首页> 外文期刊>Chembiochem: A European journal of chemical biology >2-Methoxypyridine as a Thymidine Mimic in Watson-Crick Base Pairs of DNA and PNA: Synthesis, Thermal Stability, and NMR Structural Studies
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2-Methoxypyridine as a Thymidine Mimic in Watson-Crick Base Pairs of DNA and PNA: Synthesis, Thermal Stability, and NMR Structural Studies

机译:2-甲氧基吡啶作为胸苷模仿Watson-Crick碱基对DNA和PNA:合成,热稳定性和NMR结构研究

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摘要

The development of nucleic acid base-pair analogues that use new modes of molecular recognition is important both for fundamental research and practical applications. The goal of this study was to evaluate 2-methoxypyridine as a cationic thymidine mimic in the A-T base pair. The hypothesis was that including protonation in the Watson-Crick base pairing scheme would enhance the thermal stability of the DNA double helix without compromising the sequence selectivity. DNA and peptide nucleic acid (PNA) sequences containing the new 2-methoxypyridine nucleobase (P) were synthesized and studied by using UV thermal melting and NMR spectroscopy. Introduction of P nucleobase caused a loss of thermal stability of approximate to 10 degrees C in DNA-DNA duplexes and approximate to 20 degrees C in PNA-DNA duplexes over a range of mildly acidic to neutral pH. Despite the decrease in thermal stability, the NMR structural studies showed that P-A formed the expected protonated base pair at pH 4.3. Our study demonstrates the feasibility of cationic unnatural base pairs; however, future optimization of such analogues will be required.
机译:使用新的分子识别模式的核酸基对类似物的发展对于基本研究和实际应用,重要的是重要的。本研究的目的是评估2-甲氧基吡啶作为阳离子胸苷模仿A-T碱基对。假设是在Watson-Crick碱基配对方案中包含质子化将增强DNA双螺旋的热稳定性而不损害序列选择性。通过使用UV热熔和NMR光谱合成并研究含有新的2-甲氧基吡啶核酶(P)的DNA和肽核酸(PNA)序列。 P nucleobase的引入导致DNA-DNA双链体中近似为10摄氏度的热稳定性的损失,并在PNA-DNA双链体中近似为20℃,在一定温和的酸性至中性pH中。尽管热稳定性降低,但NMR结构研究表明,P-A在pH4.3处形成预期的质子化碱基对。我们的研究表明了阳离子不自然基对的可行性;但是,将来需要未来的这种类似物的优化。

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