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Oncolytic virus–mediated expansion of dual-specific CAR T cells improves efficacy against solid tumors in mice

嵌合抗原受体 溶瘤病毒 癌症研究 T细胞受体 T细胞 抗原 生物 水泡性口炎病毒 黑色素瘤 免疫疗法 胶质瘤 免疫学 病毒学 免疫系统 病毒
作者
Laura Evgin,Tim Kottke,Jason M. Tonne,Jill Thompson,Amanda L. Huff,Jacob P. van Vloten,Madelyn Moore,Josefine Michael,Christopher B. Driscoll,José S. Pulido,Eric Swanson,Richard B. Kennedy,Matt Coffey,Houra Loghmani,Luis Sánchez-Pérez,Gloria Olivier,Kevin J. Harrington,Hardev Pandha,Alan Melcher,Rosa María Díaz
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science]
卷期号:14 (640): eabn2231-eabn2231 被引量:201
标识
DOI:10.1126/scitranslmed.abn2231
摘要

Oncolytic viruses (OVs) encoding a variety of transgenes have been evaluated as therapeutic tools to increase the efficacy of chimeric antigen receptor (CAR)-modified T cells in the solid tumor microenvironment (TME). Here, using systemically delivered OVs and CAR T cells in immunocompetent mouse models, we have defined a mechanism by which OVs can potentiate CAR T cell efficacy against solid tumor models of melanoma and glioma. We show that stimulation of the native T cell receptor (TCR) with viral or virally encoded epitopes gives rise to enhanced proliferation, CAR-directed antitumor function, and distinct memory phenotypes. In vivo expansion of dual-specific (DS) CAR T cells was leveraged by in vitro preloading with oncolytic vesicular stomatitis virus (VSV) or reovirus, allowing for a further in vivo expansion and reactivation of T cells by homologous boosting. This treatment led to prolonged survival of mice with subcutaneous melanoma and intracranial glioma tumors. Human CD19 CAR T cells could also be expanded in vitro with TCR reactivity against viral or virally encoded antigens and was associated with greater CAR-directed cytokine production. Our data highlight the utility of combining OV and CAR T cell therapy and show that stimulation of the native TCR can be exploited to enhance CAR T cell activity and efficacy in mice.
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