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首页> 外文期刊>Medical hypotheses >Injectable allogeneic bone mesenchymal stem cells: a potential minimally invasive therapy for atrophic nonunion.
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Injectable allogeneic bone mesenchymal stem cells: a potential minimally invasive therapy for atrophic nonunion.

机译:可注射的同种异体骨间充质干细胞:萎缩性骨不连的潜在微创疗法。

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摘要

How to enhance atrophic nonunion repairing is a common challenge encountered in orthopaedic surgeons. With the increasing popularity of minimally invasive techniques, one of the major thrusts in treatment approaches for atrophic nonunions is to develop injectable systems that can shorten the surgical operation time, reduce the morbidity and costs for patients. Bone mesenchymal stem cells (BMSCs) may provide new strategies to treat atrophic nonunion because of their prolonged self-renewal capacity and ability to differentiate into osteogenic lineage under the proper conditions. However, providing an autologous BMSCs in the clinical setting is often limited, because the patient's marrow is damaged or the cell yield from healthy marrow is reduced. Due to the limitation of autologous BMSCs in clinical application, we turn to consider allogeneic BMSCs as seeding cells in atrophic nonunion repair. Allogeneic BMSCs could are isolated from one or more donors would have the potential to be expanded and cryopreserved for future use. Previous studies have indicated that BMSCs possess immune-privileged properties, which avoid or actively suppress the immunological responses. Here we propose the hypothesis that the application of osteo-induced allogeneic BMSCs in fibrin gels for delivery of the cells by means of an injectable device would enhance repair of atrophic nonunion without the use of immunosuppressive therapy. Furthermore, fibrin gel could be useful as BMSCs carrier to deliver cells in vivo, there is no immunogenicity to be expected and BMSCs were able to spread and proliferate into the fibrin. Therefore, if the hypothesis is proved to be practical, it might represent a novel minimally invasive therapeutic approach and enhance atrophic nonunion repairing.
机译:如何增强萎缩性骨不连的修复是整形外科医师所面临的普遍挑战。随着微创技术的日益普及,萎缩性骨不连的治疗方法的主要重点之一是开发可缩短手术时间,降低患者发病率和成本的可注射系统。骨髓间充质干细胞(BMSCs)可能会提供新的策略来治疗萎缩性骨不连,因为它们具有延长的自我更新能力以及在适当条件下能够分化为成骨细胞系的能力。然而,在临床环境中提供自体骨髓间充质干细胞通常受到限制,因为患者的骨髓受损或健康骨髓的细胞产量降低。由于自体骨髓间充质干细胞在临床应用中的局限性,我们转向将同种异体骨髓间充质干细胞作为萎缩性骨不连修复中的种子细胞。可以从一个或多个供体中分离出同种异体骨髓间充质干细胞,它们有可能被扩增和冷冻保存以备将来使用。先前的研究表明,骨髓间充质干细胞具有免疫特权的特性,可以避免或积极抑制免疫反应。在这里,我们提出这样的假说,即在纤维蛋白凝胶中将骨诱导的同种异体骨髓间充质干细胞用于通过注射装置递送细胞的方法,将在不使用免疫抑制疗法的情况下增强对萎缩性骨不连的修复。此外,纤维蛋白凝胶可以用作BMSCs载体在体内递送细胞,没有免疫原性,BMSCs能够扩散并增殖到纤维蛋白中。因此,如果该假设被证明是可行的,则它可能代表了一种新颖的微创治疗方法,并增强了萎缩性骨不连的修复。

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