Multifunctional Bioactive Nanozyme Systems for Enhanced Diabetic Wound Healing

Author:

Gao Suyue12,He Xuefeng12,Liu Hengdeng12,Liu Yiling12,Wang Hanwen12,Zhou Ziheng12,Chen Lei12,Ji Xiaoyuan3ORCID,Yang Ronghua4,Xie Julin12

Affiliation:

1. Department of Burns The First Affiliated Hospital of Sun Yat‐Sen University Guangzhou Guangdong 510080 China

2. Institute of Precision Medicine The First Affiliated Hospital Sun Yat‐Sen University Guangzhou Guangdong 510080 China

3. Academy of Medical Engineering and Translational Medicine Medical College Tianjin University Tianjin 300072 China

4. Department of Burn and Plastic Surgery Guangzhou First People's Hospital South China University of Technology Guangzhou Guangdong 510180 China

Abstract

AbstractThe protracted transition from inflammation to proliferation in diabetic wound healing poses significant challenges, exacerbated by persistent inflammatory responses and inadequate vascularization. To address these issues, a novel nanozymatic therapeutic approach utilizing asymmetrically structured MnO₂–Au–mSiO₂@aFGF Janus nanoparticles is engineered. Nanozymes featuring a mSiO₂ head and MnO₂ extensions, into which acidic fibroblast growth factor (aFGF) is encapsulated, resulting in MnO₂–Au–mSiO₂@aFGF Janus nanoparticles (mSAM@aFGF), are synthesized. This nanozyme system effectively emulates enzymatic activities of catalase (CAT) and superoxide dismutase (SOD), catalyzing degradation of reactive oxygen species (ROS) and generating oxygen. In addition, controlled release of aFGF fosters tissue regeneration and vascularization. In vitro studies demonstrate that mSAM@aFGF significantly alleviates oxidative stress in cells, and enhances cell proliferation, migration, and angiogenesis. An injectable hydrogel based on photocrosslinked hyaluronic acid (HAMA), incorporating the nanozymatic ROS‐scavenging and growth factor‐releasing system, is developed. The HAMA‐mSAM@aFGF hydrogel exhibits multifaceted benefits in a diabetic wound model, including injectability, wound adhesion, hemostasis, anti‐inflammatory effects, macrophage polarization from M1 to M2 phenotype, and promotion of vascularization. These attributes underscore the potential of this system to facilitate transition from chronic inflammation to the proliferative phase of wound repair, offering a promising therapeutic strategy for diabetic wound management.

Funder

National Natural Science Foundation of China

Publisher

Wiley

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