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Rational Design of Therapeutic siRNAs: Minimizing Off-targeting Potential to Improve the Safety of RNAi Therapy for Huntingtons Disease

机译:合理设计治疗性siRNA:最小化脱靶潜能提高针对亨廷顿氏病的RNAi治疗的安全性

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摘要

RNA interference (RNAi) provides an approach for the treatment of many human diseases. However, the safety of RNAi-based therapies can be hampered by the ability of small inhibitory RNAs (siRNAs) to bind to unintended mRNAs and reduce their expression, an effect known as off-target gene silencing. Off-targeting primarily occurs when the seed region (nucleotides 2–8 of the small RNA) pairs with sequences in 3′-UTRs of unintended mRNAs and directs translational repression and destabilization of those transcripts. To date, most therapeutic RNAi sequences are selected primarily for gene silencing efficacy, and later evaluated for safety. Here, in designing siRNAs to treat Huntington's disease (HD), a dominant neurodegenerative disorder, we prioritized selection of sequences with minimal off-targeting potentials (i.e., those with a scarcity of seed complements within all known human 3′-UTRs). We identified new promising therapeutic candidate sequences which show potent silencing in cell culture and mouse brain. Furthermore, we present microarray data demonstrating that off-targeting is significantly minimized by using siRNAs that contain “safe” seeds, an important strategy to consider during preclinical development of RNAi-based therapeutics.
机译:RNA干扰(RNAi)提供了一种治疗许多人类疾病的方法。但是,基于RNAi的疗法的安全性可能会受到小抑制性RNA(siRNA)与意外mRNA结合并降低其表达的能力的阻碍,这种作用称为脱靶基因沉默。脱靶主要发生在种子区域(小RNA的2-8核苷酸)与意外mRNA的3'-UTR中的序列配对并指导这些转录物的翻译抑制和不稳定时。迄今为止,大多数治疗性RNAi序列的选择主要是为了提高基因沉默的效率,然后评估其安全性。在这里,在设计治疗显性神经退行性疾病亨廷顿氏病(HD)的siRNA时,我们优先选择了脱靶潜能最小的序列(即在所有已知的人类3'-UTR中缺乏种子补体的序列)。我们确定了新的有前途的治疗候选序列,该序列在细胞培养和小鼠脑中显示出有效的沉默。此外,我们目前提供的微阵列数据表明,通过使用含有“安全”种子的siRNA,可以大大降低脱靶的可能性,这是在基于RNAi的疗法的临床前开发过程中要考虑的重要策略。

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