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Design and in vitro release study of siRNA loaded Layer by Layer nanoparticles with sustained gene silencing effect

机译:纳米粒子持续基因沉默效应的分层纳米粒子的设计和体外释放研究

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ABSTRACT, Objectives: Clinical translation of siRNA therapeutics has been severely limited due to the lack of stable and sustained siRNA delivery systems. Furthermore, when nanocarrier systems with siRNA are administered systemically to treat diseases, insufficient doses reach the target tissue. Here we report the successful development of a new nanocarrier system for the management of fibrosis. Methods: The new carrier has a hydroxyapatite core, with alternating layers of siRNA and a cationic peptide. The siRNA used here targets secreted protein acidic and rich in cysteine (SPARC), a key matricellular protein involved in the regulation of collagen fibrillogenesis and assembly. We have also used FRET studies to elucidate the fate of the particles inside cells, including the mechanistic details of layer-by-layer detachment. Results: In vitro studies using murine conjunctiva fibroblasts show sustained release over 2 weeks, and that such released siRNA sustained SPARC knockdown without affecting cell growth, and maintained siRNA presence in the cells for at least two weeks with a single-dose treatment. Release studies of siRNA from particles in vitro gave insight on how the particles delivered prolonged gene-silencing effects. Conclusion: A single treatment of the layer-by-layer nanoparticle designed can achieve sustained gene silencing over 2 weeks. Localized delivery of stabilized siRNA with sustained-release capabilities opens the door for many other applications of siRNA-based gene regulation.
机译:摘要,目标:由于缺乏稳定和持续的siRNA递送系统,SiRNA治疗剂的临床翻译受到严重限制。此外,当具有SiRNA的纳米载波系统系统性地施用以治疗疾病,剂量不足达到靶组织。在这里,我们举报了一个新的纳米载波系统的成功开发,用于纤维化的管理。方法:新型载体具有羟基磷灰石核,具有siRNA的交替层和阳离子肽。这里使用的siRNA靶向分泌的蛋白质酸性和富含半胱氨酸(SPARC)的含量,该蛋白质是胶原纤维生成和组装的调节。我们还使用FRET研究来阐明细胞内颗粒的命运,包括层逐层脱离的机械细节。结果:使用鼠结膜成纤维细胞的体外研究显示超过2周的持续释放,并且这种释放的siRNA持续的SPARC敲低,而不会影响细胞生长,并通过单剂量处理保持在细胞中的siRNA存在至少两周。体外颗粒的siRNA的释放研究已经了解粒子如何延长基因沉默效果。结论:逐层纳米粒子设计的单一处理可以在2周内实现持续基因沉默。具有持续释放能力的稳定siRNA的局部递送为SiRNA的基因调控的许多其他应用打开门。

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