首页> 外文期刊>Nucleic Acids Research >QUINAZOLINE-2,4(1H,3H)-DIONE AS A SUBSTITUTE FOR THYMINE IN TRIPLE-HELIX FORMING OLIGONUCLEOTIDES - A REASSESSMENT
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QUINAZOLINE-2,4(1H,3H)-DIONE AS A SUBSTITUTE FOR THYMINE IN TRIPLE-HELIX FORMING OLIGONUCLEOTIDES - A REASSESSMENT

机译:喹唑啉-2,4(1H,3H)-二酮替代三螺旋形成寡核苷酸中的胸腺嘧啶-重新评估

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摘要

A major limitation in triple-helix formation arises from the weak energy of interaction between the third strand and the double-stranded target, We tried to increase the stacking interaction contribution within the third strand by extending the aromatic domain of thymine, We report here the use of 2,4-quinazolinedione as a substitute for thymine in the canonical TA*T triplet, The synthesis and the characterization of the quinazoline beta nucleoside Q and of its phosphoramidite derivative is described, Triple-helix-forming oligonucleotides incorporating Q have been prepared and their ability to form triplexes has been evaluated by UV-monitored thermal denaturation measurements, The introduction of one or multiple Q residues, either contiguous or remote from each other, slightly destabilized triple-stranded structures, whatever the nucleic acid base composition (pyrimidine or GT) of the third strand.
机译:第三螺旋形成的主要局限性在于第三链与双链靶之间相互作用的能量较弱,我们试图通过延伸胸腺嘧啶的芳族结构域来增加第三链内的堆叠相互作用。 2,4-喹唑啉二酮在常规TA * T三联体中作为胸腺嘧啶的替代品,描述了喹唑啉β核苷Q及其亚磷酰胺衍生物的合成和表征,制备了掺有Q的三螺旋形成寡核苷酸及其形成三链体的能力已通过UV监控的热变性测量进行了评估。引入一个或多个Q残基(彼此相邻或相距很远),不稳定的三链结构,无论核酸碱基组成是什么(嘧啶或GT)。

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