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Suppression of microRNAs by dual-targeting and clustered Tough Decoy inhibitors

机译:通过双重靶向和成簇的Tough Decoy抑制剂抑制microRNA

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摘要

MicroRNAs (miRNAs) are ubiquitous regulators of gene expression that contribute to almost any cellular process. Methods for managing of miRNA activity are attracting increasing attention in relation to diverse experimental and therapeutic applications. DNA-encoded miRNA inhibitors expressed from plasmid or virus-based vectors provide persistent miRNA suppression and options of tissue-directed micromanaging. In this report, we explore the potential of exploiting short, hairpin-shaped RNAs for simultaneous suppression of two or more miRNAs. Based on the “Tough Decoy” (TuD) design, we create dual-targeting hairpins carrying two miRNA recognition sites and demonstrate potent co-suppression of different pairs of unrelated miRNAs by a single DNA-encoded inhibitor RNA. In addition, enhanced miRNA suppression is achieved by expression of RNA polymerase II-transcribed inhibitors carrying clustered TuD hairpins with up to a total of eight miRNA recognition sites. Notably, by expressing clustered TuD inhibitors harboring a single recognition site for each of a total of six miRNAs, we document robust parallel suppression of multiple miRNAs by inhibitor RNA molecules encoded by a single expression cassette. These findings unveil a new potential of TuD-based miRNA inhibitors and pave the way for standardizing synchronized suppression of families or clusters of miRNAs.
机译:MicroRNA(miRNA)是普遍存在的基因表达调节剂,几乎参与任何细胞过程。与各种实验和治疗应用相关的miRNA活性管理方法正引起越来越多的关注。从质粒或基于病毒的载体表达的DNA编码的miRNA抑制剂可提供持续的miRNA抑制作用,并提供组织定向的微管理选项。在本报告中,我们探索了利用短发夹状RNA同时抑制两个或多个miRNA的潜力。基于“强诱饵”(TuD)设计,我们创建了带有两个miRNA识别位点的双靶发夹,并通过单个DNA编码的抑制剂RNA证明了不同对互不相关的miRNA的有效共抑制。另外,通过表达带有簇状TuD发夹的RNA聚合酶II转录的抑制剂来实现增强的miRNA抑制,簇状TuD发夹具有多达八个miRNA识别位点。值得注意的是,通过表达对总共六个miRNA的每个都具有单个识别位点的簇状TuD抑制剂,我们记录了由单个表达盒编码的抑制剂RNA分子对多个miRNA的稳健平行抑制。这些发现揭示了基于TuD的miRNA抑制剂的新潜力,并为标准化同步抑制miRNA家族或簇的方式铺平了道路。

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