Dynamic multistage nanozyme hydrogel reprograms diabetic wound microenvironment: synergistic oxidative stress alleviation and mitochondrial restoration

氧化应激 氧化磷酸化 细胞生物学 活性氧 线粒体 化学 氧化损伤 生物 生物化学
作者
Jingyu Yan,Yifan Zhao,Chenying Cui,Lihong Zhou,Yurong Xu,Ziyang Bai,Kaifang Zhang,Jiahui Tong,Yingyu Liu,Lingxiang Sun,Meijun Du,Yanling Mi,Xing Wang,Xiuping Wu,Bing Li
出处
期刊:Materials today bio [Elsevier BV]
卷期号:32: 101780-101780 被引量:2
标识
DOI:10.1016/j.mtbio.2025.101780
摘要

Chronic diabetic wounds remain a significant clinical challenge due to persistent bacterial infections, oxidative stress, impaired angiogenesis, and mitochondrial dysfunction. Traditional therapies often fail to address these interrelated pathological factors, highlighting the urgent need for innovative solutions. Here, we present a Mn-ZIF@GOx/BC (MZGB) hydrogel system, where Mn-ZIF@GOx (MZG) nanozymes are successfully integrated into a bacterial cellulose (BC) hydrogel via hydrogen bonding and electrostatic interactions. The MZGB hydrogel lowers wound pH by oxidizing excess glucose into gluconic acid. It exhibits strong ROS scavenging capabilities through its superoxide dismutase and catalase-like activities, while simultaneously providing oxygen. By restoring redox homeostasis, it protects mitochondrial function and enhances cellular energy metabolism. By reprogramming macrophages, MZGB creates a favorable immune microenvironment, significantly promoting angiogenesis through paracrine mechanisms. This facilitates cell-to-cell communication, forming a positive feedback loop. Moreover, MZGB demonstrates ROS-independent antibacterial properties. BC hydrogel ensures adhesion and moisture regulation, forming a protective barrier and maintaining an optimal wound environment. This multifunctional hydrogel represents a promising nanotherapeutic approach for efficiently treating diabetic wounds by precisely regulating the wound microenvironment.
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