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首页> 外文期刊>Theranostics >Biomimetic open porous structured core-shell microtissue with enhanced mechanical properties for bottom-up bone tissue engineering
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Biomimetic open porous structured core-shell microtissue with enhanced mechanical properties for bottom-up bone tissue engineering

机译:具有增强的机械性能的仿生开放式多孔结构核壳微组织,用于自下而上的骨组织工程

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Background : Microtissues constructed with hydrogels promote cell expansion and specific differentiation by mimicking the microarchitecture of native tissues. However, the suboptimal mechanical property and osteogenic activity of microtissues fabricated by natural polymers need further improvement for bone reconstruction application. Core-shell designed structures are composed of an inner core part and an outer part shell, combining the characteristics of different materials, which improve the mechanical property of microtissues. Methods : A micro-stencil array chip was used to fabricate an open porous core-shell micro-scaffold consisting of gelatin as shell and demineralized bone matrix particles modified with bone morphogenetic protein-2 (BMP-2) as core. Single gelatin micro-scaffold was fabricated as a control. Rat bone marrow mesenchymal stem cells (BMSCs) were seeded on the micro-scaffolds, after which they were dynamic cultured and osteo-induced in mini-capsule bioreactors to fabricate microtissues. The physical characteristics, biocompatibility, osteo-inducing and controlled release ability of the core-shell microtissue were evaluated in vitro respectively. Then microtissues were tested in vivo via ectopic implantation and orthotopic bone implantation in rat model. Results : The Young's modulus of core-shell micro-scaffold was nearly triple that of gelatin micro-scaffold, which means the core-shell micro-scaffolds have better mechanical property. BMSCs rapidly proliferated and retained the highest viability on core-shell microtissues. The improved osteogenic potential of core-shell microtissues was evidenced by the increased calcification based on von kossa staining and osteo-relative gene expression. At 3months after transplantation, core-shell microtissue group formed the highest number of mineralized tissues in rat ectopic subcutaneous model, and displayed the largest amount of new bony tissue deposition in rat orthotopic cranial defect. Conclusion : The novel core-shell microtissue construction strategy developed may become a promising cell delivery platform for bone regeneration.
机译:背景:用水凝胶构建的微组织通过模仿天然组织的微结构来促进细胞扩增和特异性分化。然而,由天然聚合物制造的微组织的次优机械性能和成骨活性需要进一步改善,以用于骨重建应用。核-壳设计的结构由内部的核部分和外部的壳组成,结合了不同材料的特性,从而改善了微组织的机械性能。方法:采用微模板阵列芯片制备以明胶为壳,以骨形态发生蛋白2(BMP-2)为核心修饰的去矿质骨基质颗粒组成的开放式多孔核-壳微支架。制备单个明胶微支架作为对照。将大鼠骨髓间充质干细胞(BMSCs)接种在微支架上,然后对其进行动态培养并在微型胶囊生物反应器中进行骨诱导以制备微组织。分别评估了核壳微组织的物理特性,生物相容性,骨诱导性和控释能力。然后通过异位植入和原位骨植入在大鼠模型中体内测试微组织。结果:核-壳微支架的杨氏模量几乎是明胶微支架的杨氏模量的三倍,这意味着核-壳微支架具有更好的机械性能。骨髓间充质干细胞迅速增殖,并在核壳微组织上保持最高的生存能力。基于von kossa染色和骨相关基因表达的钙化增加证明了核壳微组织的成骨潜力得到改善。移植后3个月,核壳微组织组在大鼠异位皮下模型中形成了最多的矿化组织,并在大鼠原位颅骨缺损中显示出最大量的新骨组织沉积。结论:开发的新型核-壳微组织构建策略可能成为有希望的骨再生细胞递送平台。

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