首页> 美国卫生研究院文献>International Journal of Molecular Sciences >Innovative Strategy for 3D Transfection of Primary Human Stem Cells with BMP-2 Expressing Plasmid DNA: A Clinically Translatable Strategy for Ex Vivo Gene Therapy
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Innovative Strategy for 3D Transfection of Primary Human Stem Cells with BMP-2 Expressing Plasmid DNA: A Clinically Translatable Strategy for Ex Vivo Gene Therapy

机译:用表达BMP-2的质粒DNA进行人类干细胞3D转染的创新策略:体内基因治疗的临床可翻译策略

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摘要

Ex vivo gene therapy offers enormous potential for cell-based therapies, however, cumbersome in vitro cell culture conditions have limited its use in clinical practice. We have optimized an innovative strategy for the transient transfection of bone morphogenetic protein-2 (BMP-2) expressing plasmids in suspended human stem cells within 5-min that enables efficient loading of the transfected cells into a 3D hydrogel system. Such a short incubation time for lipid-based DNA nanoparticles (lipoplexes) reduces cytotoxicity and at the same time reduces the processing time for cells to be transplanted. The encapsulated human mesenchymal stromal/stem cells (hMSCs) transfected with BMP-2 plasmid demonstrated high expression of an osteogenic transcription factor, namely RUNX2, but not the chondrogenic factor (SOX9), within the first three days. This activation was also reflected in the 7-day and 21-day experiment, which clearly indicated the induction of osteogenesis but not chondrogenesis. We believe our transient transfection method demonstrated in primary MSCs can be adapted for other therapeutic genes for different cell-based therapeutic applications.
机译:离体基因疗法为基于细胞的疗法提供了巨大的潜力,但是,繁琐的体外细胞培养条件限制了其在临床实践中的使用。我们优化了一种创新策略,用于在5分钟内在悬浮的人类干细胞中瞬时转染表达骨形态发生蛋白2(BMP-2)的质粒,从而使转染的细胞有效地装载到3D水凝胶系统中。对基于脂质的DNA纳米颗粒(脂质复合物)的如此短的温育时间减少了细胞毒性,同时减少了要移植细胞的处理时间。用BMP-2质粒转染的封装的人间充质基质/干细胞(hMSC)在头三天内显示了成骨转录因子(即RUNX2)而非软骨生成因子(SOX9)的高表达。在7天和21天的实验中也反映了这种激活,该实验清楚地表明诱导了成骨作用,但没有诱导软骨形成。我们相信在原代MSC中证明的我们的瞬时转染方法可以适用于其他治疗基因,用于不同的基于细胞的治疗应用。

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