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首页> 外文期刊>Molecules >Modulation of the RNA Interference Activity Using Central Mismatched siRNAs and Acyclic Threoninol Nucleic Acids (aTNA) Units
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Modulation of the RNA Interference Activity Using Central Mismatched siRNAs and Acyclic Threoninol Nucleic Acids (aTNA) Units

机译:使用中央错配的siRNA和无环苏氨酸核酸(aTNA)单元对RNA干扰活性的调节

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摘要

The understanding of the mechanisms behind nucleotide recognition by Argonaute 2, core protein of the RNA-induced silencing complex, is a key aspect in the optimization of small interfering RNAs (siRNAs) activity. To date, great efforts have been focused on the modification of certain regions of siRNA, such as the 3'/5'-termini and the seed region. Only a few reports have described the roles of central positions flanking the cleavage site during the silence process. In this study, we investigate the potential correlations between the thermodynamic and silencing properties of siRNA molecules carrying, at internal positions, an acyclic L-threoninol nucleic acid (aTNA) modification. Depending on position, the silencing is weakened or impaired. Furthermore, we evaluate the contribution of mismatches facing either a natural nucleotide or an aTNA modification to the siRNA potency. The position 11 of the antisense strand is more permissive to mismatches and aTNA modification, in respect to the position 10. Additionally, comparing the ON-/OFF-target silencing of central mismatched siRNAs with 5'-terminal modified siRNA, we concluded: (i) central perturbation of duplex pairing features weights more on potency rather than silencing asymmetry; (ii) complete bias for the ON-target silencing can be achieved with single L-threoninol modification near the 5'-end of the sense strand.
机译:对RNA诱导的沉默复合物的核心蛋白Argonaute 2进行核苷酸识别的机理的了解,是优化小干扰RNA(siRNA)活性的关键方面。迄今为止,已经将很大的努力集中在siRNA的某些区域的修饰上,例如3'/ 5'-末端和种子区域。只有少数报告描述了在沉默过程中位于裂解位点两侧的中心位置的作用。在这项研究中,我们研究了在内部位置携带无环L-苏氨酸核酸(aTNA)修饰的siRNA分子的热力学和沉默特性之间的潜在相关性。根据位置的不同,静音会减弱或减弱。此外,我们评估面对天然核苷酸或aTNA修饰的错配对siRNA效能的贡献。与位置10相比,反义链的位置11更容许错配和aTNA修饰。此外,比较中央错配siRNA与5'末端修饰siRNA的ON / OFF靶沉默,我们得出以下结论:( i)双工配对的中心扰动的特征是权重更多,而不是沉默不对称; (ii)可以通过在有义链的5'末端附近进行单次L-苏氨酸修饰来实现对靶标沉默的完全偏倚。

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