Center of Experimental Orthopaedics, Saarland University, D-66421 Homburg/Saar, Germany.
AO Research Institute Davos, 7270 Davos Platz, Switzerland.
Int J Mol Sci. 2018 Sep 5;19(9):2635. doi: 10.3390/ijms19092635.
The repair of focal articular cartilage defects remains a problem. Combining gene therapy with tissue engineering approaches using bone marrow-derived mesenchymal stem cells (MSCs) may allow the development of improved options for cartilage repair. Here, we examined whether a three-dimensional fibrin-polyurethane scaffold provides a favorable environment for the effective chondrogenic differentiation of human MSCs (hMSCs) overexpressing the cartilage-specific SOX9 transcription factor via recombinant adeno-associated virus (rAAV) -mediated gene transfer cultured in a hydrodynamic environment . Sustained SOX9 expression was noted in the constructs for at least 21 days, the longest time point evaluated. Such spatially defined SOX9 overexpression enhanced proliferative, metabolic, and chondrogenic activities compared with control (reporter gene transfer) treatment. Of further note, administration of the SOX9 vector was also capable of delaying premature hypertrophic and osteogenic differentiation in the constructs. This enhancement of chondrogenesis by spatially defined overexpression of human SOX9 demonstrate the potential benefits of using rAAV-modified hMSCs seeded in fibrin-polyurethane scaffolds as a promising approach for implantation in focal cartilage lesions to improve cartilage repair.
关节内软骨缺损的修复仍然是一个问题。将基因治疗与骨髓间充质干细胞(MSCs)的组织工程方法相结合,可能为软骨修复开发出更好的选择。在这里,我们研究了三维纤维蛋白-聚氨酯支架是否通过重组腺相关病毒(rAAV)介导的基因转移为在流体动力学环境中培养的过表达软骨特异性 SOX9 转录因子的人 MSCs(hMSCs)的有效软骨分化提供了有利的环境。在至少 21 天的最长时间点评估中,观察到构建体中持续表达 SOX9。与对照(报告基因转移)处理相比,这种空间限定的 SOX9 过表达增强了增殖、代谢和软骨形成活性。此外,SOX9 载体的给药也能够延迟构建体中过早的肥大和成骨分化。通过空间限定的人 SOX9 过表达增强软骨形成,证明了使用 rAAV 修饰的 hMSC 接种于纤维蛋白-聚氨酯支架作为在局灶性软骨病变中植入以改善软骨修复的有前途的方法的潜在益处。
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