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首页> 外文期刊>Tissue engineering, Part A >Heparin-chitosan-coated acellular bone matrix enhances perfusion of blood and vascularization in bone tissue engineering scaffolds.
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Heparin-chitosan-coated acellular bone matrix enhances perfusion of blood and vascularization in bone tissue engineering scaffolds.

机译:肝素-壳聚糖涂层的脱细胞骨基质可增强骨骼组织工程支架中的血液灌注和血管生成。

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摘要

Currently, the main hurdle in the tissue engineering field is how to provide sufficient blood supply to grafted tissue substitutes in the early post-transplanted period. For three-dimensional, cell-dense, thick tissues to survive after transplantation, treatments are required for hypoxia, nutrient insufficiency, and the accumulation of waste products. In this study, a biomacromolecular layer-by-layer coating process of chitosan/heparin onto a decellularized extracellular bone matrix was designed to accelerate the blood perfusion and re-endothelialization process. The results of in vitro measurements of the activated partial thromboplastin time supported the theory that the combination of chitosan and heparin could bring both anticoagulation and hemocompatibility to the scaffold. A rabbit bone defect model was established for further evaluation of the application of this kind of surface-modified scaffold in vivo. The final results of computed tomography (CT) perfusion imaging and histological examination proved that this facile coating approach could significantly promote blood perfusion and re-endothelialization in the early post-transplanted period compared with an acellular bone matrix due to its much-improved anticoagulation property.
机译:当前,组织工程领域中的主要障碍是如何在移植后早期为移植的组织替代物提供足够的血液供应。为了使三维,细胞致密的厚组织能够在移植后存活,需要对缺氧,营养不足和废物积聚进行治疗。在这项研究中,壳聚糖/肝素在脱细胞的细胞外骨基质上的生物大分子逐层包衣过程被设计为加速血液灌注和再内皮化过程。活化的部分凝血活酶时间的体外测量结果支持以下理论:壳聚糖和肝素的组合可以为支架带来抗凝和血液相容性。建立了兔骨缺损模型,以进一步评估这种表面修饰的支架在体内的应用。计算机断层扫描(CT)灌注成像和组织学检查的最终结果证明,与无细胞骨基质相比,这种简便的包被方法在移植后早期可以显着促进血液灌注和重新内皮化,因为其抗凝性能大大提高。

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