A T‐Cell Inspired Sonoporation System Enhances Low‐Dose X‐Ray‐Mediated Pyroptosis and Radioimmunotherapy Efficacy by Restoring Gasdermin‐E Expression

Author:

Yin Hao12,Hu Xiaoqu3,Xie Congying13,Li Yida1,Gao Yanjun1,Zeng Hanqian3,Zhu Wenting4,Xie Danli2,Wang Qinyang12ORCID

Affiliation:

1. Department of Radiation and Medical Oncology Wenzhou Key Laboratory of Basic Science and Translational Research of Radiation Oncology Zhejiang Engineering Research Center for Innovation and Application of Intelligent Radiotherapy Technology The Second Affiliated Hospital and Yuying Children's Hospital of Wenzhou Medical University Wenzhou Zhejiang 325035 P. R. China

2. Institute for Advanced Research Wenzhou Medical University Wenzhou Zhejiang 325035 P. R. China

3. Department of Radiation and Medical Oncology The First Affiliated Hospital of Wenzhou Medical University Wenzhou Medical University Wenzhou Zhejiang 325035 P. R. China

4. Department of Oncology Xijing Hospital of Air Force Military Medical University Shaanxi Xi'an 710032 China

Abstract

AbstractGenome editing has the potential to improve the unsatisfactory therapeutic effect of antitumor immunotherapy. However, the cell plasma membrane prevents the entry of almost all free genome‐manipulation agents. Therefore, a system can be spatiotemporally controlled and can instantly open the cellular membrane to allow the entry of genome‐editing agents into target cells is needed. Here, inspired by the ability of T cells to deliver cytotoxins to cancer cells by perforation, an ultrasound (US)‐controlled perforation system (UPS) is established to enhance the delivery of free genome‐manipulating agents. The UPS can perforate the tumor cell membrane while maintaining cell viability via a controllable lipid peroxidation reaction. In vitro, transmembrane‐incapable plasmids can enter cells and perform genome editing with the assistance of UPS, achieving an efficiency of up to 90%. In vivo, the UPS is biodegradable, nonimmunogenic, and tumor‐targeting, enabling the puncturing of tumor cells under US. With the application of UPS‐assisted genome editing, gasdermin‐E expression in 4T1 tumor‐bearing mice is successfully restored, which leads to pyroptosis‐mediated antitumor immunotherapy via low‐dose X‐ray irradiation. This study provides new insights for designing a sonoporation system for genome editing. Moreover, the results demonstrate that restoring gasdermin expression by genome editing significantly improves the efficacy of radioimmunotherapy.

Funder

National Natural Science Foundation of China

Publisher

Wiley

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