Synergistic effects of herpes oncolytic virus and cyclophosphamide for recurrent malignant glioma: a narrative review

Author:

Iqbal Javed1,Hafeez Muhammad Hassan2,Amin Aamir3,Moradi Iman4,Chhabra Anisha5,Iqbal Ather6,Patel Tirath7,Shafique Muhammad Ashir8,Nadeem Abdullah9,Jamil Usama10

Affiliation:

1. King Edward Medical University

2. Shalamar Medical and Dental College

3. Harefield Hospital, Guy’s and St Thomas’ NHS foundation trust, Harefield, UK

4. University of British Columbia, Vancouver, BC, Canada

5. Desert Mountain High School, Scottsdale, AZ, USA

6. Shaukat Khanum Memorial Cancer Hospital and Research Centre, Lahore

7. American University of Antigua College of Medicine, Saint John, Antigua and Barbuda

8. Jinnah Sindh Medical University

9. Dow University of Health Sciences, Karachi, Pakistan

10. Kabul University, Kabul, Afghanistan

Abstract

Gliomas, comprising nearly 80% of brain malignancies, present a formidable challenge with glioblastomas being the most aggressive subtype. Despite multidisciplinary care, including surgery and chemoradiotherapy, the prognosis remains grim, emphasizing the need for innovative treatment strategies. The blood-brain barrier complicates drug access, and the diverse histopathology hinders targeted therapies. Oncolytic herpes viruses (oHSVs), particularly HSV1716, G207, and rQNestin34.5v, show promise in glioma treatment by selectively replicating in tumor cells. Preclinical and clinical studies demonstrate the safety and efficacy of oHSVs, with T-Vec being FDA-approved. However, challenges like viral delivery limitations and antiviral responses persist. The combination of oHSVs and combining cyclophosphamide (CPA) addresses these challenges, demonstrating increased transgene expression and viral activity. The immunosuppressive properties of CPA, particularly in metronomic schedules, enhance oHSV efficacy, supporting the development of this combination for recurrent malignant gliomas. CPA with oHSVs enhances viral oncolysis and extends survival. CPA’s immunomodulatory effects, suppressing regulatory T cells, improve oHSV efficiency. While obstacles remain, this synergistic approach offers hope for improved outcomes, necessitating further research and clinical validation.

Publisher

Ovid Technologies (Wolters Kluwer Health)

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