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Circular RNA oligonucleotides. Synthesis, nucleic acid binding properties, and a comparison with circular DNAs

机译:环状RNA寡核苷酸。合成,核酸结合特性以及与环状DNA的比较

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We report the synthesis and nucleic acid binding properties of two cyclic RNA oligonucleotides designed to bind single-stranded nucleic acids by pyr·pur·pyr-type triple helix formation. The circular RNAs are 34 nucleotides in size and were cyclized using a template-directed nonenzymatic ligation. To ensure isomeric 3′-5′ purity in the ligation reaction, one nucleotide at the ligation site is a 2′-deoxyribose. One circle (1) is complementary to the sequence 5′-A12, and the second (2) is complementary to 5′-AAGAAAGAAAAG. Results of thermal denaturation experiments and mixing studies show that both circles bind complementary single-stranded DNA or RNA substrates by triple helix formation, in which two domains in a pyrimidine-rich circle sandwich a central purine-rich substrate. The affinities of these circles with their purine complements are much higher than the affinities of either the linear precursors or simple Watson-Crick DNA complements. For example, circle 1 binds rA12 (pH 7.0, 10 mM MgCl2, 100 mM NaCl) with a Tm of 48°C and a Kd (37°C) of 4.1 × 10?9 M, while the linear precursor of the circle binds with a Tm of 34°C and a Kd of 1.2 × 10?6 M. The complexes of circle 2 are pH-dependent, as expected for triple helical complexes involving C(+)G·C triads, and mixing plots for both circles reveal one-to-one stoichiometry of binding either to RNA or DNA substrates. Comparison of circular RNAs with previously synthesized circular DNA oligonucleotides of the same sequence reveals similar behavior in the binding of DNA, but strikingly different behavior in the binding of RNA. The cyclic DNAs show high DNA-binding selectivity, giving relatively weaker duplex-type binding with complementary RNAs. The relative order of thermodynamic stability for the four types of triplex studied here is found to be DDD RRR RDR DRD. The results are discussed in the context of recent reports of strong triplex dependence on RNA versus DNA backbones. Triplex-forming circular RNAs represent a novel and potentially useful strategy for high-affinity binding of RNA.
机译:我们报告了两个环状RNA寡核苷酸的合成和核酸结合特性,这两个环状RNA寡核苷酸旨在通过pyr·pur·pyr型三重螺旋的形成结合单链核酸。环状RNA的大小为34个核苷酸,并使用模板指导的非酶连接进行环化。为了确保连接反应中的异构体3'-5'的纯度,在连接位点的一个核苷酸是2'-脱氧核糖。一个圆(1)与序列5'-A 12 互补,第二个圆(2)与5'-AAGAAAGAAAAG互补。热变性实验和混合研究的结果表明,两个圆圈均通过三螺旋形成结合互补的单链DNA或RNA底物,其中,富含嘧啶的圆圈中的两个域夹着富含嘌呤的中央底物。这些圆与嘌呤补体的亲和力远高于线性前体或简单的Watson-Crick DNA补体的亲和力。例如,圆1以48°C的T m 结合rA 12 (pH 7.0、10 mM MgCl 2 ,100 mM NaCl)。且K d (37°C)为4.1×10 ?9 M,而圆的线性前体与T m 结合环温度为34°C,K d 为1.2×10 ?6 M。圆2的配合物是pH依赖的,如涉及C(+ G·C三联体,以及两个圆圈的混合图显示了与RNA或DNA底物结合的一对一化学计量。将环状RNA与先前合成的相同序列的环状DNA寡核苷酸进行比较,发现在DNA结合中的行为相似,但在RNA结合中的行为却截然不同。环状DNA显示出高的DNA结合选择性,与互补RNA的双链型结合相对较弱。此处研究的四种三元组的热力学稳定性的相对顺序为DDD RRR> RDR DRD。在有关RNA与DNA骨架对RNA的三重依赖的最新报道的背景下讨论了结果。形成三链体的环状RNA代表了RNA高亲和力结合的一种新颖且潜在有用的策略。

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