首页> 外文期刊>Journal of biomedical materials research, Part A >Primary human osteoblast culture on 3D porous collagen-hydroxyapatite scaffolds
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Primary human osteoblast culture on 3D porous collagen-hydroxyapatite scaffolds

机译:在3D多孔胶原蛋白-羟基磷灰石支架上进行原代人成骨细胞培养

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There is a need in tissue-engineering for 3D scaffolds that mimic the natural extracellular matrix of bone to enhance cell adhesion, proliferation, and differentiation. The scaffold is also required to be degradable. A highly porous scaffold has been developed to incorporate two of the extracellular components found in bone - collagen and hydroxyapatite (HA). The scaffold's collagen component is an afibrillar monomeric type I atelocollagen extracted from foetal calf's skin. This provided a novel environment for the inclusion of HA powder. Five hundred thousand primary human osteoblasts were seeded onto 4 mm cubed scaffolds that varied in ratio of HA to collagen. Weight ratios of 1:99, 25:75, 50:50, and 75:25 hydroxyapatite:collagen (HA:Collagen) were analysed. The scaffolds plus cells were cultured for 21 days. DNA assays and live/dead viability staining demonstrated that all of the scaffolds supported cell proliferation and viability. An alkaline phosphatase assay showed similar osteoblast phenotype maintenance on all of the 3D scaffolds analysed at 21 days. MicroCT analysis demonstrated an increase in total sample volume (correlating to increase in unmineralised matrix production). An even distribution of HA throughout the collagen matrix was observed using this technique. Also at 3 weeks, reductions in the percentage of the mineralised phase of the constructs were seen. These results indicate that each of the ratios of HA/collagen scaffolds have great potential for bone tissue engineering.
机译:在组织工程中需要模仿骨骼的天然细胞外基质以增强细胞粘附,增殖和分化的3D支架。支架也必须是可降解的。已经开发出一种高度多孔的支架,以结合骨骼中发现的两种细胞外成分-胶原蛋白和羟磷灰石(HA)。支架的胶原蛋白成分是从胎牛皮肤中提取的小纤维单体I型端粒胶原蛋白。这提供了包含HA粉末的新环境。将五十万个原代人类成骨细胞接种到4 mm的立方体支架上,这些支架的HA与胶原蛋白的比例有所不同。分析了羟基磷灰石:胶原蛋白(HA:胶原蛋白)的重量比为1:99、25:75、50:50和75:25。将支架加细胞培养21天。 DNA分析和活/死活力染色表明,所有支架均支持细胞增殖和活力。碱性磷酸酶测定显示在21天分析的所有3D支架上,成骨细胞表型维持相似。 MicroCT分析表明总样品量增加(与未矿化基质产量增加相关)。使用该技术观察到HA在整个胶原蛋白基质中均匀分布。同样在3周时,观察到构造物矿化相的百分比降低。这些结果表明,HA /胶原蛋白支架的每个比例在骨组织工程中具有巨大的潜力。

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