首页> 美国卫生研究院文献>Nucleic Acids Research >The binding of an antisense oligonucleotide to a hairpin structure via triplex formation inhibits chemical and biological reactions.
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The binding of an antisense oligonucleotide to a hairpin structure via triplex formation inhibits chemical and biological reactions.

机译:反义寡核苷酸通过三链体形成与发夹结构的结合抑制了化学和生物反应。

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摘要

We have investigated the binding of a 26-mer antisense oligodeoxynucleotide to a 69-mer DNA hairpin with a 13 base pair stem, bearing an Rsa1 restriction site. The 5' part of the 26-mer annealed to a stretch of six purines at the bottom of the hairpin. The 3' part was designed to fold back to form a triplex with both the stem of the hairpin and with the sequence paired to its own 5' region. Using non-denaturing polyacrylamide gel electrophoresis, melting curves (Tm) and chemical footprinting, we were able to show the formation of a 'double-hairpin' complex between the 69-mer and the 26-mer antisense oligopyrimidines. The association was both sequence and pH-dependent. The formation of a double hairpin complex was shown to prevent the alkylation of the 69-mer DNA target by an oligonucleotide-nitrogen mustard conjugate and to selectively inhibit the action of Rsa1.
机译:我们已经研究了26-mer反义寡脱氧核苷酸与带有13个碱基对的茎,带有Rsa1限制性位点的69-mer DNA发夹的结合。 26-mer的5'部分在发夹底部退火成六个嘌呤。 3'部分设计成可向后折叠,与发夹的茎和序列配对至其自身5'区域的三链体形成。使用非变性聚丙烯酰胺凝胶电泳,熔解曲线(Tm)和化学足迹,我们能够显示69-mer和26-mer反义寡嘧啶之间形成的“双发夹”复合物。该关联是序列和pH依赖性的。已显示双发夹复合物的形成可防止寡核苷酸-氮芥子偶联物对69-mer DNA靶的烷基化并选择性抑制Rsa1的作用。

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