this overview, we summarize promising results from studies in which carrier cells have shown their usefulness for improved systemic oncolytic virus delivery and better oncolytic virus therapy against lung cancer.
Keywords: antibody neutralization; cell-mediated carrier; lung cancer; oncolytic viral therapy; _target delivery.
© 2024 The Author(s).
Conflict of interest statement
The authors declare no conflict of interest. This work was supported in part by TÜSEB grant no. 2022-B-01-16483 (to R.M.), for the design of the study; in the collection, analyses, or interpretation of data; in the writing of the manuscript or in the decision to publish the results.
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