首页> 美国卫生研究院文献>Frontiers in Physiology >Combination of Collagen-Based Scaffold and Bioactive Factors Induces Adipose-Derived Mesenchymal Stem Cells Chondrogenic Differentiation In vitro
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Combination of Collagen-Based Scaffold and Bioactive Factors Induces Adipose-Derived Mesenchymal Stem Cells Chondrogenic Differentiation In vitro

机译:胶原蛋白支架和生物活性因子的组合诱导脂肪来源的间充质干细胞体外软骨分化。

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摘要

Recently, multipotent mesenchymal stem cells (MSCs) have attracted much attention in the field of regenerative medicine due to their ability to give rise to different cell types, including chondrocytes. Damaged articular cartilage repair is one of the most challenging issues for regenerative medicine, due to the intrinsic limited capability of cartilage to heal because of its avascular nature. While surgical approaches like chondral autografts and allografts provide symptoms and function improvement only for a short period, MSC based stimulation therapies, like microfracture surgery or autologous matrix-induced chondrogenesis demonstrate to be more effective. The use of adult chondrocytes, which are the main cellular constituent of cartilage, in medical practice, is indeed limited due to their instability in monolayer culture and difficulty to collect donor tissue (articular and nasal cartilage). The most recent cartilage engineering approaches combine cells, biomaterial scaffold and bioactive factors to promote functional tissue replacements. Many recent evidences demonstrate that scaffolds providing specific microenvironmental conditions can promote MSCs differentiation toward a functional phenotype. In the present work, the chondrogenic potential of a new Collagen I based 3D scaffold has been assessed in vitro, in combination with human adipose-derived MSCs which possess a higher chondrogenic potential compared to MSCs isolated from other tissues. Our data indicate that the scaffold was able to promote the early stages of chondrogenic commitment and that supplementation of specific soluble factors was able to induce the complete differentiation of MSCs in chondrocytes as demonstrated by the appearance of cartilage distinctive markers (Sox 9, Aggrecan, Matrilin-1, and Collagen II), as well as by the cartilage-specific Alcian Blue staining and by the acquisition of typical cellular morphology. Such evidences suggest that the investigated scaffold formulation could be suitable for the production of medical devices that can be beneficial in the field of articular cartilage engineering, thus improving the efficacy and durability of the current therapeutic options.
机译:最近,多能间充质干细胞(MSCs)由于其产生包括软骨细胞在内的不同细胞类型的能力而在再生医学领域引起了很多关注。关节软骨修复受损是再生医学中最具挑战性的问题之一,这是由于软骨的无血管特性,其固有的有限的愈合能力。虽然像软骨自体移植和同种异体移植这样的外科手术方法仅在短期内提供症状和功能改善,但基于MSC的刺激疗法(如微骨折手术或自体基质诱导的软骨形成)却显示出更有效的效果。在医学实践中,成年软骨细胞是软骨的主要细胞成分,由于其在单层培养中的不稳定性以及难以收集供体组织(关节和鼻软骨),的使用确实受到限制。最新的软骨工程方法结合了细胞,生物材料支架和生物活性因子来促进功能性组织置换。最近的许多证据表明,提供特定微环境条件的支架可以促进MSC向功能表型的分化。在当前的工作中,已经对新的基于胶原I的3D支架的软骨形成潜力进行了评估,并与从其他组织分离的MSC相比具有更高软骨形成潜力的人脂肪来源的MSC进行了评估。我们的数据表明,该支架能够促进软骨形成承诺的早期阶段,并且补充特定的可溶性因子能够诱导软骨细胞中MSC的完全分化,这通过软骨独特标志物的出现(Sox 9,Aggrecan,Matrilin -1和胶原蛋白II),以及通过软骨特有的Alcian Blue染色和通过采集典型的细胞形态来获得。这样的证据表明,所研究的支架制剂可能适合于在关节软骨工程领域中有益的医疗器械的生产,从而提高了当前治疗选择的功效和耐用性。

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