An oncolytic virus delivering tumor-irrelevant bystander T cell epitopes induces anti-tumor immunity and potentiates cancer immunotherapy

Author:

Chen Xiangyu,Zhao Jing,Yue Shuai,Li Ziyu,Duan Xiang,Lin Yao,Yang Yang,He Junjian,Gao Leiqiong,Pan Zhiwei,Yang Xiaofan,Su Xingxing,Huang Min,Li Xiao,Zhao Ye,Zhang Xuehui,Li Zhirong,Hu Li,Tang Jianfang,Hao Yaxing,Tian QinORCID,Wang Yifei,Xu Lifan,Huang Qizhao,Cao Yingjiao,Chen Yaokai,Zhu Bo,Li YanORCID,Bai FanORCID,Zhang GuozhongORCID,Ye LilinORCID

Abstract

AbstractTumor-specific T cells are crucial in anti-tumor immunity and act as targets for cancer immunotherapies. However, these cells are numerically scarce and functionally exhausted in the tumor microenvironment (TME), leading to inefficacious immunotherapies in most patients with cancer. By contrast, emerging evidence suggested that tumor-irrelevant bystander T (TBYS) cells are abundant and preserve functional memory properties in the TME. To leverage TBYS cells in the TME to eliminate tumor cells, we engineered oncolytic virus (OV) encoding TBYS epitopes (OV-BYTE) to redirect the antigen specificity of tumor cells to pre-existing TBYS cells, leading to effective tumor inhibition in multiple preclinical models. Mechanistically, OV-BYTE induced epitope spreading of tumor antigens to elicit more diverse tumor-specific T cell responses. Remarkably, the OV-BYTE strategy targeting human severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2)-specific T cell memory efficiently inhibited tumor progression in a human tumor cell-derived xenograft model, providing important insights into the improvement of cancer immunotherapies in a large population with a history of SARS-CoV-2 infection or coronavirus disease 2019 (COVID-19) vaccination.

Funder

National Natural Science Foundation of China

Publisher

Springer Science and Business Media LLC

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