MXene and Near‐Infrared Carbon Dots Co‐Encapsulated Hydrogel Facilitates Infected Bone Defect Reconstruction

自愈水凝胶 材料科学 生物医学工程 脚手架 生物膜 骨愈合 体内 生物材料 纳米技术 细菌 医学 外科 高分子化学 生物 生物技术 遗传学
作者
Longfei Xiao,Yang Wang,Jinming Cai,Jinyan Hu,Hongjing Dou,Yu Zhu,Bijiang Geng,Dengyu Pan,Longxiang Shen
出处
期刊:Advanced Healthcare Materials [Wiley]
标识
DOI:10.1002/adhm.202500248
摘要

Inadequate bone differentiation and intractable biofilm formation due to stubborn bacterial infection complicate infected bone defect repair. Adding harmful antibiotics into scaffolds not only promotes multidrug-resistant bacteria but also decreases bone repair effect. Furthermore, dynamic monitor of scaffolds' degradation is crucial for achieving visualized bone defect repair, however, currently reported biomaterials do not have imaging tracing capabilities. On this basis, this work develops a scaffold material with triple functionality for visualized therapy of infected bone defects: antibacterial, osteogenesis, and near-infrared (NIR) imaging capabilities. Single-layer Ti3C2Tx with broad-spectrumantibacterial activity and negatively charged carbon dots (CDs) with osteogenic activity are synthesized for infected bone defect repair. To validate antibacterial and osteogenic activities in vivo, 3D injectable hydrogels encapsulated with Ti3C2Tx and CDs (CD/Ti3C2Tx/GelMA) are constructed. NIR imaging is used to monitor the degradation process of CD/Ti3C2Tx/GelMA hydrogels in infected bone defect models, which indicated that CDs are completely released from hydrogels in about 30 days. Owing to the continuous release of Ti3C2Tx and CDs, the obtained CD/Ti3C2Tx/GelMA hydrogels can efficiently promote the repair of infected bone defects within 60 days. These findings develop a new biomaterial with great performance for visualized antibacterial and osteogenic therapy of infected bone defects.
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