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首页> 外文期刊>Bone >Surface modification with fibrin/hyaluronic acid hydrogel on solid-free form-based scaffolds followed by BMP-2 loading to enhance bone regeneration.
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Surface modification with fibrin/hyaluronic acid hydrogel on solid-free form-based scaffolds followed by BMP-2 loading to enhance bone regeneration.

机译:在无固体形式的支架上用纤维蛋白/透明质酸水凝胶进行表面修饰,然后加载BMP-2以增强骨骼再生。

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摘要

Bone tissue engineering often requires a well-defined scaffold that is highly porous. The multi-head deposition system (MHDS), a form of solid freeform fabrication, has raised great interest as a method for fabricating scaffolds, since it yields a highly porous inter-connective structure without the use of cytotoxic solvents, and permits the diffusion of nutrients and oxygen. However, this method is not suitable for introducing proteins, as it includes a heating process. Hydrogels incorporated with protein coating of the scaffold surface could overcome this MHDS limitation. In the present study, the surface of a scaffold fabricated using MHDS was coated with a mixture of fibrin and hyaluronic acid (HA) and used as a vehicle for delivery of both bone morphogenetic protein-2 (BMP-2) and adipose-derived stromal cells (ASCs). Fibrin/HA coating of the scaffold significantly enhanced initial cell attachment. Furthermore, the in vitro release of BMP-2 from fibrin/HA-coated scaffolds was sustained for 3 days and it stimulated the alkaline phosphatase activity of ASCs seeded on the scaffold for 10 days more actively and continuously than did the soluble BMP-2 that was added to the culture media, not the scaffold itself. Importantly, the transplantation of undifferentiated ASCs inoculated on BMP-2-loaded, fibrin/HA-coated scaffolds resulted in more improved bone formation and mineralization than did the transplantation of undifferentiated ASCs seeded on uncoated scaffolds or on fibrin/HA-coated scaffolds without BMP-2, but containing BMP-2 in the cell suspension medium. These results show that BMP-2-loaded, fibrin/HA-coated scaffolds fabricated using MHDS may be useful in stimulating bone regeneration from undifferentiated ASCs in vivo.
机译:骨组织工程通常需要定义明确的,高度多孔的支架。多头沉积系统(MHDS)是一种固体自由形式的制造形式,作为一种制造脚手架的方法引起了人们极大的兴趣,因为它无需使用细胞毒性溶剂即可产生高度多孔的互连结构,并且可以扩散营养和氧气。但是,该方法不适合引入蛋白质,因为它包括加热过程。结合了支架表面蛋白质涂层的水凝胶可以克服MHDS的局限性。在本研究中,使用MHDS制造的支架表面涂有纤维蛋白和透明质酸(HA)的混合物,并用作递送骨形态发生蛋白2(BMP-2)和脂肪来源的基质的载体单元(ASC)。支架的纤维蛋白/ HA涂层显着增强了初始细胞附着。此外,BMP-2从纤维蛋白/ HA包被的支架中的体外释放持续了3天,与可溶性BMP-2相比,BMP-2的活性和连续性更能连续地刺激接种在支架上的ASC的碱性磷酸酶活性10天。被添加到文化媒体,而不是脚手架本身。重要的是,与未分化的ASCs移植在未涂覆BMP-2的,未涂覆BMP的纤维蛋白/ HA涂覆的支架上或未涂覆BMP-2的未分化的ASCs相比,未分化的ASCs移植导致的骨形成和矿化程度更高。 -2,但在细胞悬浮液中含有BMP-2。这些结果表明,使用MHDS制备的BMP-2负载的纤维蛋白/ HA涂层支架可用于刺激体内未分化ASC的骨再生。

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