Monitoring ROS Responsive Fe3O4‐based Nanoparticle Mediated Ferroptosis and Immunotherapy via 129Xe MRI

Author:

Zhang Lei12,Qiu Maosong12,Wang Ruifang12,Li Sha12,Liu Xiaoxun12,Xu Qiuyi12,Xiao Long12,Jiang Zhong‐Xing12,Zhou Xin123,Chen Shizhen123ORCID

Affiliation:

1. State Key Laboratory of Magnetic Resonance and Atomic and Molecular Physics National Center for Magnetic Resonance in Wuhan Wuhan Institute of Physics and Mathematics Innovation Academy for Precision Measurement Science and Technology Chinese Academy of Sciences – Wuhan National Laboratory for Optoelectronics Wuhan 430071 P. R. China

2. University of Chinese Academy of Sciences Beijing 100049 P. R. China

3. School of Biomedical Engineering Hainan University Haikou Hainan 570228 P. R. China

Abstract

AbstractThe immune checkpoint blockade strategy has improved the survival rate of late‐stage lung cancer patients. However, the low immune response rate limits the immunotherapy efficiency. Here, we report a ROS‐responsive Fe3O4‐based nanoparticle that undergoes charge reversal and disassembly in the tumor microenvironment, enhancing the uptake of Fe3O4 by tumor cells and triggering a more severe ferroptosis. In the tumor microenvironment, the nanoparticle rapidly disassembles and releases the loaded GOx and the immune‐activating peptide Tuftsin under overexpressed H2O2. GOx can consume the glucose of tumor cells and generate more H2O2, promoting the disassembly of the nanoparticle and drug release, thereby enhancing the therapeutic effect of ferroptosis. Combined with Tuftsin, it can more effectively reverse the immune‐suppressive microenvironment and promote the recruitment of effector T cells in tumor tissues. Ultimately, in combination with α‐PD‐L1, there is significant inhibition of the growth of lung metastases. Additionally, the hyperpolarized 129Xe method has been used to evaluate the Fe3O4 nanoparticle‐mediated immunotherapy, where the ventilation defects in lung metastases have been significantly improved with complete lung structure and function recovered. The ferroptosis‐enhanced immunotherapy combined with non‐radiation evaluation methodology paves a new way for designing novel theranostic agents for cancer therapy.

Funder

Key Technologies Research and Development Program

National Natural Science Foundation of China

Natural Science Foundation of Hubei Province

Publisher

Wiley

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