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New Modified Deoxythymine with Dibranched Tetraethylene Glycol Stabilizes G-Quadruplex Structures

机译:具有双支化四乙二醇的新型改性脱氧胸腺嘧啶可稳定G-四链体结构。

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摘要

Methods for stabilizing G-quadruplex formation is a promising therapeutic approach for cancer treatment and other biomedical applications because stable G-quadruplexes efficiently inhibit biological reactions. Oligo and polyethylene glycols are promising biocompatible compounds, and we have shown that linear oligoethylene glycols can stabilize G-quadruplexes. Here, we developed a new modified deoxythymine with dibranched or tribranched tetraethylene glycol (TEG) and incorporated these TEG-modified deoxythymines into a loop region that forms an antiparallel G-quadruplex. We analyzed the stability of the modified G-quadruplexes, and the results showed that the tribranched TEG destabilized G-quadruplexes through entropic contributions, likely through steric hindrance. Interestingly, the dibranched TEG modification increased G-quadruplex stability relative to the unmodified DNA structures due to favorable enthalpic contributions. Molecular dynamics calculations suggested that dibranched TEG interacts with the G-quadruplex through hydrogen bonding and CH-π interactions. Moreover, these branched TEG-modified deoxythymine protected the DNA oligonucleotides from degradation by various nucleases in human serum. By taking advantage of the unique interactions between DNA and branched TEG, advanced DNA materials can be developed that affect the regulation of DNA structure.
机译:稳定G-四链体形成的方法是用于癌症治疗和其他生物医学应用的有前途的治疗方法,因为稳定的G-四链体有效地抑制了生物反应。寡聚乙二醇和聚乙二醇是有前途的生物相容性化合物,而且我们已经证明直链聚乙二醇可以稳定G-四链体。在这里,我们开发了一种新的带有二支或三支四甘醇(TEG)的修饰的脱氧胸腺嘧啶,并将这些TEG修饰的脱氧胸腺嘧啶掺入形成反平行G-四链体的环区域​​。我们分析了修饰的G-四链体的稳定性,结果表明三支TEG通过熵的贡献(可能是通过空间位阻)使G-四链体不稳定。有趣的是,由于有利的焓贡献,相对于未修饰的DNA结构,二分支的TEG修饰增加了G-四链体的稳定性。分子动力学计算表明,支链的TEG通过氢键和CH-π相互作用与G-四链体相互作用。此外,这些支化的TEG修饰的脱氧胸腺嘧啶保护DNA寡核苷酸免受人类血清中各种核酸酶的降解。通过利用DNA与支链TEG之间的独特相互作用,可以开发出影响DNA结构调节的高级DNA材料。

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