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Triggering endogenous Z-RNA sensing for anti-tumor therapy through ZBP1-dependent necroptosis

Tao Yang, Guodong Wang, Mingxiang Zhang, Xiaohu Hu, Qi Li, Fenglin Yun, Yingying Xing, Xinyang Song, Haibing Zhang, Guohong Hu, Youcun Qian

2023Cell Reports51 citationsDOIOpen Access PDF

Abstract

ZBP1 senses viral Z-RNAs to induce necroptotic cell death to restrain viral infection. ZBP1 is also thought to recognize host cell-derived Z-RNAs to regulate organ development and tissue inflammation in mice. However, it remains unknown how the host-derived Z-RNAs are formed and how these endogenous Z-RNAs are sensed by ZBP1. Here, we report that oxidative stress strongly induces host cell endogenous Z-RNAs, and the Z-RNAs then localize to stress granules for direct sensing by ZBP1 to trigger necroptosis. Oxidative stress triggers dramatically increase Z-RNA levels in tumor cells, and the Z-RNAs then directly trigger tumor cell necroptosis through ZBP1. Localization of the induced Z-RNAs to stress granules is essential for ZBP1 sensing. Oxidative stress-induced Z-RNAs significantly promote tumor chemotherapy via ZBP1-driven necroptosis. Thus, our study identifies oxidative stress as a critical trigger for Z-RNA formation and demonstrates how Z-RNAs are directly sensed by ZBP1 to trigger anti-tumor necroptotic cell death.

Topics & Concepts

NecroptosisProgrammed cell deathCell biologyEndogenyBiologyRNAStress granuleOxidative stressCancer researchApoptosisMessenger RNABiochemistryTranslation (biology)GeneRNA Research and SplicingRNA modifications and cancerinterferon and immune responses