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首页> 外文期刊>Nucleic Acids Research >Probing alternative foldings of the HIV-1 leader RNA by antisense oligonucleotide scanning arrays
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Probing alternative foldings of the HIV-1 leader RNA by antisense oligonucleotide scanning arrays

机译:通过反义寡核苷酸扫描阵列探索HIV-1前导RNA的其他折叠

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摘要

Scanning arrays of antisense DNA oligonucleotides provide a novel and systematic means to study structural features within an RNA molecule. We used this approach to probe the structure of the untranslated leader of the human immunodeficiency virus type 1 (HIV-1) RNA genome. This 335 nt RNA encodes multiple important replication signals and adopts two mutually exclusive conformations. The poly(A) and the dimer initiation signal (DIS) sequences of the leader RNA are base-paired in the long-distance interaction (LDI) conformation, but both domains form distinct hairpins in the branched multiple hairpins (BMH) conformation. An RNA switch mechanism has been proposed to regulate the activity of the DIS dimerization signal that is masked in one, yet exposed in the other conformation. The two RNA conformations demonstrate discrete differences in the array-based hybridization patterns. LDI shows increased hybridization in the poly(A) region and decreased hybridization in the DIS region when compared with BMH. These results provide additional evidence for the structure models of the two alternative leader RNA conformations. We also found a correlation between the efficiency of oligonucleotide hybridization and the accessibility of the RNA structure as determined by chemical and enzymatic probing in previous studies. The array approach therefore provides a very sensitive method to detect structural differences in related transcripts.
机译:反义DNA寡核苷酸的扫描阵列提供了一种新颖而系统的方法来研究RNA分子内的结构特征。我们使用这种方法来探测人类免疫缺陷病毒1型(HIV-1)RNA基因组的非翻译前导的结构。该335 nt RNA编码多个重要的复制信号,并采用两个互斥的构象。前导RNA的poly(A)和二聚体起始信号(DIS)序列在长距离相互作用(LDI)构象中是碱基配对的,但是两个结构域在分支的多个发夹(BMH)构象中形成不同的发夹。已经提出了一种RNA开关机制来调节DIS二聚化信号的活性,所述DIS二聚化信号被一个掩蔽,但是以另一个构象暴露。这两个RNA构象表明基于阵列的杂交模式中的离散差异。与BMH相比,LDI在poly(A)区域显示增加的杂交,在DIS区域显示减少的杂交。这些结果为两个替代的前导RNA构象的结构模型提供了额外的证据。我们还发现寡核苷酸杂交的效率与RNA结构的可及性之间存在相关性,这在先前的研究中已通过化学和酶促探测确定。因此,阵列方法提供了一种非常敏感的方法来检测相关转录本中的结构差异。

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