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ss-siRNAs allele selectively inhibit ataxin-3 expression: multiple mechanisms for an alternative gene silencing strategy

机译:ss-siRNAs等位基因选择性抑制ataxin-3的表达:替代基因沉默策略的多种机制

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Single-stranded silencing RNAs (ss-siRNAs) provide an alternative approach to gene silencing. ss-siRNAs combine the simplicity and favorable biodistribution of antisense oligonucleotides with robust silencing through RNA interference (RNAi). Previous studies reported potent and allele-selective inhibition of human huntingtin expression by ss-siRNAs that target the expanded CAG repeats within the mutant allele. Mutant ataxin-3, the genetic cause of Machado–Joseph Disease, also contains an expanded CAG repeat. We demonstrate here that ss-siRNAs are allele-selective inhibitors of ataxin-3 expression and then redesign ss-siRNAs to optimize their selectivity. We find that both RNAi-related and non-RNAi-related mechanisms affect gene expression by either blocking translation or affecting alternative splicing. These results have four broad implications: (i) ss-siRNAs will not always behave similarly to analogous RNA duplexes; (ii) the sequences surrounding CAG repeats affect allele-selectivity of anti-CAG oligonucleotides; (iii) ss-siRNAs can function through multiple mechanisms and; and (iv) it is possible to use chemical modification to optimize ss-siRNA properties and improve their potential for drug discovery.
机译:单链沉默RNA(ss-siRNA)为基因沉默提供了另一种方法。 ss-siRNA将反义寡核苷酸的简单性和良好的生物分布与通过RNA干扰(RNAi)产生的强大沉默相结合。先前的研究报道,靶向突变等位基因中扩展的CAG重复序列的ss-siRNA对人类亨廷顿蛋白表达具有有效和等位基因选择性抑制作用。突变的共济失调蛋白3(Machado–Joseph Disease)的遗传原因,也包含扩展的CAG重复序列。我们在这里证明ss-siRNA是抗紫杉素3表达的等位基因选择性抑制剂,然后重新设计ss-siRNA以优化其选择性。我们发现RNAi相关和非RNAi相关的机制通过阻止翻译或影响替代剪接影响基因表达。这些结果具有四个广泛的含义:(i)ss-siRNA的行为不会总是类似于类似的RNA双链体; (ii)围绕CAG重复序列的序列影响抗CAG寡核苷酸的等位基因选择性; (iii)ss-siRNA可以通过多种机制发挥作用,并且; (iv)可以使用化学修饰来优化ss-siRNA特性并提高其发现药物的潜力。

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