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Covalently tethering siRNA to hydrogels for localized, controlled release and gene silencing

机译:将siRNA与水凝胶共价绑定以实现局部,控制释放和基因沉默

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Small interfering RNA (siRNA) has found many applications in tissue regeneration and disease therapeutics. Effective and localized siRNA delivery remains challenging, reducing its therapeutic potential. Here, we report a strategy to control and prolong siRNA release by directly tethering transfection-capable siRNA to photocrosslinked dextran hydrogels. siRNA release is governed via the hydrolytic degradation of ester and/or disulfide linkages between the siRNA and hydrogels, which is independent of hydrogel degradation rate. The released siRNA is shown to be bioactive by inhibiting protein expression in green fluorescent protein–expressing HeLa cells without the need of a transfection agent. This strategy provides an excellent platform for controlling nucleic acid delivery through covalent bonds with a biomaterial and regulating cellular gene expression, which has promising potential in many biomedical applications.
机译:小干扰RNA(siRNA)在组织再生和疾病治疗中发现了许多应用。有效和局部的siRNA递送仍然具有挑战性,降低了其治疗潜力。在这里,我们报告了通过直接将具有转染能力的siRNA束缚到光交联的葡聚糖水凝胶来控制和延长siRNA释放的策略。 siRNA的释放取决于siRNA与水凝胶之间酯和/或二硫键的水解降解,而水解降解与水凝胶的降解速率无关。通过抑制表达绿色荧光蛋白的HeLa细胞中的蛋白表达而无需转染剂,表明释放的siRNA具有生物活性。该策略提供了一个极好的平台,可通过与生物材料的共价键控制核酸的传递并调节细胞基因的表达,这在许多生物医学应用中都具有广阔的前景。

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