首页> 美国卫生研究院文献>Tissue Engineering. Part A >Improved Mesenchymal Stem Cells Attachment and In Vitro Cartilage Tissue Formation on Chitosan-Modified Poly(l-Lactide-co-Epsilon-Caprolactone) Scaffold
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Improved Mesenchymal Stem Cells Attachment and In Vitro Cartilage Tissue Formation on Chitosan-Modified Poly(l-Lactide-co-Epsilon-Caprolactone) Scaffold

机译:壳聚糖修饰的聚(1-丙交酯-ε-己内酯)支架上的间充质干细胞附着和体外软骨组织形成的改善。

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摘要

Considering the load-bearing physiological requirement of articular cartilage, scaffold for cartilage tissue engineering should exhibit appropriate mechanical responses as natural cartilage undergoing temporary deformation on loading with little structural collapse, and recovering to the original geometry on unloading. A porous elastomeric poly l-lactide-co-ɛ-caprolactone (PLCL) was generated and crosslinked at the surface to chitosan to improve its wettability. Human bone marrow derived mesenchymal stem cells (MSC) attachment, morphological change, proliferation and in vitro cartilage tissue formation on the chitosan-modified PLCL scaffold were compared with the unmodified PLCL scaffold. Chitosan surface promoted more consistent and even distribution of the seeded MSC within the scaffold. MSC rapidly adopted a distinct spread-up morphology on attachment on the chitosan-modified PLCL scaffold with the formation of F-actin stress fiber which proceeded to cell aggregation; an event much delayed in the unmodified PLCL. Enhanced cartilage formation on the chitosan-modified PLCL was shown by real-time PCR analysis, histological and immunochemistry staining and biochemical assays of the cartilage extracellular matrix components. The Young's modulus of the derived cartilage tissues on the chitosan-modified PLCL scaffold was significantly increased and doubled that of the unmodified PLCL. Our results show that chitosan modification of the PLCL scaffold improved the cell compatibility of the PLCL scaffold without significant alteration of the physical elastomeric properties of PLCL and resulted in the formation of cartilage tissue of better quality.
机译:考虑到关节软骨的承载生理要求,用于软骨组织工程的支架应表现出适当的机械响应,因为天然软骨在加载时会发生暂时变形,几乎没有结构塌陷,并且在卸载时会恢复到原始几何形状。产生了多孔弹性体聚l-丙交酯-co-ε-己内酯(PLCL),并在表面交联至壳聚糖以改善其润湿性。比较了壳聚糖修饰的PLCL支架上人骨髓来源的间充质干细胞(MSC)的附着,形态变化,增殖和体外软骨组织形成与未修饰的PLCL支架。壳聚糖表面促进了种子MSC在支架内的更加一致和均匀的分布。 MSC在壳聚糖修饰的PLCL支架上附着时迅速采用了独特的扩展形态,形成F-肌动蛋白应激纤维,并逐渐聚集。未修改的PLCL中大大延迟的事件。通过实时PCR分析,软骨细胞外基质成分的组织学和免疫化学染色以及生化分析,可以证明壳聚糖修饰的PLCL上软骨形成的增强。壳聚糖修饰的PLCL支架上衍生的软骨组织的杨氏模量显着增加,是未修饰的PLCL的两倍。我们的结果表明,对PLCL支架进行壳聚糖修饰可改善PLCL支架的细胞相容性,而不会显着改变PLCL的物理弹性,并导致形成质量更好的软骨组织。

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