Trabectedin promotes oncolytic virus antitumor efficacy, viral gene expression, and immune effector function in models of bone sarcoma.

在骨肉瘤模型中,曲贝替定可促进溶瘤病毒的抗肿瘤功效、病毒基因表达和免疫效应功能

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作者:Ringwalt Emily M, Currier Mark A, Glaspell Andrea M, Chen Chun-Yu, Cannon Matthew V, Cam Maren, Gross Amy C, Gust Matthew, Wang Pin-Yi, Boon Louis, Biederman Laura E, Schwarz Emily, Rajappa Prajwal, Lee Dean A, Mardis Elaine R, Carson William E, Roberts Ryan D, Cripe Timothy P
We previously reported that the DNA alkylator and transcriptional-blocking chemotherapeutic agent trabectedin enhances oncolytic herpes simplex viroimmunotherapy in human sarcoma xenograft models, though the mechanism remained to be elucidated. Here we report trabectedin disrupts the intrinsic cellular antiviral response which increases viral transcript presence in the human tumor cells. We also extended our synergy findings to syngeneic murine sarcoma models, which are poorly susceptible to virus infection. In the absence of robust virus replication, we found trabectedin enhanced viroimmunotherapy efficacy by reducing infiltrating immunosuppressive CD4 T and myeloid cells and stimulating granzyme expression in infiltrating T and natural killer cells to cause immune-mediated tumor regressions. Thus, trabectedin enhances both the direct virus-mediated killing of tumor cells and the viral-induced activation of cytotoxic effector lymphocytes to cause tumor regressions across models. Our data provide a strong rationale for clinical translation as both mechanisms should be simultaneously active in human patients.

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