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Synthesis and triplex-forming properties of cyclic oligonucleotides with (G,A)-antiparallel strands

机译:具有(G,A)-反平行链的环状寡核苷酸的合成和三链体形成特性

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摘要

Cyclic oligonucleotides carrying an oligopurine Watson - Crick sequence linked to the corresponding (G,A)-and (G,T)-antiparallel strands were prepared by nonenzymatic template-assisted cyclization of phosphorylated precursors. Cyclization was attempted using 3′-phosphate and 5′-phosphate linear precursors with carbodiimide or BrCN activation. The best results were obtained with the 5′-phosphorylated precursors and carbodiimide activation. Cyclic oligonucleotides bind polypyrimidine target sequence by formation of antiparallel triplexes. We have used UV and circular dichroism (CD) spectroscopy to analyze triplexes formed by cyclic oligonucleotides carrying G and A in the reverse-Hoogsteen strand. The relative stability of the triplexes formed by cyclic and linear oligonucleotides with a common polypyrimidine target was determined by melting experiments. The most-stable triplexes were formed by the cyclic oligonucleotide, followed by the unphosphorylated and phosphorylated oligonucleotide precursors, and, finally, the corresponding hairpin. Although the differences in binding affinity between cyclic oligonucleotides and their corresponding linear precursors are small, the use of cyclic oligonucleotides offers a clear advantage over conventional duplex recognition.
机译:通过非酶模板辅助磷酸化前体的环化反应,制备带有连接至相应的(G,A)和(G,T)-反平行链的寡嘌呤Watson-Crick序列的环状寡核苷酸。尝试使用具有碳二亚胺或BrCN活化作用的3'-磷酸盐和5'-磷酸盐线性前体进行环化。 5'-磷酸化的前体和碳二亚胺活化获得了最佳结果。环状寡核苷酸通过形成反平行三链体结合聚嘧啶靶序列。我们已经使用紫外线和圆二色性(CD)光谱来分析由反向Hoogsteen链中带有G和A的环状寡核苷酸形成的三链体。通过熔解实验确定由具有共同的聚嘧啶靶的环状和线性寡核苷酸形成的三链体的相对稳定性。环状寡核苷酸形成最稳定的三链体,然后是未磷酸化和磷酸化的寡核苷酸前体,最后是相应的发夹。尽管环状寡核苷酸及其相应的线性前体之间的结合亲和力差异很小,但是环状寡核苷酸的使用提供了优于常规双链识别的明显优势。

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