透明质酸
活性氧
伤口愈合
明胶
细胞外基质
材料科学
自愈水凝胶
苯硼酸
血管生成
氧气
化学
共价键
体内
巨噬细胞
生物物理学
再生(生物学)
生物医学工程
基质(化学分析)
右旋糖酐
纳米技术
导电体
谷胱甘肽
氧化磷酸化
细胞迁移
过氧化物
细胞外
作者
Huiyuan Zheng,Huan Xin,Futai Du,Yue Wang,Yutong Ma,Sen-Peng Li,Wentao Sun,Bo Li,Qingming Ma
标识
DOI:10.1021/acsami.6c06897
摘要
Complex wounds remain a clinical challenge due to their multifaceted pathophysiology, which involves persistent inflammation, oxidative stress, tissue hypoxia, and impaired angiogenesis. To address these issues, we developed an injectable, self-healing, and conductive hydrogel based on a dual dynamic covalent network formed by cross-linking phenylboronic acid-modified oxidized hyaluronic acid (OHA-PBA) and dopamine-grafted gelatin (GelDA). This network mimics the native extracellular matrix with its capacity for hydration regulation and cell adhesion, in addition to responding to the acidic and highly reactive oxygen species (ROS) wound microenvironment to enable intelligent drug release. By incorporating honeycomb-like manganese dioxide nanozymes (PHMP NPs) preloaded with puerarin (PUE) and conductive black phosphorus nanosheets (BP Ns), the hydrogel achieves sustained oxygen generation, ROS and reactive nitrogen species scavenging, electrical conductivity, and pro-angiogenic activity. In vivo experiments confirmed that the hydrogel significantly accelerates wound closure through multitarget mechanisms: downregulating pro-inflammatory factors (TNF-α, IL-6), promoting M2 macrophage polarization, and enhancing VEGF-mediated vascularization. This integrated strategy provides a comprehensive and translatable solution for advanced wound management.
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