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8-Azaguanine Reporter of Purine lonization States in Structured RNAs

机译:结构化RNA中嘌呤离子化状态的8-氮鸟嘌呤报道分子

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摘要

The fluorescent nucleotide analogue 8-azaguanosine-5'-triphosphate (8azaGTP) is prepared easily by in vitro enzymatic synthesis methods. 8azaGTP is an efficient substrate for T7 RNA polymerase and is incorporated specifically opposite cytosine in the transcription template, as expected for a nucleobase analogue with the same Watson-Crick hydrogen bonding face as guanine. 8-Azaguanine (8azaG) in oligonucleotides also is recognized as guanine during ribonuclease T1 digestion. Moreover, replacement of guanine by 8azaG does not alter the melting temperature of base-paired RNAs significantly, evidence that 8azaG does not disrupt stacking and hydrogen bonding interactions. SazaGTP displays a high fluorescent quantum yield when the N1 position is deprotonated at high pH, but fluorescence intensity decreases significantly when N1 is protonated at neutral pH. Fluorescence is quenched 10-fold to 100-fold when 8azaG is incorporated into base-paired RNA and remains pH-dependent, although apparent pK_a values determined from the pH dependence of fluorescence intensity shift in the basic direction. Thus, 8azaG is a guanine analogue that does not perturb RNA structure and displays pH-dependent fluorescence that can be used to probe the ionization states of nucleobases in structured RNAs. A key application will be in determining the ionization state of active site nucleobases that have been implicated in the catalytic mechanisms of RNA enzymes.
机译:荧光核苷酸类似物8-氮杂鸟苷-5'-三磷酸酯(8azaGTP)可通过体外酶促合成方法轻松制备。 8azaGTP是T7 RNA聚合酶的有效底物,并在转录模板中特异地掺入了胞嘧啶,这与具有与鸟嘌呤相同的Watson-Crick氢键面的核碱基类似物一样。寡核苷酸中的8-氮鸟嘌呤(8azaG)在核糖核酸酶T1消化过程中也被识别为鸟嘌呤。此外,用8azaG取代鸟嘌呤不会显着改变碱基配对RNA的解链温度,这证明8azaG不会破坏堆叠和氢键相互作用。当在高pH下将N1位置去质子化时,SazaGTP显示出高荧光量子产率,但是当在中性pH下将N1质子化时,荧光强度显着降低。当将8azaG掺入碱基配对的RNA中时,荧光被淬灭10倍至100倍,并且保持pH依赖性,尽管根据荧光强度的pH依赖性确定的明显pK_a值沿基本方向移动。因此,8azaG是一种鸟嘌呤类似物,不会干扰RNA结构,并显示可用于探测结构化RNA中核碱基电离状态的pH依赖性荧光。关键应用将是确定已经参与RNA酶催化机制的活性位点核碱基的电离状态。

著录项

  • 来源
    《Journal of the American Chemical Society》 |2007年第11期|p.3426-3432|共7页
  • 作者单位

    Department of Molecular Biology and The Skaggs Institute for Chemical Biology, The Scripps Research Institute, 10550 North Torrey Pines Road, MB35, La Jolla, California 92037;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 化学;
  • 关键词

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