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Monovalent cation effects on intermolecular purine-purine-pyrimidine triple-helix formation.

机译:单价阳离子对分子间嘌呤-嘌呤-嘧啶三螺旋形成的影响。

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摘要

The binding of a 19-mer guanosine-rich oligodeoxyribonucleotide, TG3TG4TG4TG3T (ODN 1), to a complementary polypurine DNA target was investigated by DNase I footprinting and restriction endonuclease protection assays. Monovalent cations inhibited intermolecular purine-purine-pyrimidine triple-helical DNA formation, with K+ and Rb+ being most effective, followed by NH4+ and Na+. Li+ and Cs+ had little to no effect. Similar results were observed with the G/A-rich oligonucleotide AG3AG4AG4AG3AGCT. Kinetic studies indicated that monovalent cations interfered with oligonucleotide-duplex DNA association but did not significantly promote triplex dissociation. The observed order of monovalent cation inhibition of triplex formation is reminiscent of their effect on tetraplex formation with G/T-rich oligonucleotides. However, using electrophoretic mobility shift assays we found that the oligonucleotide ODN 1 did not appear to form a four-stranded species under conditions promoting tetraplex formation. Taken together, our data suggest that processes other than the self-association of oligonucleotides into tetraplexes might be involved in the inhibitory effect of monovalent cations on purine-pyrimidine-purine triplex formation.
机译:通过DNase I足迹法和限制性内切核酸酶保护试验,研究了富含19-mer鸟苷的寡脱氧核糖核苷酸TG3TG4TG4TG3T(ODN 1)与互补性嘌呤DNA靶标的结合。单价阳离子抑制分子间嘌呤-嘌呤-嘧啶三螺旋DNA的形成,其中K +和Rb +最有效,其次是NH4 +和Na +。 Li +和Cs +几乎没有影响。用富含G / A的寡核苷酸AG3AG4AG4AG3AGCT观察到相似的结果。动力学研究表明,单价阳离子干扰寡核苷酸-双链DNA缔合,但不会显着促进三链体解离。观察到的对三链体形成的单价阳离子抑制的顺序让人想起它们对富含G / T的寡核苷酸对四链体形成的影响。但是,使用电泳迁移率变动分析,我们发现寡核苷酸ODN 1在促进四重体形成的条件下似乎未形成四链物质。两者合计,我们的数据表明,寡核苷酸自缔合成四链体以外的过程可能与单价阳离子对嘌呤-嘧啶-嘌呤三联体形成的抑制作用有关。

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  • 作者

    Cheng, A J; Van Dyke, M W;

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  • 年度 1993
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  • 原文格式 PDF
  • 正文语种 en
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