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Osteochondral tissue engineering based on biomimetic osteochondral scaffold contained calcified cartilage layer compounding with ADSCs in vitro and vivo

机译:基于仿生骨质色神经支架的骨质色素组织工程含有钙化软骨层,在体外和体内与ADSCs配混

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Introduction: The biomimetic osteochondral scaffold contained calcified cartilage layer (CCL) was fabricated with slik fibroin (SF) and hydroxyapatite (HA). To investigate the effects of biomimetic osteochondral scaffold contained CCL compounding with ADSCs on regeneration of the osteochondral defect, especially the role of CCL in vivo, and explore the feasibility of this design as a concept of osteochondral tissue engineering. Materials and Methods: We fabricated a novel biomimetic osteochondral scaffold with CCL using SF and HA by the combination of paraffin-sphere leaching and modified temperature gradient-guided thermal-induced phase separation (TIPS) technique (Figure 1). ADSCs were seeded into the scaffold. The structure of scaffold, the cell adhesion, proliferation and viability on scaffold were observed by SEM, micro-CT, Dead/Live staining and other tests. Two different cell fluorescence labeling technique (DiO/Dil) were adopted for verifying the isolation of CCL between the osteogenic and chondral layers. The osteochondral defect model on rabbit bilateral knees were established, and implanted with the CCL+ADSCs, Non-CCL+ADSCs, CCL (no cells) and non-treated groups. At 4w, 8w and 12w after implantation, gross observation score, histological and immunohistochemical assessment, biochemical quantitative and biomectianical testing of new osteochondral tissue, micro-CT scans for new bone, were executed. Figure 1. Schematic diagrams of preparation process Results and Discussion: The scaffold had a consecutively overlapping trilayer structure with different densities and pore structures, approximately bionic the normal osteochondral structure. SEM, Dead/Live staining and other tests had shown good ability of cell adhesion, proliferation on scaffold. The CCL effectively isolated the cells among chondral and osteogenic layers(Figure 2). The cartilage regeneration in CCL+ADSCs group was better than Non-CCL+ADSCs group and CCL group, mainly reflected in flatness and integrity of cartilage. The content of GAG and type Ⅱ collagen in new cartilage tissue in CCL+ADSCs group more than the other groups(Figure 3). The results meant that the CCL contributed to the growth of cartilage. The quality and intensity of new bone in CCL+ADSCs and Non-CCL+ADSCs groups were higher than the CCL group, and no significant differences between first two groups. It meant that the ADSCs produced positive effects on the growth of bone. Figure 2. The isolated role of CCL Figure 3. Histological assessment of new osteochondral tissue Conclusion: The biomimetic osteochondral scaffold contained CCL approximately bionics the normal osteochondral structure, the CCL can isolate the different microenvironment for the growth of cartilage and bone. The scaffold compounding with ADSCs satisfactory regenerate the rabbit osteochondral defect, the CCL can accelerate the growth of cartilage tissue, especially the secretion of ECM, and the ADSCs contributes to the quality and intensity of new bone. the National Natural Science Foundation of China (Nos.31470937, 31300798, 31000432 and 81272046).
机译:简介:含有钙化软骨层(CCL)的生物摩托骨质支架(CCL)用Slik丝蛋白(SF)和羟基磷灰石(HA)制备。为了探讨仿生骨骨骨支架的效果CCL复合与ADSC对骨质色神经缺损的再生,尤其是CCL在体内的作用,并探讨了这种设计的可行性作为骨质色组织工程的概念。材料与方法:通过石蜡球浸出和改性温度梯度引导的热诱导的相分离(TIPS)技术,使用SF和HA用CCL制造了一种新的生物仿生骨髓支架用CCL。将ADSC接种到支架中。通过SEM,微型CT,死/活染料和其他测试观察支架的结构的支架,细胞粘附,增殖和活力。采用两种不同的细胞荧光标记技术(DIO / DIO)来验证骨质发生和骨囊层之间CCL的分离。建立了兔双侧膝关节缺陷模型,并植入了CCL + ADSCs,非CCL + ADSCs,CCL(无细胞)和未治疗组。在4W,8W和12W植入后,进行了粗略观察评分,组织学和免疫组织化学评估,新骨髓组织的生物化学定量和生物学检测,新骨的微型CT扫描。图1.制备工艺结果和讨论的示意图:支架具有具有不同密度和孔结构的连续重叠的三层结构,致正常骨质色神经结构。 SEM,死亡/直播染色和其他测试表明了良好的细胞粘附能力,支架上的粘附能力。 CCL有效地分离了骨髓和骨质形成层中细胞(图2)。 CCL + ADSCS组的软骨再生优于非CCL + ADSCS组和CCL组,主要反映在软骨的平整度和完整性。 CCL + ADSCS组新软骨组织中GAG和Ⅱ型胶原蛋白的含量多于其他基团(图3)。结果意味着CCL促成了软骨的生长。 CCL + ADSC和非CCL + ADSCS组新骨的质量和强度高于CCL组,前两组之间没有显着差异。这意味着ADSCS对骨骼的生长产生了积极影响。图2. CCL的分离作用图3.新骨质色组织组织学的组织学评估结论:染色骨质色神经支架含有CCL大约仿生学正常骨质色神经结构,CCL可以分离不同的微环境以进行软骨和骨的生长。通过ADSCS的支架配合令人满意的再生兔骨色神经缺损,CCL可以加速软骨组织的生长,特别是ECM的分泌,并且ADSCS有助于新骨的质量和强度。中国国家自然科学基金(No.31470937,31300798,31000432和81272046)。

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