Treatment of malignant melanoma with coxsackievirus A21 (V937): An emerging oncolytic virotherapy

Author:

Sakunchotpanit Goranit12ORCID,Patil Mihir K.13ORCID,Venkatesh Kaushik14,Rohan Thomas Z.15,Cheng Debby14,Nambudiri Vinod E.14

Affiliation:

1. Department of Dermatology Brigham and Women's Hospital Boston Massachusetts USA

2. Tufts University School of Medicine Boston Massachusetts USA

3. Carle Illinois College of Medicine Urbana Illinois USA

4. Harvard Medical School Boston Massachusetts USA

5. Sidney Kimmel Medical College Thomas Jefferson University Philadelphia Pennsylvania USA

Abstract

AbstractDespite rising melanoma incidence in recent decades, there is a trend towards overall decreased mortality, reflecting multiple factors including improved treatment options for metastatic disease. While local treatments are the mainstay for early‐stage melanoma, metastatic disease necessitates systemic treatment, with oncolytic virotherapy emerging as a promising option. For this review, articles were retrieved from PubMed from 1964 through 2024. We conducted title, abstract and full‐text screening in accordance with Preferred Reporting Items for Systematic Reviews and Meta‐Analyses guidelines to identify articles describing the use of coxsackievirus A21 (V937), either as monotherapy or as part of combination therapy for malignant melanoma. Fifteen articles met inclusion criteria, offering preclinical and clinical data on V937's efficacy in reducing tumour burden. In addition to reporting manageable safety profiles, clinical trial data examining intratumoral V937 combination therapy with pembrolizumab and ipilimumab also endorsed favourable objective response rates compared to immune checkpoint inhibitor monotherapy (47% vs. 38% and 21% vs. 10%, respectively). In contrast, intravenous V937 monotherapy failed to yield additional benefit in a cohort of patients with Stage IIIC/IV melanoma (n = 3) despite achieving detectable levels in tumour tissue (1 × 109 TCID50). Although small subsets of patients experienced severe adverse effects and study design limitations imposed constraints on collected data, evidence for the efficacy of V937 remains encouraging. With few clinical trials evaluating V937 in melanoma, additional data is required before routine usage in standard treatment for metastatic lesions.

Publisher

Wiley

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