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含有非锁定碱基类似物的 siRNA 可提高基因沉默的特异性。

Improved specificity of gene silencing by siRNAs containing unlocked nucleobase analogs.

机构信息

Marina Biotech Inc., 3830 Monte Villa Parkway, Bothell, WA 98021, USA.

出版信息

Nucleic Acids Res. 2011 Mar;39(5):1823-32. doi: 10.1093/nar/gkq961. Epub 2010 Nov 2.

Abstract

siRNAs confer sequence specific and robust silencing of mRNA. By virtue of these properties, siRNAs have become therapeutic candidates for disease intervention. However, their use as therapeutic agents can be hampered by unintended off-target effects by either or both strands of the siRNA duplex. We report here that unlocked nucleobase analogs (UNAs) confer desirable properties to siRNAs. Addition of a single UNA at the 5'-terminus of the passenger strand blocks participation of the passenger strand in RISC-mediated target down-regulation with a concomitant increase in guide strand activity. Placement of a UNA in the seed region of the guide strand prevents miRNA-like off-target silencing without compromising siRNA activity. Most significantly, combined substitution of UNA at the 3'-termini of both strands, the addition of a UNA at the 5'-terminus of the passenger strand, and a single UNA in the seed region of the guide strand, reduced the global off-target events by more than 10-fold compared to unmodified siRNA. The reduction in off-target events was specific to UNA placement in the siRNA, with no apparent new off-target events. Taken together, these results indicate that when strategically placed, UNA substitutions have important implications for the design of safe and effective siRNA-based therapeutics.

摘要

siRNAs 赋予 mRNA 序列特异性和强大的沉默作用。由于这些特性,siRNAs 已成为疾病干预的治疗候选物。然而,siRNA 双链体的任一条链都可能产生非靶向效应,从而阻碍其作为治疗剂的应用。我们在此报告称,未锁定碱基类似物 (UNAs) 可为 siRNA 赋予理想的特性。在过客链的 5' 末端添加单个 UNA 会阻止过客链参与 RISC 介导的靶向下调节,同时增加引导链的活性。在引导链的种子区域放置 UNA 可防止 miRNA 样的非靶向沉默,而不会影响 siRNA 的活性。最重要的是,与未修饰的 siRNA 相比,在两条链的 3' 末端联合替换 UNA、在过客链的 5' 末端添加 UNA 以及在引导链的种子区域添加单个 UNA,可将全局非靶向事件减少 10 倍以上。非靶向事件的减少是 UNA 在 siRNA 中的位置特异性的,没有明显的新的非靶向事件。总之,这些结果表明,当策略性地放置时,UNA 取代对安全有效的基于 siRNA 的治疗剂的设计具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/984d/3061082/c0b515536f13/gkq961f1.jpg

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