Dual‐Functional Artificial Peroxidases with Ferriporphyrin Centers for Amplifying Tumor Immunotherapies via Immunogenic Cell Death

Abstract Constructing highly effective sonosensitizers that integrate tumor microenvironment (TME)‐adaptive and ultrasound (US)‐controllable production of reactive oxygen species (ROS) to amplify tumor immunotherapies is extremely desirable but remains challenging. Here, inspired by the coordination structure and biocatalytic effects of Fe‐based peroxidase, a dual‐functional artificial peroxidase is synthesized with ferriporphyrin networks (FePorNW‐DAP) to serve a TME‐adaptive and US‐controllable ROS‐generator for amplifying tumor immunotherapies in breast cancer via immunogenic cell death. Owing to the structural advantages of the ferriporphyrin‐based large d–π‐conjugated networks with the monatomic Fe─N 4 coordination center, moderate interaction with H 2 O 2 , and decreased bandgap, the FePorNW‐DAP displays efficient dual‐functional ROS production capabilities to combat tumor cells and amplify the tumor immunotherapies, 1) utilize locally produced H 2 O 2 in the TME to catalytically generate potent •OH and other ROS species; simultaneously, 2) external US irradiation can further boost the generation of •OH and 1 O 2 . This work provides not only critical evidence that the proposed dual‐functional artificial peroxidases can induce a strong antitumor immune response and immune memory but also offers essential guidance for creating a high‐performance and biocompatible strategy to regulate the immunosuppression TME and enhance the antitumor immune responses of breast cancer.