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High-throughput sequence analysis reveals structural diversity and improved potency among RNA inhibitors of HIV reverse transcriptase

机译:高通量序列分析揭示了HIV逆转录酶RNA抑制剂之间的结构多样性和更高的效力

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摘要

Systematic evolution of ligands through exponential enrichment (SELEX) is a well-established method for generating nucleic acid populations that are enriched for specified functions. High-throughput sequencing (HTS) enhances the power of comparative sequence analysis to reveal details of how RNAs within these populations recognize their targets. We used HTS analysis to evaluate RNA populations selected to bind type I human immunodeficiency virus reverse transcriptase (RT). The populations are enriched in RNAs of independent lineages that converge on shared motifs and in clusters of RNAs with nearly identical sequences that share common ancestry. Both of these features informed inferences of the secondary structures of enriched RNAs, their minimal structural requirements and their stabilities in RT-aptamer complexes. Monitoring population dynamics in response to increasing selection pressure revealed RNA inhibitors of RT that are more potent than the previously identified pseudoknots. Improved potency was observed for inhibition of both purified RT in enzymatic assays and viral replication in cell-based assays. Structural and functional details of converged motifs that are obscured by simple consensus descriptions are also revealed by the HTS analysis. The approach presented here can readily be generalized for the efficient and systematic post-SELEX development of aptamers for down-stream applications.
机译:通过指数富集(SELEX)进行配体的系统进化是一种成熟的方法,用于生成针对特定功能富集的核酸群体。高通量测序(HTS)增强了比较序列分析的功能,以揭示这些群体中RNA如何识别其靶标的细节。我们使用HTS分析来评估选择结合I型人类免疫缺陷病毒逆转录酶(RT)的RNA种群。种群中富集了独立谱系的RNA,这些RNA聚集在共享的基序上,并且聚集在具有几乎相同序列且共享共同祖先的RNA簇中。这两个功能有助于推断出富集RNA的二级结构,其最低限度的结构要求以及它们在RT-适体复合物中的稳定性。监测响应选择压力增加的种群动态,发现RT的RNA抑制剂比先前鉴定的假结更有效。在酶法测定中抑制纯化的RT和在基于细胞的测定中抑制病毒复制均观察到增强的效力。 HTS分析还揭示了被简单的共识描述所掩盖的聚合基序的结构和功能细节。此处介绍的方法可以很容易地推广到SELEX后高效,系统的下游适配体开发中。

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