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负载两亲性结构纳米胶束的ROS/pH双响应水凝胶敷料用于感染伤口修复

ROS/pH Dual-Responsive Hydrogel Dressings Loaded with Amphiphilic Structured Nano Micelles for the Repair of Infected Wounds.

作者信息

Wang Jun, Lin Yanxia, Fan Huijing, Cui Jianfeng, Wang Yuanxiang, Wang Zilan

机构信息

The Department of Rehabilitation Medicine, Shenzhen Qianhai Shekou Free Trade Zone Hospital, Shenzhen, 518067, People's Republic of China.

Guangzhou Myers Biotechnology Co., Ltd, Guangzhou, 510660, People's Republic of China.

出版信息

Int J Nanomedicine. 2025 Jun 23;20:8119-8142. doi: 10.2147/IJN.S522589. eCollection 2025.

Abstract

BACKGROUND

Bacterial infections in wounds have emerged as an increasingly significant healthcare concern. The toxins secreted by bacteria cause persistent inflammation and excessive oxidative stress, resulting in serious tissue damage and ultimately delay wound healing.

METHODS

Herein, a ROS/pH dual-responsive hydrogel dressing loaded with amphiphilic structured nano micelles was developed for efficiently promoting infected wound healing. First, chitosan-grafted α-lipoic acid (CSLA) and curcumin (Cur) formed stable amphiphilic nano micelles (CSLA@Cur) through ultrasonic self-assembly. Subsequently, CSLA@Cur was incorporated into a hydrogel formed from 4-carboxyphenylboronic acid-modified gelatin methacrylate (GelMA-CPBA) and oxidized chondroitin sulfate (OCS) via Schiff base formation, boronate ester bonding, and free radical polymerization to obtain GC/OCS-CL@Cur hydrogel dressing. The mechanical properties, antimicrobial, antioxidant, and ROS/pH responsiveness of GC/OCS-CL@Cur were evaluated. Cellular assays were performed to investigate the biocompatibility of GC/OCS-CL@Cur and its role in promoting angiogenesis, scavenging intracellular ROS and regulating macrophage polarization. A full-thickness skin defect rat model with bacterial infection was established to investigate the ability of GC/OCS-CL@Cur to enhance wound repair in vivo.

RESULTS

The unique cross-linked structure of GC/OCS-CL@Cur significantly improves the mechanical properties of hydrogels. Importantly, GC/OCS-CL@Cur exhibited sensitive ROS/pH dual responsiveness, which enabled the controlled release of CSLA@Cur and efficient delivery of Cur. Moreover, GC/OCS-CL@Cur possessed excellent antimicrobial activity and efficient ROS scavenging ability. In vitro cellular assays demonstrated that GC/OCS-CL@Cur could effectively scavenge intracellular ROS (up to 90% scavenging ratio), promote macrophage polarization to M2 phenotype, and enhance angiogenesis. In vivo experiments showed that GC/OCS-CL@Cur significantly regulated the expression level of inflammatory cytokines, and healed more than 95% of wounds in 14 days, showing excellent wound healing ability.

CONCLUSION

These results demonstrate the successful development of a dual-responsive (ROS/pH) hydrogel dressing with integrated antibacterial, antioxidant, and anti-inflammatory properties, showcasing significant potential for treating infected wounds.

摘要

背景

伤口中的细菌感染已成为日益严重的医疗保健问题。细菌分泌的毒素会导致持续的炎症和过度的氧化应激,从而造成严重的组织损伤并最终延迟伤口愈合。

方法

在此,开发了一种负载两亲结构纳米胶束的ROS/pH双响应水凝胶敷料,用于有效促进感染伤口愈合。首先,壳聚糖接枝α-硫辛酸(CSLA)和姜黄素(Cur)通过超声自组装形成稳定的两亲纳米胶束(CSLA@Cur)。随后,通过席夫碱形成、硼酸酯键合和自由基聚合,将CSLA@Cur掺入由4-羧基苯基硼酸改性的甲基丙烯酸明胶(GelMA-CPBA)和氧化硫酸软骨素(OCS)形成的水凝胶中,以获得GC/OCS-CL@Cur水凝胶敷料。评估了GC/OCS-CL@Cur的力学性能、抗菌、抗氧化和ROS/pH响应性。进行细胞试验以研究GC/OCS-CL@Cur的生物相容性及其在促进血管生成、清除细胞内ROS和调节巨噬细胞极化中的作用。建立了细菌感染的全层皮肤缺损大鼠模型,以研究GC/OCS-CL@Cur在体内增强伤口修复的能力。

结果

GC/OCS-CL@Cur独特的交联结构显著改善了水凝胶的力学性能。重要的是,GC/OCS-CL@Cur表现出灵敏的ROS/pH双响应性,这使得CSLA@Cur能够控释并有效递送Cur。此外,GC/OCS-CL@Cur具有优异的抗菌活性和高效的ROS清除能力。体外细胞试验表明,GC/OCS-CL@Cur能够有效清除细胞内ROS(清除率高达90%),促进巨噬细胞极化为M2表型,并增强血管生成。体内实验表明,GC/OCS-CL@Cur显著调节炎症细胞因子的表达水平,在14天内愈合了超过95%的伤口,显示出优异的伤口愈合能力。

结论

这些结果表明成功开发了一种具有综合抗菌、抗氧化和抗炎特性的双响应(ROS/pH)水凝胶敷料,展示了治疗感染伤口的巨大潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bf64/12205371/b937ae695450/IJN-20-8119-g0001.jpg

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