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用于血管生成和骨再生的载血管内皮生长因子支架与生物活性玻璃的涂层

Coating of VEGF-releasing scaffolds with bioactive glass for angiogenesis and bone regeneration.

作者信息

Leach J Kent, Kaigler Darnell, Wang Zhuo, Krebsbach Paul H, Mooney David J

机构信息

Division of Engineering and Applied Sciences, Harvard University, Cambridge, MA 02138, USA.

出版信息

Biomaterials. 2006 Jun;27(17):3249-55. doi: 10.1016/j.biomaterials.2006.01.033. Epub 2006 Feb 21.

Abstract

Bioactive glasses are potentially useful as bone defect fillers, and vascular endothelial growth factor (VEGF) has demonstrated benefit in bone regeneration as well. We hypothesized that the specific combination of prolonged localized VEGF presentation from a matrix coated with a bioactive glass may enhance bone regeneration. To test this hypothesis, the capacity of VEGF-releasing polymeric scaffolds with a bioactive glass coating was examined in vitro and in vivo using a rat critical-sized defect model. In the presence of a bioactive glass coating, we did not detect pronounced differences in the differentiation of human mesenchymal stem cells in vitro. However, we observed significantly enhanced mitogenic stimulation of endothelial cells in the presence of the bioactive glass coating, with an additive effect with VEGF release. This trend was maintained in vivo, where coated VEGF-releasing scaffolds demonstrated significant improvements in blood vessel density at 2 weeks versus coated control scaffolds. At 12 weeks, bone mineral density was significantly increased in coated VEGF-releasing scaffolds versus coated controls, while only a slight increase in bone volume fraction was observed. The results of this study suggest that a bioactive glass coating on a polymeric substrate participates in bone healing through indirect processes which enhance angiogenesis and bone maturation and not directly on osteoprogenitor differentiation and bone formation. The mass of bioactive glass used in this study provides a comparable and potentially additive, response to localized VEGF delivery over early time points. These studies demonstrate a materials approach to achieve an angiogenic response formerly limited to the delivery of inductive growth factors.

摘要

生物活性玻璃作为骨缺损填充材料具有潜在的应用价值,血管内皮生长因子(VEGF)在骨再生方面也已显示出益处。我们推测,由生物活性玻璃涂层基质实现的VEGF长时间局部递送的特定组合可能会增强骨再生。为了验证这一假设,我们使用大鼠临界尺寸骨缺损模型在体外和体内检测了具有生物活性玻璃涂层的VEGF释放聚合物支架的性能。在存在生物活性玻璃涂层的情况下,我们在体外未检测到人间充质干细胞分化的明显差异。然而,我们观察到在存在生物活性玻璃涂层的情况下,内皮细胞的促有丝分裂刺激显著增强,与VEGF释放具有相加效应。这种趋势在体内得以维持,与未涂层的对照支架相比,涂有VEGF释放支架在2周时血管密度有显著改善。在12周时,与未涂层的对照相比,涂有VEGF释放支架的骨矿物质密度显著增加,而骨体积分数仅略有增加。本研究结果表明,聚合物基质上的生物活性玻璃涂层通过增强血管生成和骨成熟的间接过程参与骨愈合,而不是直接作用于骨祖细胞分化和骨形成。本研究中使用的生物活性玻璃质量在早期时间点对局部VEGF递送提供了相当且可能具有相加性的反应。这些研究展示了一种材料方法,可实现以前仅限于递送诱导性生长因子的血管生成反应。

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