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首页> 外文期刊>Tissue engineering, Part A >Biomimetic Engineering of Nanofibrous Gelatin Scaffolds with Noncollagenous Proteins for Enhanced Bone Regeneration
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Biomimetic Engineering of Nanofibrous Gelatin Scaffolds with Noncollagenous Proteins for Enhanced Bone Regeneration

机译:纳米纤维明胶支架具有非可粘连蛋白增强骨再生的仿生工程

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摘要

Biomimetic approaches are widely used in scaffolding designs to enhance tissue regeneration. In this study, we integrated noncollagenous proteins (NCPs) from bone extracellular matrix (ECM) with three-dimensional nanofibrous gelatin (NF-Gelatin) scaffolds to form an artificial matrix (NF-Gelatin-NCPs) mimicking both the nano-structured architecture and chemical composition of natural bone ECM. Through a chemical coupling process, the NCPs were evenly distributed over all the surfaces (inner and outer) of the NF-gelatin-NCPs. The in vitro study showed that the number of osteoblasts (MC3T3-E1) on the NF-Gelatin-NCPs was significantly higher than that on the NF-Gelatin after being cultured for 14 days. Both the alkaline phosphatase (ALP) activity and the expression of osteogenic genes (OPN, BSP, DMP1, CON, and Runx2) were significantly higher in the NF-Gelatin-NCPs than in the NF-Gelatin at 3 weeks. Von Kossa staining, backscattered scanning electron microscopy, and microcomputed tomography all revealed a higher amount of mineral deposition in the NF-Gelatin-NCPs than in the NF-Gelatin after in vitro culturing for 3 weeks. The in vivo calvarial defect study indicated that the NF-Gelatin-NCPs recruited more host cells to the defect and regenerated a higher amount of bone than the controls after implantation for 6 weeks. Immunohistochemical staining also showed high-level mineralization of the bone matrix in the NF-Gelatin-NCPs. Taken together, both the in vitro and in vivo results confirmed that the incorporation of NCPs onto the surfaces of the NF-Gelatin scaffold significantly enhanced osteogenesis and mineralization. Biomimetic engineering of the surfaces of the NF-Gelatin scaffold with NCPs, therefore, is a promising strategy to enhance bone regeneration.
机译:仿生方法广泛用于脚手架设计以增强组织再生。在本研究中,我们用三维纳米纤维(ECM)与三维纳米纤维(NF-明胶)支架中的非胶囊蛋白(ECM)集成了非胶囊蛋白(ECM),以形成模仿纳米结构架构的人工基质(NF-明胶-NCP)和天然骨ECM的化学成分。通过化学偶联方法,NCP均匀地分布在NF-明胶-NCP的所有表面(内部和外部)上。体外研究表明,在培养14天后,NF-明胶-NCPS上的骨赘(MC3T3-E1)的数量显着高于NF-明胶上。碱性磷酸酶(ALP)活性和成骨基因(OPN,BSP,DMP1,CON和RONX2)的表达在NF-明胶-NCP中显着高于NF-明胶3周。 von Kossa染色,背散射扫描电子显微镜,微仿性断层扫描均显示出在NF-明胶-NCP中的矿物沉积量高于在体外培养3周后在NF-明胶中的矿物沉积。体内颅骨缺陷研究表明,NF-明胶-NCP募集到缺陷的宿主细胞更多,并在植入后再生骨量较高6周。免疫组织化学染色也显示出NF-明胶-NCPS中的骨基质的高水平矿化。一起携带,体外和体内结果证实,将NCP掺入NF-明胶支架的表面上显着增强了成骨和矿化。因此,NC-Gelatin支架的仿生工程为NCPS,因此是提高骨再生的有希望的策略。

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