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采用纤维蛋白/透明质酸水凝胶对无定形形态基支架进行表面改性,随后负载 BMP-2 以增强骨再生。

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

机构信息

Department of Biomedical Science, CHA University, Seoul, Republic of Korea.

出版信息

Bone. 2011 Feb;48(2):298-306. doi: 10.1016/j.bone.2010.09.029. Epub 2010 Sep 24.

Abstract

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.

摘要

骨组织工程通常需要具有高度多孔性的明确定义的支架。多喷头沉积系统(MHDS)作为一种无模制造方法,由于其可以在不使用细胞毒性溶剂的情况下产生高度多孔的互联结构,并允许营养物质和氧气扩散,因此作为制造支架的方法引起了极大的兴趣。然而,该方法不适合引入蛋白质,因为它包括加热过程。将蛋白质包被在支架表面的水凝胶可以克服 MHDS 的这一局限性。在本研究中,使用 MHDS 制造的支架的表面涂覆了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)和脂肪源性基质细胞(ASCs)的载体。支架表面的纤维蛋白/HA 涂层显著增强了初始细胞附着。此外,纤维蛋白/HA 涂层支架中 BMP-2 的体外释放持续了 3 天,并且比添加到培养基中的可溶性 BMP-2更积极和持续地刺激接种在支架上的 ASC 的碱性磷酸酶活性,而不是支架本身。重要的是,将接种在负载 BMP-2 的纤维蛋白/HA 涂层支架上的未分化 ASCs 移植到体内,可导致更多的骨形成和矿化改善,而将未分化的 ASCs 移植到未涂层的支架上或未负载 BMP-2 但在细胞悬浮液培养基中含有 BMP-2 的纤维蛋白/HA 涂层支架上的移植效果更好。这些结果表明,使用 MHDS 制造的负载 BMP-2 的纤维蛋白/HA 涂层支架可能有助于刺激体内未分化 ASCs 的骨再生。

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