Employing Piezoelectric Mg2+‐Doped Hydroxyapatite to Target Death Receptor‐Mediated Necroptosis: A Strategy for Amplifying Immune Activation

Author:

Yang Jiani12,Du Yaqian3,Yao Yuanfei12,Liao Yuanyu12,Wang Bojun12,Yu Xuefan12,Yuan Kaikun4,Zhang Yanqiao12,He Fei3,Yang Piaoping3ORCID

Affiliation:

1. Department of Gastrointestinal Medical Oncology Harbin Medical University Cancer Hospital Harbin 150001 P. R. China

2. Key Laboratory of Tumor Immunology in Heilongjiang Harbin Medical University Cancer Hospital Harbin 150080 China

3. Key Laboratory of Superlight Materials and Surface Technology Ministry of Education College of Materials Science and Chemical Engineering Harbin Engineering University Harbin 150001 P. R. China

4. Department of Neurosurgery First Affiliated Hospital of Harbin Medical University Harbin 150001 P. R. China

Abstract

AbstractAlthough immunogenic cell death (ICD) inducers evidently enhance the effectiveness of immunotherapy, their potential is increasingly restricted by the development of apoptosis resistance in tumor cells, poor immunogenicity, and low T‐cell immune responsiveness. In this study, for the first time, piezoelectrically catalyzed Mg2+‐doped hydroxyapatite (Mg‐HAP) nanoparticles, which are coated with a mesoporous silica layer and loaded with ONC201 as an agonist to specifically target the death receptor DR5 on tumor cells, ultimately developing an Mg‐HAP@MS/ONC201 nanoparticle (MHMO NP) system, are engineered. Owing to its excellent piezoelectric properties, MHMO facilitates the release of a significant amount of reactive oxygen species and Ca2+ within tumor cells, effectively promoting the upregulation of DR5 expression and inducing tumor cell necroptosis to ultimately overcome apoptosis resistance. Concurrently, Mg2+ released in the tumor microenvironment promotes CD8+ T receptor activation in response to the antitumor immune reaction induced by ICD. Using RNA‐seq analysis, it is elucidated that MHMO can activate the NF‐κB pathway under piezoelectric catalysis, thus inducing M1‐type macrophage polarization. In summary, a dual‐targeting therapy system that targets both tumor cells and the tumor microenvironment under piezoelectric catalysis is designed. This system holds substantial potential for advancements in tumor immunotherapy.

Funder

Natural Science Foundation of Heilongjiang Province

Natural Science Foundation of Shandong Province

National Natural Science Foundation of China

Publisher

Wiley

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