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首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >Intra-articular delivery of synovium-resident mesenchymal stem cells via BMP-7-loaded fibrous PLGA scaffolds for cartilage repair
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Intra-articular delivery of synovium-resident mesenchymal stem cells via BMP-7-loaded fibrous PLGA scaffolds for cartilage repair

机译:通过BMP-7加载的纤维化PLGA支架进行静脉内递送滑膜 - 静脉间充质干细胞用于软骨修复

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摘要

Delivery of synovium-resident mesenchymal stem cells (synMSCs) to cartilage defect site might provide a novel therapeutic modally for treatment of articular cartilage diseases. However, low isolation efficiency of synMSCs limits their therapeutic application. Niche-preserving non-enzymatic isolation of synMSCs was firstly attempted by employing micro-organ culture system based on recapitulating tissue-specific homeostasis ex vivo. The isolated synMSCs retained superior long-term growth competency, proliferation and chondrogenic potential to bone marrow-derived MSCs (BMSCs). It was noted that synMSCs demonstrated 9-fold increase in cartilaginous micro-tissue formation and 13-fold increase in sulfated proteoglycans deposition compared to BMSCs. For delivery of synMSCs, fibrous PLGA scaffolds were specifically designed for full-thickness osteochondral defects in rabbits. The scaffolds provided effective micro-environment for growth and host-integration of synMSCs. Combined delivery of synMSCs with bone morphogenetic proteins-7 (BMP-7) was designed to achieve synergistic therapeutic efficacy. BMP-7-loaded PLGA nanoparticles electrosprayed onto the scaffolds released BMP-7 over 2 weeks to conform with its aimed role in stimulating early stage endochondral ossification. Scaffold-supported combined administration of synMSCs with BMP-7 resulted in high proteoglycan and collagen type II induction and thick hyaline cartilage formation. Intra-articular co-delivery of synMSCs with BMP-7 via fibrous PLGA scaffolds may be a promising therapeutic modality for articular cartilage repair.
机译:将Synovium-Resident间充质干细胞(Synmscs)输送到软骨缺陷部位,可以提供一种新的治疗模式,用于治疗关节软骨疾病。然而,SYNMSCS的低隔离效率限制了其治疗应用。首先通过使用基于重新携带的组织特异性稳态,通过使用微型器官培养系统来试图维持尼基肽的非酶促分离。孤立的SYNMSCS对骨髓衍生的MSCs(BMSCs)保持优异的长期生长能力,增殖和软骨性潜力。有人指出,与BMSC相比,SYNMSS在软骨微组织形成和硫酸化蛋白多糖沉积中增加了13倍的增加。为了交付同步,纤维化PLGA支架专门用于兔子的全厚度骨质缺陷。脚手架提供了有效的微环境,用于增长和宿主的Synmscs。设计与骨形态发生蛋白-7(BMP-7)的同步递送递送,以达到协同治疗效果。 BMP-7加载的PLGA纳米粒子电喷雾到支架上释放BMP-7超过2周,以符合其针对刺激早期oftochongront骨化的作用。支持支架支持的Synmscs的组合施用BMP-7导致高蛋白质酚和胶原II型诱导和厚透明软骨形成。通过纤维PLGA支架具有BMP-7的关节内同步的同步递送可以是用于关节软骨修复的有希望的治疗方式。

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