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骨骼组织修复的评估,第2部分:通过在体外鸡股骨缺损模型中释放双生长因子的水凝胶增强骨骼组织修复

Evaluation of skeletal tissue repair, part 2: enhancement of skeletal tissue repair through dual-growth-factor-releasing hydrogels within an ex vivo chick femur defect model.

作者信息

Smith E L, Kanczler J M, Gothard D, Roberts C A, Wells J A, White L J, Qutachi O, Sawkins M J, Peto H, Rashidi H, Rojo L, Stevens M M, El Haj A J, Rose F R A J, Shakesheff K M, Oreffo R O C

机构信息

Bone & Joint Research Group, Human Development and Health, Institute of Developmental Sciences, University of Southampton, Southampton, UK.

Bone & Joint Research Group, Human Development and Health, Institute of Developmental Sciences, University of Southampton, Southampton, UK.

出版信息

Acta Biomater. 2014 Oct;10(10):4197-205. doi: 10.1016/j.actbio.2014.05.025. Epub 2014 Jun 4.

Abstract

There is an unmet need for improved, effective tissue engineering strategies to replace or repair bone damaged through disease or injury. Recent research has focused on developing biomaterial scaffolds capable of spatially and temporally releasing combinations of bioactive growth factors, rather than individual molecules, to recapitulate repair pathways present in vivo. We have developed an ex vivo embryonic chick femur critical size defect model and applied the model in the study of novel extracellular matrix (ECM) hydrogel scaffolds containing spatio-temporal combinatorial growth factor-releasing microparticles and skeletal stem cells for bone regeneration. Alginate/bovine bone ECM (bECM) hydrogels combined with poly(d,l-lactic-co-glycolic acid) (PDLLGA)/triblock copolymer (10-30% PDLLGA-PEG-PLDLGA) microparticles releasing dual combinations of vascular endothelial growth factor (VEGF), chondrogenic transforming growth factor beta 3 (TGF-β3) and the bone morphogenetic protein BMP2, with human adult Stro-1+bone marrow stromal cells (HBMSCs), were placed into 2mm central segmental defects in embryonic day 11 chick femurs and organotypically cultured. Hydrogels loaded with VEGF combinations induced host cell migration and type I collagen deposition. Combinations of TGF-β3/BMP2, particularly with Stro-1+HBMSCs, induced significant formation of structured bone matrix, evidenced by increased Sirius red-stained matrix together with collagen expression demonstrating birefringent alignment within hydrogels. This study demonstrates the successful use of the chick femur organotypic culture system as a high-throughput test model for scaffold/cell/growth factor therapies in regenerative medicine. Temporal release of dual growth factors, combined with enriched Stro-1+HBMSCs, improved the formation of a highly structured bone matrix compared to single release modalities. These studies highlight the potential of a unique alginate/bECM hydrogel dual growth factor release platform for bone repair.

摘要

对于改进的、有效的组织工程策略以替代或修复因疾病或损伤而受损的骨骼,存在未满足的需求。最近的研究集中在开发能够在空间和时间上释放生物活性生长因子组合而非单个分子的生物材料支架,以重现体内存在的修复途径。我们开发了一种体外鸡胚股骨临界尺寸缺损模型,并将该模型应用于研究新型细胞外基质(ECM)水凝胶支架,该支架含有时空组合生长因子释放微粒和用于骨再生的骨骼干细胞。藻酸盐/牛骨ECM(bECM)水凝胶与聚(d,l-乳酸-共-乙醇酸)(PDLLGA)/三嵌段共聚物(10-30% PDLLGA-PEG-PLDLGA)微粒结合,释放血管内皮生长因子(VEGF)、软骨生成转化生长因子β3(TGF-β3)和骨形态发生蛋白BMP2的双重组合,并与人成年Stro-1+骨髓基质细胞(HBMSCs)一起,植入胚胎第11天鸡胚股骨的2mm中央节段性缺损处,并进行器官型培养。负载VEGF组合的水凝胶诱导宿主细胞迁移和I型胶原沉积。TGF-β3/BMP2的组合,特别是与Stro-1+HBMSCs一起,诱导了结构化骨基质的显著形成,这通过天狼星红染色基质增加以及胶原表达证明水凝胶内双折射排列得以证实。本研究证明了鸡胚股骨器官型培养系统作为再生医学中支架/细胞/生长因子疗法的高通量测试模型的成功应用。与单一释放方式相比,双重生长因子的时间释放与富集的Stro-1+HBMSCs相结合,改善了高度结构化骨基质的形成。这些研究突出了独特的藻酸盐/bECM水凝胶双重生长因子释放平台在骨修复方面的潜力。

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