Transposable elements potentiate radiotherapy-induced cellular immune reactions via RIG-I-mediated virus-sensing pathways

Author:

Du Junyan,Kageyama Shun-IchiroORCID,Yamashita Riu,Tanaka Kosuke,Okumura Masayuki,Motegi Atsushi,Hojo Hidehiro,Nakamura MasakiORCID,Hirata HidenariORCID,Sunakawa HironoriORCID,Kotani DaisukeORCID,Yano Tomonori,Kojima Takashi,Hamaya Yamato,Kojima Motohiro,Nakamura YukaORCID,Suzuki AyakoORCID,Suzuki YutakaORCID,Tsuchihara KatsuyaORCID,Akimoto Tetsuo

Abstract

AbstractRadiotherapy (RT) plus immunotherapy is a promising modality; however, the therapeutic effects are insufficient, and the molecular mechanism requires clarification to further develop combination therapies. Here, we found that the RNA virus sensor pathway dominantly regulates the cellular immune response in NSCLC and ESCC cell lines. Notably, transposable elements (TEs), especially long terminal repeats (LTRs), functioned as key ligands for the RNA virus sensor RIG-I, and the mTOR–LTR–RIG-I axis induced the cellular immune response and dendritic cell and macrophage infiltration after irradiation. Moreover, RIG-I-dependent immune activation was observed in ESCC patient tissue. scRNA sequencing and spatial transcriptome analysis revealed that radiotherapy induced the expression of LTRs, and the RNA virus sensor pathway in immune and cancer cells; this pathway was also found to mediate tumour conversion to an immunological hot state. Here, we report the upstream and ligand of the RNA virus sensor pathway functions in irradiated cancer tissues.

Publisher

Springer Science and Business Media LLC

Subject

General Agricultural and Biological Sciences,General Biochemistry, Genetics and Molecular Biology,Medicine (miscellaneous)

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