Tumor Microenvironment Specific Regulation Ca‐Fe‐Nanospheres for Ferroptosis‐Promoted Domino Synergistic Therapy and Tumor Immune Response

Author:

Chu Xu1,Hou Hua‐Ying2,Duan Meng‐Die2,Zhang Yu‐Juan2,Zhu Yu‐Ying1,Liu Yi134,Li Shu‐Lan1ORCID

Affiliation:

1. State Key Laboratory of Separation Membranes and Membrane Processes & Key Laboratory of Hollow Fiber Membrane Materials and Membrane Processes (MOE) School of Material Science and Engineering & School of Chemistry Tiangong University Tianjin 300387 P. R. China

2. School of Electronic and Information Engineering & School of Chemical Engineering and Technology Tiangong University Tianjin 300387 P. R. China

3. School of Chemical and Environmental Engineering Wuhan Polytechnic University Wuhan 430023 P. R. China

4. Hubei Key Laboratory of Radiation Chemistry and Functional Materials School of Nuclear Technology and Chemistry and Biology Hubei University of Science and Technology Xianning 437100 China

Abstract

AbstractReactive oxygen species (ROS)‐mediated emerging treatments exhibit unique advantages in cancer therapy in recent years. While the efficacy of ROS‐involved tumor therapy is greatly restricted by complex tumor microenvironment (TME). Herein, a dual‐metal CaO2@CDs‐Fe (CCF) nanosphere, with TME response and regulation capabilities, are proposed to improve ROS lethal power by a multiple cascade synergistic therapeutic strategy with domino effect. In response to weak acidic TME, CCF will decompose, accompanied with intracellular Ca2+ upregulated and abundant H2O2 and O2 produced to reverse antitherapeutic TME. Then the exposed CF cores can act as both Fenton agent and sonosensitizer to generate excessive ROS in the regulated TME for enhanced synergistic CDT/SDT. In combination with calcium overloading, the augmented ROS induced oxidative stress will cause more severe mitochondrial damage and cellular apoptosis. Furthermore, CCF can also reduce GPX4 expression and enlarge the lipid peroxidation, causing ferroptosis and apoptosis in parallel. These signals of damage will finally initiate damage‐associated molecular patterns to activate immune response and to realize excellent antitumor effect. This outstanding domino ROS/calcium loading synergistic effect endows CCF with excellent anticancer effect to efficiently eliminate tumor by apoptosis/ferroptosis/ICD both in vitro and in vivo.

Funder

National Natural Science Foundation of China

Natural Science Foundation of Tianjin Municipality

Publisher

Wiley

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