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首页> 外文期刊>FEBS Letters >Highly efficient gene silencing in mouse brain by overhanging‐duplex oligonucleotides via intraventricular route
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Highly efficient gene silencing in mouse brain by overhanging‐duplex oligonucleotides via intraventricular route

机译:通过静脉内途径通过悬垂双相寡核苷酸在小鼠脑中高效基因沉默

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Gapmer‐type antisense oligonucleotides have not yet been approved for the treatment of central nervous system diseases, whereas steric‐blocking‐type antisense oligonucleotides have been well‐developed for clinical use. We here characterize a new type of double‐stranded oligonucleotides, overhanging‐duplex oligonucleotides, which are composed of the parent gapmer and its extended complementary RNA. By intracerebroventricular injection, overhanging oligonucleotides show greater silencing potency with more efficient delivery into mouse brains than the parent single‐stranded gapmer. Structure–activity relationship analyses reveal that the potency enhancement requires 13‐mer or more overhanging oligonucleotides with a phosphorothioate backbone. Overhanging oligonucleotides provide a new platform of therapeutic oligonucleotides for gene modulation in the central nervous system.
机译:Gapmer型反义寡核苷酸尚未批准用于治疗中枢神经系统疾病,而空间阻断型反义寡核苷酸对于临床用途是良好的。我们在这里表征了一种新型的双链寡核苷酸,悬垂 - 双链寡核苷酸,其由母gapmer及其扩展的互补RNA组成。通过颅内腔内注射,悬垂的寡核苷酸显示出更大的沉默效力,比母体单链间隙均更有效地输送到小鼠脑中。结构 - 活性关系分析表明,效力增强需要具有硫代磷酸盐骨架的13- MER或​​更多悬垂的寡核苷酸。悬垂的寡核苷酸提供了中枢神经系统中基因调制的治疗寡核苷酸的新平台。

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