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In vitro cartilage tissue engineering with 3D porous aqueous-derived silk scaffolds and mesenchymal stem cells

机译:使用3D多孔水源性丝支架和间充质干细胞进行体外软骨组织工程

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Adult cartilage tissue has limited self-repair capacity, especially in the case of severe damages caused by developmental abnormalities, trauma, or aging-related degeneration like osteoarthritis. Adult mesenchymal stem cells (MSCs) have the potential to differentiate into cells of different lineages including bone, cartilage, and fat. In vitro cartilage tissue engineering using autologous MSCs and three-dimensional (3-D) porous scaffolds has the potential for the successful repair of severe cartilage damage. Ideally, scaffolds designed for cartilage tissue engineering should have optimal structural and mechanical properties, excellent biocompatibility, controlled degradation rate, and good handling characteristics. In the present work, a novel, highly porous silk scaffold was developed by an aqueous process according to these criteria and subsequently combined with MSCs for in vitro cartilage tissue engineering. Chondrogenesis of MSCs in the silk scaffold was evident by real-time RT-PCR analysis for cartilage-specific ECM gene markers, histological and immunohistochemical evaluations of cartilage-specific ECM components. Dexamethasone and TGF-beta 3 were essential for the survival, proliferation and chondrogenesis of MSCs in the silk scaffolds. The attachment, proliferation, and differentiation of MSCs in the silk scaffold showed unique characteristics. After 3 weeks of cultivation, the spatial cell arrangement and the collagen type-II distribution in the MSCs-silk scaffold constructs resembles those in native articular cartilage tissue, suggesting promise for these novel 3-D degradable silk-based scaffolds in MSC-based cartilage repair. Further in vivo evaluation is necessary to fully recognize the clinical relevance of these observations. (c) 2005 Elsevier Ltd. All rights reserved.
机译:成人软骨组织的自我修复能力有限,尤其是在由于发育异常,创伤或与衰老相关的变性(如骨关节炎)引起的严重损害的情况下。成人间充质干细胞(MSC)具有分化为包括骨骼,软骨和脂肪在内的不同谱系细胞的潜力。使用自体MSC和三维(3-D)多孔支架进行体外软骨组织工程具有成功修复严重软骨损伤的潜力。理想地,为软骨组织工程设计的支架应具有最佳的结构和机械性能,出色的生物相容性,可控的降解速率以及良好的处理特性。在目前的工作中,根据这些标准通过水性方法开发了一种新型的,高度多孔的丝绸支架,随后与MSCs结合用于体外软骨组织工程。通过实时RT-PCR分析软骨特异性ECM基因标记,软骨特异性ECM成分的组织学和免疫组织化学评估,可以证明丝支架中MSC的软骨形成。地塞米松和TGF-β3对于丝支架中MSC的存活,增殖和软骨形成至关重要。丝支架中的MSCs的附着,增殖和分化显示出独特的特征。培养3周后,MSCs-丝支架构建物中的空间细胞排列和II型胶原分布与天然关节软骨组织中的相似,这为基于MSC软骨的这些新型3D可降解丝基支架提供了希望。修理。为了充分认识这些观察结果的临床相关性,必须进行进一步的体内评估。 (c)2005 Elsevier Ltd.保留所有权利。

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