Naked siLNA-mediated gene silencing of lung bronchoepithelium EGFP expression after intravenous administration.

Oligonucleotides Pub Date : 2009-06-01 DOI:10.1089/oli.2008.0175

Sys Zoffmann Glud, Jesper B Bramsen, Frederik Dagnaes-Hansen, Jesper Wengel, Kenneth Alan Howard, Jens R Nyengaard, Jørgen Kjems

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引用次数: 51

Abstract

The use of systemic siRNA therapeutics for RNA interference-mediated silencing of disease genes is limited by serum instability and inadequate biodistribution. We have previously reported on the EGFP gene silencing effect of chitosan/siRNA nanoparticles in the bronchoepithelium of mice lungs following intranasal delivery and improved serum stability and reduced off-targeting effects in vitro by incorporation of locked nucleic acid (LNA). In this study, we examine the pulmonary gene silencing effect of siLNAs targeting enhanced-green-fluorescent-protein (EGFP) in lung bronchoepithelium upon intravenous delivery of naked siLNAs and upon intranasal delivery of either naked siLNA or chitosan/siLNA nanoparticles. We show that naked siLNA administered intravenously efficiently reduces the EGFP protein expression. A similar effect is obtained with intranasal delivery of chitosan nanoparticles containing siLNA whereas intranasally instilled naked siLNA did not cause a knockdown.

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裸silna介导的静脉给药后肺支气管上皮EGFP表达的基因沉默。

系统性siRNA疗法用于RNA干扰介导的疾病基因沉默受到血清不稳定和不充分的生物分布的限制。我们之前报道了经鼻给药后壳聚糖/siRNA纳米颗粒在小鼠肺支气管上皮中的EGFP基因沉默作用，以及通过结合锁定核酸(LNA)改善血清稳定性和减少体外脱靶效应。在这项研究中，我们研究了靶向增强绿色荧光蛋白(EGFP)的siLNAs在静脉注射裸siLNA和鼻内注射裸siLNA或壳聚糖/siLNA纳米颗粒时在肺支气管上皮细胞中的肺基因沉默作用。我们发现，静脉注射裸siLNA可以有效降低EGFP蛋白的表达。鼻内递送含有siLNA的壳聚糖纳米颗粒获得了类似的效果，而鼻内灌注裸siLNA不会引起敲除。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Oligonucleotides 生物-生化与分子生物学

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>12 weeks