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Periosteal matrix-derived hydrogel promotes bone repair through an early immune regulation coupled with enhanced angio- and osteogenesis

机译:通过与增强的血管和成骨和骨质发生的早期免疫调节,骨膜基质衍生的水凝胶促进骨修复

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摘要

Bone healing is a complex physiological process initiated by early regulation of the inflammatory immunity and entails multiple events including angiogenesis, osteogenic differentiation, and biomineralization. Here, we fabricated an injectable periosteal extracellular matrix (PEM) hydrogel that dynamically integrates multiple biological functions and, therefore, acts at different stages of the fracture healing process. PEM hydrogels were fully characterized compared with a collagen I hydrogel. The effects of PEM hydrogels on the different phases of the healing process were assessed in vitro. PEM hydrogels induced the recruitment and M2-polarization of macrophages, promoted the differentiation of MSCs into endothelial-like cells, HUVEC tube formation, osteogenic differentiation of primary calvarial osteoblasts and MSCs, and mineralization after being immersed in simulated body fluid. The dynamic and multiphase effects of the hydrogels were evaluated using a rat critical-sized calvarial defect model in vivo. During the early phase of repair, PEM hydrogels facilitated the M1-to-M2 transition of macrophages. As bone repair progressed, PEM hydrogels promoted blood vessel migration, the development of relative larger blood vessels, and functional vascularization. These effects were also verified in a subcutaneous embedding model. Eventually, PEM hydrogels promoted mature bone formation in large bone defects to a greater extent than collagen I hydrogels. These biological effects coordinated well with the natural process of bone regeneration. Thus, PEM hydrogels may serve as promising biomaterials in bone tissue engineering.
机译:骨愈合是一种复杂的生理过程,其早期调节炎症免疫引起,并且需要多种事件,包括血管生成,骨质发生分化和生物矿化。在这里,我们制造了一种可注射的骨膜细胞外基质(PEM)水凝胶,其动态整合多种生物学功能,因此,在裂缝愈合过程的不同阶段上作用。与胶原I水凝胶相比,PEM水凝胶完全表征。在体外评估PEM水凝胶对愈合过程不同阶段的影响。 PEM水凝胶诱导巨噬细胞的募集和M2偏振,促进MSCs的分化为内皮样细胞,Huvec管形成,初级颅骨成骨细胞和MSC的成骨分化,以及浸入模拟体液中后的矿化。使用体内大鼠临界大小的颅骨缺陷模型评估水凝胶的动态和多相效应。在早期的修复期间,PEM水凝胶促进了巨噬细胞的M1-TO-M2转变。由于骨修复进展,PEM水凝胶促进了血管迁移,相对较大血管的发育,以及功能性血管化。在皮下嵌入模型中也验证了这些效果。最终,PEM水凝胶在大的骨缺陷中促进成熟的骨形成,而不是胶原蛋白I水凝胶。这些生物学效应与骨再生的自然过程很好。因此,PEM水凝胶可以作为骨组织工程中的有前途的生物材料。

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