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

Javed Iqbal, Muhammad Hassan Hafeez, Aamir Amin, Iman Moradi, Anisha Chhabra, Ather Iqbal, Tirath Patel, Muhammad Ashir Shafique, Abdullah Nadeem, Usama Jamil
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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.
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疱疹溶解病毒和环磷酰胺治疗复发性恶性胶质瘤的协同效应:综述
胶质瘤占脑部恶性肿瘤的近80%,是最具侵袭性的亚型胶质母细胞瘤,是一项艰巨的挑战。尽管有包括手术和放化疗在内的多学科治疗,但预后仍然不容乐观,因此需要创新的治疗策略。血脑屏障使药物的获取变得复杂,组织病理学的多样性也阻碍了靶向治疗。肿瘤溶解性疱疹病毒(oHSV),尤其是 HSV1716、G207 和 rQNestin34.5v,通过选择性地在肿瘤细胞中复制,显示出治疗胶质瘤的前景。临床前和临床研究证明了 oHSVs 的安全性和有效性,其中 T-Vec 已获得美国 FDA 批准。然而,病毒传递限制和抗病毒反应等挑战依然存在。oHSVs 与环磷酰胺(CPA)的结合解决了这些难题,显示出更强的转基因表达和病毒活性。环磷酰胺的免疫抑制特性,尤其是在节律性计划中,可提高 oHSV 的疗效,支持将这种组合用于复发性恶性胶质瘤的开发。CPA 与 oHSVs 可增强病毒溶解并延长存活期。CPA 的免疫调节作用可抑制调节性 T 细胞,从而提高 oHSV 的效率。虽然障碍依然存在,但这种协同方法为改善疗效带来了希望,需要进一步的研究和临床验证。
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