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PdZn/Co<sub>SA</sub>‐NC Nanozymes with Highly Efficient SOD/CAT Activities for Treatment of Osteoarthritis via Regulating Immune Microenvironment

Xin Yang, Manli Tan, Jianfeng Guo, Jianhui Xiang, Feiying Yin, Jiejia Deng, Ji Luo, Shihui Xiao, Miao Mo, Hanjie Wang, Jinmin Zhao, Li Zheng, Jian‐Wen Cheng, Jingping Zhong

2024Advanced Functional Materials57 citationsDOIOpen Access PDF

Abstract

Abstract Inflammatory infiltration of synovial M1 macrophages, high levels of ROS, and NO exacerbate osteoarthritis (OA) progression. The PdZn/Co SA ‐NC nanozymes, which are highly ordered PdZn intermetallic nanoparticles loaded with Co single atom N‐doped carbon‐rich in multi‐level pores, in an attempt to serve as SOD and CAT mimicking nanozymes for OA therapy is designed. The PdZn/Co SA ‐NC nanozymes' high electron transfer and dual active site sufficient exposure enhances free radical adsorption and lower reaction energies, accelerating SOD‐like, CAT‐like, and GPx‐like catalyzed reactions, outperforming Co SA ‐NC and PdZn/NC alone. Furthermore, PdZn/Co SA ‐NC nanozymes exhibit favorable biocompatibility, reduce synovial macrophage oxidative stress in OA, alleviate hypoxia, restore mitochondrial function, regulate energy metabolism, increase antioxidant factors, and reduce inflammatory factors, thus effectively mitigating the progression of OA. Mechanistically, PdZn/Co SA ‐NC nanozymes downregulate M1‐type phenotypic markers like IL‐1β by regulating purine metabolism. The PdZn/Co SA ‐NC nanozymes offer a novel approach to treating oxidative stress‐related inflammatory diseases.

Topics & Concepts

Materials scienceOsteoarthritisImmune systemNanotechnologyBiologyMedicineImmunologyPathologyAlternative medicineAdvanced Nanomaterials in CatalysisNanoplatforms for cancer theranosticsExtracellular vesicles in disease