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Achilles Tendon Repair by Decellularized and Engineered Xenografts in a Rabbit Model

机译:Achilles肌腱修复在兔模型中脱细胞化和工程的异种移植物修复

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Tendon tissue ruptures often require the replacement of damaged tissues. The use of auto- or allografts is notoriously limited due to the scarce supply and the high risks of immune adverse reactions. To overcome these limitations, tissue engineering (TE) has been considered a promising approach. Among several biomaterials, decellularized xenografts are available in large quantity and could represent a possible solution for tendon reconstruction. The present study is aimed at evaluating TE xenografts in Achilles tendon defects. Specifically, the ability to enhance the biomechanical functionality, while improving the graft interaction with the host, was tested. The combination of decellularized equine-derived tendon xenografts with or without the matrix repopulation with autologous bone marrow mesenchymal stem cells (BMSCs) under stretch-perfusion dynamic conditions might improve the side-to-side tendon reconstruction. Thirty-six New Zealand rabbits were used to create 2?cm long segmental defects of the Achilles tendon. Then, animals were implanted with autograft (AG) as the gold standard control, decellularized graft (DG), or in vitro tissue-engineered graft (TEG) and evaluated postoperatively at 12 weeks. After sacrifice, histological, immunohistochemical, biochemical, and biomechanical analyses were performed along with the matrix metalloproteinases. The results demonstrated the beneficial role of undifferentiated BMSCs loaded within decellularized xenografts undergoing a stretch-perfusion culture as an immunomodulatory weapon reducing the inflammatory process. Interestingly, AG and TEG groups exhibited similar results, behaved similarly, and showed a significant superior tissue healing compared to DG in terms of newly formed collagen fibres and biomechanical parameters. Whereas, DG demonstrated a massive inflammatory and giant cell response associated with graft destruction and necrosis, absence of type I and III collagen, and a higher amount of proteoglycans and MMP-2, thus unfavourably affecting the biomechanical response. In conclusion, this in vivo study suggests a potential use of the proposed tissue-engineered constructs for tendon reconstruction.
机译:肌腱组织破裂通常需要更换受损组织。由于稀缺供应和免疫不良反应的高风险,使用自动或同种异体移植物的使用是众所周知的。为了克服这些限制,组织工程(TE)被认为是一个有希望的方法。在几种生物材料中,脱细胞化异种移植物的数量可用,并且可以代表肌腱重建的可能解决方案。本研究旨在评估在阿基尔斯肌腱缺陷中的特生移植物。具体地,测试了增强生物力学功能的能力,同时改善与宿主的接枝相互作用。在拉伸 - 灌注动态条件下具有或不具有基质骨髓间充质干细胞(BMSC)的脱细胞的马克酸肌腱移植物的组合可以改善侧向肌腱重建。三六十六个新西兰兔子用于创造2厘米的Achilles肌腱节段缺陷。然后,将动物植入自体移植物(Ag)作为金标准对照,脱细胞化移植物(DG)或体外组织工程移植物(TEG),并在术后12周进行评估。牺牲后,组织学,免疫组织化学,生物化学和生物力学分析与基质金属蛋白酶一起进行。结果表明,未分化的BMSC的有益作用,其在经历拉伸灌注培养的脱细胞化异种移植物中作为免疫调节武器减少炎症过程。有趣的是,AG和TEG集团表现出类似的结果,表现得同样,并且与新形成的胶原纤维和生物力学参数相比,与DG相比表现出显着的卓越组织愈合。然而,DG展示了与移植物破坏和坏死相关的巨大炎症和巨型细胞应答,没有I型和III胶原,以及较高量的蛋白多糖和MMP-2,因此不利地影响生物力学反应。总之,这在体内研究表明,潜在使用所提出的组织工程构建体用于肌腱重建。

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