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A simple, noninvasive and efficient method for transdermal delivery of siRNA

机译:一种简单,无创且有效的siRNA透皮递送方法

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Effective delivery of therapeutic agents is the most challenging hurdle in the use of RNA interference for research and in the clinic. Here, we assessed whether a short synthetic peptide, ACSSSPSKHCG (TD-1), could be transported through rat footpad (follicle-free) skin and efficiently deliver small interfering RNA (siRNA) to knock down a target gene. Fluorescence microscopy revealed that topical co-administration of FITC-labeled TD-1 and FAM-labeled siRNA distributed uniformly from the epidermis to the subcutaneous tissue of rat footpad skin. Transmission electron microscopy revealed the absence of cell–cell junctions and enlarged spaces between epithelial cells in the TD-1-treated footpad skin. TD-1 delivery of anti-GAPDH siRNA significantly reduced the level of GAPDH in 72 h. TD-1 can create a transient opening in non-follicle rat skin for delivery of siRNA and reveal a novel mechanism of transdermal delivery of TD-1 and siRNA into the epidermis for gene knockdown. The system might have potential for siRNA delivery in skin for drug therapy.
机译:在研究和临床中使用RNA干扰时,有效地输送治疗剂是最具挑战性的障碍。在这里,我们评估了短合成肽ACSSSPSKHCG(TD-1)是否可以通过大鼠足垫(无卵泡)皮肤运输并有效地递送小干扰RNA(siRNA)来敲低靶基因。荧光显微镜显示,FITC标记的TD-1和FAM标记的siRNA的局部共同给药从表皮到大鼠足垫皮肤的皮下组织均匀分布。透射电子显微镜显示在经TD-1处理的脚垫皮肤中,没有细胞间连接,上皮细胞之间的空间增大。 TD-1的抗GAPDH siRNA在72小时内显着降低了GAPDH的水平。 TD-1可以在非滤泡大鼠皮肤中产​​生一个短暂的开口以传递siRNA,并揭示了TD-1和siRNA透皮传递到表皮中以进行基因敲除的新机制。该系统可能具有将siRNA递送至皮肤进行药物治疗的潜力。

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