首页> 外文期刊>Stem Cell Research & Therapy >Mesenchymal stem cell-loaded porous tantalum integrated with biomimetic 3D collagen-based scaffold to repair large osteochondral defects in goats
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Mesenchymal stem cell-loaded porous tantalum integrated with biomimetic 3D collagen-based scaffold to repair large osteochondral defects in goats

机译:间充质干细胞负载的多孔钽与仿生3D胶原基支架相结合,可修复山羊的大型骨软骨缺损

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The body is unable to repair and regenerate large area bone defects. Moreover, the repair capacity of articular cartilage is very limited. There has long been a lack of effective treatments for osteochondral lesions. The engineered tissue with biphase synthetic for osteochondral repair has become one of the hot research fields over the past few years. In this study, an integrated biomanufacturing platform was constructed with bone marrow mesenchymal stem cells (BMSCs)/porous tantalum (pTa) associated with chondrocytes/collagen membranes (CM) to repair large osteochondral defects in load-bearing areas of goats. Twenty-four goats with a large osteochondral defect in the femoral heads of the left hind legs were randomly divided into three groups: eight were treated with chondrocytes/CM-BMSCs/pTa, eight were treated with pure CM-pTa composite, and the other eight goats were untreated. The repair effect was assessed by X-ray, gross observation, and histomorphology for 16?weeks after the operation. In addition, the biocompatibility of chondrocytes/CM-BMSCs/pTa was observed by flow cytometry, CCK8, immunocytochemistry, and Q-PCR. The characteristics of the chondrocytes/CM-BMSCs/pTa were evaluated using both scanning electron microscopy and mechanical testing machine. The integrated repair material consists of pTa, injectable fibrin sealant, and CM promoted adhesion and growth of BMSCs and chondrocytes. pTa played an important role in promoting the differentiation of BMSCs into osteoblasts. Three-dimensional CM maintained the phenotype of chondrocytes successfully and expressed chondrogenic genes highly. The in vivo study showed that after 16?weeks from implantation, osteochondral defects in almost half of the femoral heads had been successfully repaired by BMSC-loaded pTa associated with biomimetic 3D collagen-based scaffold. The chondrocytes/CM-BMSCs/pTa demonstrated significant therapeutic efficacy in goat models of large osteochondral defect. This provides a novel therapeutic strategy for large osteochondral lesions in load-bearing areas caused by severe injury, necrosis, infection, degeneration, and tumor resection with a high profile of safety, effectiveness, and simplicity.
机译:身体无法修复和再生大面积的骨缺损。而且,关节软骨的修复能力非常有限。长期以来,一直缺乏有效的治疗骨软骨损伤的方法。在过去的几年中,具有双相合成的骨软骨修复工程组织已经成为研究的热点之一。在这项研究中,构建了一个集成的生物制造平台,其中包括骨髓间充质干细胞(BMSC)/多孔钽(pTa)和软骨细胞/胶原膜(CM),以修复山羊承重区域的大型软骨软骨缺损。将二十四只在左后腿股骨头处具有较大软骨软骨缺损的山羊随机分为三组:八只用软骨细胞/ CM-BMSCs / pTa处理,八只用纯CM-pTa复合物处理,另一只八只山羊未经治疗。术后16周通过X线,肉眼观察和组织形态学评估修复效果。另外,通过流式细胞术,CCK8,免疫细胞化学和Q-PCR观察到了软骨细胞/ CM-BMSCs / pTa的生物相容性。使用扫描电子显微镜和机械测试仪评估软骨细胞/ CM-BMSCs / pTa的特性。整合的修复材料由pTa,可注射的纤维蛋白密封剂和CM促进BMSC和软骨细胞的粘附和生长组成。 pTa在促进BMSCs向成骨细胞的分化中起重要作用。三维CM成功地维持了软骨细胞的表型,并高度表达了软骨形成基因。体内研究表明,植入后16周,股骨软骨缺损已通过BMSC加载的pTa与仿生3D胶原基支架相关联成功修复。软骨细胞/ CM-BMSCs / pTa在大骨软骨缺损的山羊模型中显示出显着的治疗功效。这为由重伤,坏死,感染,变性和肿瘤切除引起的承重区域的大型骨软骨病变提供了一种新颖的治疗策略,具有高度的安全性,有效性和简便性。

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