Abstract
Previously, we described VSV-GP, a modified version of the vesicular stomatitis virus, as a non-neurotoxic oncolytic virus that is effective for the treatment of malignant glioblastoma and ovarian cancer. Here, we evaluate the therapeutic efficacy of VSV-GP for malignant melanoma. All of the human, mouse, and canine melanoma cell lines that were tested, alongside most primary human melanoma cultures, were infected by VSV-GP and efficiently killed. Additionally, we found that VSV-GP prolonged the survival of mice in both a xenograft and a syngeneic mouse model. However, only a few mice survived with long-term tumor remission. When we analyzed the factors that might limit VSV-GP’s efficacy, we found that vector-neutralizing antibodies did not play a role in this context, as even after eight subsequent immunizations and an observation time of 42 weeks, no vector-neutralizing antibodies were induced in VSV-GP immunized mice. In contrast, the type I IFN response might have contributed to the reduced efficacy of the therapy, as both of the cell lines that were used for the mouse models were able to mount a protective IFN response. Nevertheless, early treatment with VSV-GP also reduced the number and size of lung metastases in a syngeneic B16 mouse model. In summary, VSV-GP is a potent candidate for the treatment of malignant melanoma; however, factors limiting the efficacy of the virus need to be further explored.
Highlights
Melanoma is the leading cause (80%) of death from skin disease, it accounts for only 4%of all dermatologic cancers [1]
To assess the susceptibility of malignant melanoma to VSV-GP-mediated oncolytic virotherapy, we first analyzed a panel of human (A375, MDA-mB-435, MJS, NW1539, SK-MEL3, SK-MEL5), one mouse (B16-OVA), and one dog (UCDK9-M1) melanoma cell lines in vitro
The percentage of infected cells was analyzed via GFP expression using flow cytometry and the titers for VSV-G or lymphocytic choriomeningitis virus (LCMV)-GP pseudotyped viruses were calculated for each cell line
Summary
Of all dermatologic cancers [1] It is the fifth most frequently diagnosed malignancy in men and the seventh in women, with an estimation of 91,270 new cases in the United States (US) in 2018 [2,3]. The overall five-year survival rate for melanoma is 91.3%, but the prognosis is only good for patients with early stage disease, where surgical removal is possible, and tumors have not yet spread. The five-year survival rate for patients with late stage melanoma is much lower, e.g., only 16%. For metastatic stage IV melanoma [4] For this patient group, new immunotherapies have already considerably improved the prognosis. Only a fraction of tumor patients respond to checkpoint inhibitor therapy. A combination of two checkpoint inhibitors, e.g., ipilimumab and nivolumab, improves response rates. Side effects are enhanced, and still, a considerable proportion of patients does not respond [7,8]
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