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Structural variations and stabilising modifications of synthetic siRNAs in mammalian cells

机译:哺乳动物细胞中合成siRNA的结构变异和稳定修饰

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Double-stranded short interfering RNAs (siRNA) induce post-transcriptional silencing in a variety of biological systems. In the present study we have investigated the structural requirements of chemically synthesised siRNAs to mediate efficient gene silencing in mammalian cells. In contrast to studies with Drosophila extracts, we found that synthetic, double-stranded siRNAs without specific nucleotide overhangs are highly efficient in gene silencing. Blocking of the 5'-hydroxyl terminus of the antisense strand leads to a dramatic loss of RNA interference activity, whereas blocking of the 3' terminus or blocking of the termini of the sense strand had no negative effect. We further demonstrate that synthetic siRNA molecules with internal 2'-O-methyl modification, but not molecules with terminal modifications, are protected against serum-derived nucleases. Finally, we analysed different sets of siRNA molecules with various 2'-O-methyl modifications for stability and activity. We demonstrate that 2'-O-methyl modifications at specific positions in the molecule improve stability of siRNAs in serum and are tolerated without significant loss of RNA interference activity. These second generation siRNAs will be better suited for potential therapeutic application of synthetic siRNAs in vivo.
机译:双链短干扰RNA(siRNA)在多种生物系统中诱导转录后沉默。在本研究中,我们研究了化学合成的siRNA介导哺乳动物细胞中有效基因沉默的结构要求。与果蝇提取物的研究相反,我们发现没有特定核苷酸突出端的合成双链siRNA在基因沉默中非常有效。反义链的5'-羟基末端的封闭导致RNA干扰活性的显着丧失,而3'末端的封闭或有义链的末端的封闭没有负面影响。我们进一步证明,具有内部2'-O-甲基修饰的合成siRNA分子(而不是具有末端修饰的分子)具有针对血清来源的核酸酶的保护作用。最后,我们分析了具有各种2'-O-甲基修饰的不同组的siRNA分子的稳定性和活性。我们证明了在分子中特定位置的2'-O-甲基修饰可提高血清中siRNA的稳定性,并且可以耐受而不会显着降低RNA干扰活性。这些第二代siRNA将更适合合成siRNA在体内的潜在治疗应用。

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