Improvement of current immunotherapies with engineered oncolytic viruses that target cancer stem cells

Author:

Soroush Alborz1,Shahhosseini Reza2,Ghavamikia Nima3,Hjazi Ahmed4,Roudaki Shahrzad5,KhalatbariLimaki Mahdi6,Mirbolouk Mahtab7,Pakmehr SeyedAbbas8,Karimi Parvin9ORCID

Affiliation:

1. Ramsay Pharmacy Group Melbourne Australia

2. Faculty of Medicine Istanbul Medipol University Istanbul Turkey

3. Cardiovascular Research Institute, Tehran Heart Center Tehran University of Medical Sciences Tehran Iran

4. Department of Medical Laboratory Sciences, College of Applied Medical Sciences Prince Sattam bin AbdulAziz University Al‐Kharj Saudi Arabia

5. School of Pharmacy Shiraz University of Medical Sciences Shiraz Iran

6. School of Pharmacy Guilan University of Medical Sciences Rasht Iran

7. School of Pharmacy Cyprus International University Nicosia North Cyprus

8. School of Medicine Shiraz University of Medical Sciences Shiraz Iran

9. Fars Population‐Based Cancer Registry Shiraz University of Medical Sciences Shiraz Iran

Abstract

AbstractThe heterogeneity of the solid tumor microenvironment (TME) impairs the therapeutic efficacy of standard therapies and also reduces the infiltration of antitumor immune cells, all of which lead to tumor progression and invasion. In addition, self‐renewing cancer stem cells (CSCs) support tumor dormancy, drug resistance, and recurrence, all of which might pose challenges to the eradication of malignant tumor masses with current therapies. Natural forms of oncolytic viruses (OVs) or engineered OVs are known for their potential to directly target and kill tumor cells or indirectly eradicate tumor cells by involving antitumor immune responses, including enhancement of infiltrating antitumor immune cells, induction of immunogenic cell death, and reprogramming of cold TME to an immune‐sensitive hot state. More importantly, OVs can target stemness factors that promote tumor progression, which subsequently enhances the efficacy of immunotherapies targeting solid tumors, particularly the CSC subpopulation. Herein, we describe the role of CSCs in tumor heterogeneity and resistance and then highlight the potential and remaining challenges of immunotherapies targeting CSCs. We then review the potential of OVs to improve tumor immunogenicity and target CSCs and finally summarize the challenges within the therapeutic application of OVs in preclinical and clinical trials.

Funder

Prince Sattam bin Abdulaziz University

Publisher

Wiley

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