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Simultaneous Delivery of Hydrophobic Small Molecules and siRNA Using Sterosomes to Direct Mesenchymal Stem Cell Differentiation for Bone Repair

机译:疏水小分子和siRNA的同时传递利用脂质体直接间充质干细胞分化的骨修复。

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摘要

The use of small molecular drugs with gene manipulation offers synergistic therapeutic efficacy by targeting multiple signaling pathways for combined treatment. Stimulation of mesenchymal stem cells (MSCs) with osteoinductive small molecule phenamil combined with suppression of noggin is a promising therapeutic strategy that increases bone morphogenetic protein (BMP) signaling and bone repair. Our cationic Sterosome formulated with stearylamine (SA) and cholesterol (Chol) is an attractive co-delivery system that not only forms stable complexes with small interfering RNA (siRNA) molecules but also solubilizes hydrophobic small molecules in a single vehicle, for directing stem cell differentiation. Herein, we demonstrate the ability of SA/Chol Sterosomes to simultaneously deliver hydrophobic small molecule phenamil and noggin-directed siRNA to enhance osteogenic differentiation of MSCs both in in vitro two- and three-dimensional settings as well as in a mouse calvarial defect model. These results suggest a novel liposomal platform to simultaneously deliver therapeutic genes and small molecules for combined therapy.
机译:小分子药物与基因操作一起使用可通过靶向多种联合治疗途径的信号传导途径提供协同治疗效果。骨诱导性小分子苯甲酰胺与Noggin抑制相结合刺激间充质干细胞(MSCs)是增加骨形态发生蛋白(BMP)信号传导和骨修复的有前途的治疗策略。我们的由硬脂胺(SA)和胆固醇(Chol)配制而成的阳离子Sterosome是一种有吸引力的共递送系统,它不仅可以与小的干扰RNA(siRNA)分子形成稳定的复合物,而且可以在单个载体中溶解疏水性小分子,从而指导干细胞差异化。在本文中,我们证明了SA / Chol脂质体在体外二维和三维环境以及小鼠颅骨缺损模型中同时递送疏水性小分子苯甲酰胺和头蛋白定向siRNA的能力,以增强MSC的成骨分化。这些结果表明,新型脂质体平台可同时递送治疗基因和小分子以进行联合治疗。

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