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Targeting Repeated Regions Unique to a Gene Is an Effective Strategy for Discovering Potent and Efficacious Antisense Oligonucleotides

机译:针对基因独特的重复区域是发现有效而有效的反义寡核苷酸的有效策略

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摘要

Well-validated strategies for discovering potent and efficacious antisense oligonucleotides are central to realize the full therapeutic potential of RNA therapy. In this study, we focus on RNA targets where the same sequence of 16–20 nt is found in several regions across the RNA, and not in any other RNA. Targeting such unique repeated regions with oligonucleotides designed as gapmers and capable of recruiting RNase H has previously been proposed as a strategy for identifying potent gapmers. By sequence analysis of the human and monkey transcriptomes, we find that such unique repeated regions in RNA are often conserved between humans and monkeys, which allow pharmacodynamic effects to be evaluated in non-human primates before testing in humans. For eight potential RNA targets chosen in an unbiased fashion, we targeted their unique repeated regions with locked nucleic acid (LNA)-modified gapmers, and for six of them we identified gapmers that were significantly more potent and efficacious than non-repeat-targeting gapmer controls. We suggest a stochastic model for repeat-targeting gapmers that explains all effects observed so far and can help guide future work. Our results support the targeting of repeated regions as an effective strategy for discovering gapmer antisense oligonucleotides suitable for therapeutic development.
机译:发现有效而有效的反义寡核苷酸的有效策略对实现RNA治疗的全部治疗潜力至关重要。在这项研究中,我们专注于RNA靶标,在整个RNA的多个区域中发现了相同的16-20 nt序列,而在其他任何RNA中却没有。先前已经提出了用设计为gapmer并能够募集RNase H的寡核苷酸靶向这种独特的重复区域作为鉴定有效gapmer的策略。通过对人和猴转录组的序列分析,我们发现RNA的这种独特重复区域通常在人和猴之间是保守的,这允许在非人灵长类动物中进行药效学评估,然后在人中进行测试。对于以不偏不倚的方式选择的八个潜在RNA靶标,我们将其锁定的核酸(LNA)修饰的间隔物靶向了其独特的重复区域,对于其中的六个,我们确定了与非重复靶向间隔物相比更有效,更有效的间隔物控件。我们建议针对重复定位空位器的随机模型,该模型可以解释到目前为止观察到的所有效应,并且可以帮助指导未来的工作。我们的结果支持针对重复区域的靶向,作为发现适合于治疗性开发的gapmer反义寡核苷酸的有效策略。

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