Recent reports describe a new strategy for the binding of single-stranded pyrimidine sequences by triple helix formation. In this approach, a double-length purine-rich oligonucleotide binds a target strand, folding back to form an antiparallel pur pur pyr triple helix. We now describe a series of studies in which sequence and structural variations are made in such purine-rich llgands, in an effort to optimize binding properties. Comparison is made between the use of two separate strands and the use of single two-domain ligands; the latter are found to bind more tightly and to aggregate less in media containing Na+ or K+. Placement of mismatched bases in the target shows that sequence selectivity of binding is as high as that for Watson-Crick duplex formation. Variation of the lengths and sequences of loops bridging the binding domains demonstrates that dlnucleotide loops composed of pyrimidines give the highest stability. Oligoethylene glycol-derived loop replacements are shown to give good binding affinity as well. The binding of an RNA target is shown to occur with the same affinity as the binding of DNA. In general, it is found that circular variants bind more tightly than do either separate strands or singly-linked ligands and unlike linear oligomers, the circular compounds do not aggregate to a large extent even in buffers containing 100 mM K+. Such structurally optimized ligands are useful in expanding the number of possible naturally-occurring sequences which can be targeted by triplex formation.
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机译:最近的报道描述了通过三重螺旋形成结合单链嘧啶序列的新策略。在这种方法中,富含嘌呤的双倍长度的寡核苷酸结合靶链,折回以形成反平行的pur pur pur pyr三重螺旋。现在我们描述一系列研究,其中在这种富含嘌呤的配体中进行序列和结构变异,以优化结合性能。比较两条独立链的使用和单个二结构域配体的使用。发现后者在含有Na + 或K + 的介质中结合更紧密,聚集更少。靶中错配碱基的放置表明结合的序列选择性与Watson-Crick双链体形成的结合选择性一样高。桥接结合结构域的环的长度和序列的变化表明,由嘧啶组成的二核苷酸环具有最高的稳定性。寡聚乙二醇衍生的环替代物也显示出良好的结合亲和力。显示RNA靶标的结合以与DNA结合相同的亲和力发生。通常,发现环状变体与分离链或单链配体的结合更紧密,与线性低聚物不同,环状化合物即使在含有100 mM K + 。这种结构优化的配体可用于扩大可能由三链体形成靶向的天然序列的数量。
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