血管生成
脚手架
细胞生物学
干细胞
透明质酸
化学
细胞外基质
再生(生物学)
生物医学工程
生物
解剖
癌症研究
医学
作者
Gonggong Lu,Yang Xu,Quanying Liu,Wei Ma,Huan Sun,Sheng Wang,Xing Li,Yuxiang Wang,Xiang Li,Xuhui Hui,En Luo,Jun Liu,Qing Jiang,Jie Liang,Yujiang Fan,Yong Sun,Shouxin Zhang
标识
DOI:10.1038/s41467-022-30243-5
摘要
Abstract Limited stem cells, poor stretchability and mismatched interface fusion have plagued the reconstruction of cranial defects by cell-free scaffolds. Here, we designed an instantly fixable and self-adaptive scaffold by dopamine-modified hyaluronic acid chelating Ca 2+ of the microhydroxyapatite surface and bonding type I collagen to highly simulate the natural bony matrix. It presents a good mechanical match and interface integration by appropriate calcium chelation, and responds to external stress by flexible deformation. Meanwhile, the appropriate matrix microenvironment regulates macrophage M2 polarization and recruits endogenous stem cells. This scaffold promotes the proliferation and osteogenic differentiation of BMSCs in vitro, as well as significant ectopic mineralization and angiogenesis. Transcriptome analysis confirmed the upregulation of relevant genes and signalling pathways was associated with M2 macrophage activation, endogenous stem cell recruitment, angiogenesis and osteogenesis. Together, the scaffold realized 97 and 72% bone cover areas after 12 weeks in cranial defect models of rabbit (Φ = 9 mm) and beagle dog (Φ = 15 mm), respectively.
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