首页> 外文期刊>Journal of bone and mineral metabolism >Intra-articular injection of hUC-MSCs expressing miR-140-5p induces cartilage self-repairing in the rat osteoarthritis
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Intra-articular injection of hUC-MSCs expressing miR-140-5p induces cartilage self-repairing in the rat osteoarthritis

机译:表达miR-140-5p的HUC-MSCs的关节内注射诱导大鼠骨关节炎中的软骨自我修复

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Introduction Currently, osteoarthritis (OA) receives global increasing attention because it associates severe joint pain and serious disability. Stem cells intra-articular injection therapy showed a potential therapeutic superiority to reduce OA development and to improve treating outputs. However, the long-term effect of stem cells intra-articular injection on the cartilage regeneration remains unclear. Recently, miR-140-5p was confirmed as a critical positive regulator in chondrogenesis. We hypothesized that hUC-MSCs overexpressing miR-140-5p have better therapeutic effect on osteoarthritis. Materials and methods To enhance stem cell chondrogenic differentiation, we have transfected human umbilical cord mesenchymal stem cells (hUC-MSCs) with miR-140-5p mimics and miR-140-5p lentivirus to overexpress miR-140-5p in a short term or a long term accordingly. Thereafter, MSCs proliferation, chondrogenic genes expression and extracellular matrix were assessed. Destabilization of the medial meniscus (DMM) surgery was performed on the knee joints of SD rats as an OA model, and then intra-articular injection of hUC-MSCs or hUC-MSCs transfected with miR-140-5p lentivirus was carried to evaluate the cartilage healing effect with histological staining and OARSI scores. The localization of hUC-MSCs after intra-articular injection was further confirmed by immunohistochemical staining. Results Significant induction of chondrogenic differentiation in the miR-140-5p-hUC-MSCs (140-MSCs), while its proliferation was not influenced. Interestingly, intra-articular injection of 140-MSCs significantly enhanced articular cartilage self-repairing in comparison to normal hUC-MSCs. Moreover, we noticed that intra-articular injection of high 140-MSCs numbers reinforces cells assembling on the impaired cartilage surface and subsequently differentiated into chondrocytes. Conclusions In conclusion, these results indicate therapeutic superiority of hUC-MSCs overexpressing miR-140-5p to treat OA using intra-articular injection.
机译:介绍目前,骨关节炎(OA)获得全球越来越多的关注,因为它与严重的关节疼痛和严重的残疾联系起来。干细胞特性注射治疗表现出潜在的治疗优势,以减少OA开发并改善治疗产出。然而,干细胞关节内注射对软骨再生的长期效果仍不清楚。最近,MiR-140-5P被证实为软骨发生中的关键阳性调节剂。我们假设过表达miR-140-5p的HUC-MSCs对骨关节炎具有更好的治疗作用。提高干细胞软骨发生的材料和方法,我们用miR-140-5p模拟物和miR-140-5p慢病毒转染了人脐部间充质干细胞(HUC-MSCs),在短期内或相应的长期。此后,评估MSCs增殖,软骨基因表达和细胞外基质。在SD大鼠的膝关节中进行内膜肿块(DMM)手术的稳定化作为OA模型,然后进行关节内注射用miR-140-5p慢病毒转染的HUC-MSC或HUC-MSCs进行评估软骨愈合效果与组织学染色和划桨分数。通过免疫组织化学染色进一步证实了在关节内注射后HUC-MSC的定位。结果MIR-140-5P-HUC-MSCs(140-MSCs)中有显着诱导软骨分化,而其增殖不会影响。有趣的是,与正常HUC-MSCs相比,关节内注射140mSS的140mSCs显着增强了关节软骨自修复。此外,我们注意到,关节内注射高140mCS数量增强组装在受损的软骨表面上的细胞,随后分化为软骨细胞。结论总之,这些结果表明,使用关节内注射治疗MIR-140-5P的HUC-MSCs治疗OA的治疗优势。

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