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首页> 外文期刊>The Journal of investigative dermatology. >Use of self-delivery siRNAs to inhibit gene expression in an organotypic pachyonychia congenita model.
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Use of self-delivery siRNAs to inhibit gene expression in an organotypic pachyonychia congenita model.

机译:使用自我传递siRNA抑制器官型先天性先天性模型中的基因表达。

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Although RNA interference offers therapeutic potential for treating skin disorders, delivery hurdles have hampered clinical translation. We have recently demonstrated that high pressure, resulting from intradermal injection of large liquid volumes, facilitated nucleic acid uptake by keratinocytes in mouse skin. Furthermore, similar intradermal injections of small interfering RNA (siRNA; TD101) into pachyonychia congenita (PC) patient foot lesions resulted in improvement. Unfortunately, the intense pain associated with hypodermic needle administration to PC lesions precludes this as a viable delivery option for this disorder. To investigate siRNA uptake by keratinocytes, an organotypic epidermal model, in which pre-existing endogenous gene or reporter gene expression can be readily monitored, was used to evaluate the effectiveness of "self-delivery" siRNA (i.e., siRNA chemically modified to enhance cellular uptake). In this model system, self-delivery siRNA treatment resulted in reduction of pre-existing fluorescent reporter gene expression under conditions in which unmodified controls had little or no effect. Additionally, treatment of PC epidermal equivalents with self-delivery "TD101" siRNA resulted in marked reduction of mutant keratin 6a mRNA with little or no effect on wild-type expression. These results indicate that chemical modification of siRNA may overcome certain limitations to transdermal delivery (specifically keratinocyte uptake) and may have clinical utility for inhibition of gene expression in the skin.
机译:尽管RNA干扰为治疗皮肤疾病提供了治疗潜力,但递送障碍阻碍了临床翻译。我们最近证明,皮内注射大量液体会导致高压,从而促进小鼠皮肤中角质形成细胞对核酸的吸收。此外,类似的皮内注射小干扰RNA(siRNA; TD101)到先天性后足(PC)患者足部病变中也可以改善病情。不幸的是,皮下注射针给PC病变带来的剧烈疼痛使这种疾病无法作为这种疾病的可行分娩选择。为了研究角质形成细胞对siRNA的摄取,可以使用有机型表皮模型(其中可以很容易地监测预先存在的内源基因或报告基因的表达)来评估“自我递送” siRNA(即经过化学修饰以增强细胞功能的siRNA)的有效性。摄取)。在此模型系统中,在未修饰的对照几乎没有影响或没有影响的条件下,自我传递siRNA处理导致先前存在的荧光报告基因表达减少。另外,用自送“ TD101” siRNA处理PC表皮等效物导致突变型角蛋白6a mRNA显着降低,而对野生型表达几乎没有影响。这些结果表明,对siRNA的化学修饰可以克服对透皮递送的某些限制(特别是对角质形成细胞的吸收),并且可能具有抑制皮肤中基因表达的临床用途。

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