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短序列指数富集配体系统(SELEX)RNA 适体文库观察到的核苷酸偏性。

Nucleotide bias observed with a short SELEX RNA aptamer library.

机构信息

Department of Internal Medicine, University of Iowa, Iowa City, IA 52242, USA.

出版信息

Nucleic Acid Ther. 2011 Aug;21(4):253-63. doi: 10.1089/nat.2011.0288. Epub 2011 Jun 28.

Abstract

Systematic evolution of ligands by exponential enrichment (SELEX) is a powerful in vitro selection process used for over 2 decades to identify oligonucleotide sequences (aptamers) with desired properties (usually high affinity for a protein target) from randomized nucleic acid libraries. In the case of RNA aptamers, several highly complex RNA libraries have been described with RNA sequences ranging from 71 to 81 nucleotides (nt) in length. In this study, we used high-throughput sequencing combined with bioinformatics analysis to thoroughly examine the nucleotide composition of the sequence pools derived from several selections that employed an RNA library (Sel2N20) with an abbreviated variable region. The Sel2N20 yields RNAs 51 nt in length, which unlike longer RNAs, are more amenable to large-scale chemical synthesis for therapeutic development. Our analysis revealed a consistent and early bias against inclusion of adenine, resulting in aptamers with lower predicted minimum free energies (ΔG) (higher structural stability). This bias was also observed in control, "nontargeted" selections in which the partition step (against the target) was omitted, suggesting that the bias occurred in 1 or more of the amplification and propagation steps of the SELEX process.

摘要

系统进化的配体指数富集(SELEX)是一种强大的体外选择过程,已经使用了 20 多年,用于从随机核酸文库中鉴定具有所需特性(通常是对蛋白质靶标具有高亲和力)的寡核苷酸序列(适体)。在 RNA 适体的情况下,已经描述了几个高度复杂的 RNA 文库,其中 RNA 序列的长度从 71 到 81 个核苷酸(nt)不等。在这项研究中,我们使用高通量测序结合生物信息学分析,彻底检查了从几个使用缩短可变区的 RNA 文库(Sel2N20)进行的选择中获得的序列库的核苷酸组成。Sel2N20 产生 51 nt 长的 RNA,与较长的 RNA 不同,它更适合于大规模的化学合成,以用于治疗开发。我们的分析显示,对腺嘌呤的包含存在一致且早期的偏见,导致适体的预测最小自由能(ΔG)(更高的结构稳定性)降低。在没有靶标分离步骤的对照“非靶向”选择中也观察到了这种偏见,这表明这种偏见发生在 SELEX 过程的 1 个或多个扩增和繁殖步骤中。

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