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Structural studies of a stable parallel-stranded DNA duplex incorporating isoguanine:cytosine and isocytosine:guanine basepairs by nuclear magnetic resonance spectroscopy.

机译:通过核磁共振波谱研究结合了异鸟嘌呤:胞嘧啶和异胞嘧啶:鸟嘌呤碱基对的稳定平行链DNA双链体的结构研究。

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摘要

Isoguanine (2-hydroxyladenine) is a product of oxidative damage to DNA and has been shown to cause mutation. It is also a potent inducer of parallel-stranded DNA duplex structure. The structure of the parallel-stranded DNA duplex (PS-duplex) 5'-d(TiGiCAiCiGiGAiCT) + 5'-d(ACGTGCCTGA), containing the isoguanine (iG) and 5-methyl-isocytosine (iC) bases, has been determined by NMR refinement. All imino protons associated with the iG:C, G:iC, and A:T (except the two terminal A:T) basepairs are observed at 2 degrees C, consistent with the formation of a stable duplex suggested by the earlier Tm measurements [Sugiyama, H., S. Ikeda, and I. Saito. 1996. J. Am. Chem. Soc. 118:9994-9995]. All basepairs are in the reverse Watson-Crick configuration. The structural characteristics of the refined PS-duplex are different from those of B-DNA. The PS duplex has two grooves with similar width (7.0 A) and depth (7.7 A), in contrast to the two distinct grooves (major groove width 11.7 A, depth 8.5 A, and minor groove width 5.7 A, depth 7.5 A) of B-DNA. The resonances of the amino protons of iG and C are clearly resolved and observable, but those of the G and iC are very broad and difficult to observe. Several intercalators with different complexities, including ethidium, daunorubicin, and nogalamycin, have been used to probe the flexibility of the backbone of the (iG, iC)-containing PS-duplex. All of them produce drug-induced UV/vis spectra identical to their respective spectra when bound to B-DNA, suggesting that those drugs bind to the (iG, iC)-containing PS-duplex using similar intercalation processes. The results may be useful in the design of intercalator-conjugated oligonucleotides for antisense applications. The study presented in this paper augments our understanding of a growing number of parallel-stranded DNA structures, including the G-quartet, the i-motif, and the unusual homo basepaired parallel-stranded double helix. Their possible relevance is discussed.
机译:异鸟嘌呤(2-羟基丙氨酸)是对DNA的氧化损伤的产物,并已证明会引起突变。它也是平行链DNA双链体结构的有效诱导剂。确定了包含异鸟嘌呤(iG)和5-甲基-异胞嘧啶(iC)碱基的平行链DNA双链体(PS-duplex)5'-d(TiGiCAiCiGiGAiCT)+ 5'-d(ACGTGCCTGA)的结构。通过NMR提纯。所有与iG:C,G:iC和A:T(两个末端A:T除外)碱基对相关的亚氨基质子均在2摄氏度下观察到,这与早期Tm测量表明形成稳定的双链体一致[ Sugiyama,H.,S. Ikeda和I. Saito。 1996年。化学Soc。 118:9994-9995]。所有碱基对均采用反向Watson-Crick配置。精制的PS双链体的结构特征不同于B-DNA。 PS双工具有两个宽度(7.0 A)和深度(7.7 A)相似的沟槽,而两个不同的沟槽(主沟槽宽度为11.7 A,深度为8.5 A,次沟槽宽度为5.7 A,深度为7.5 A)与B-DNA。 iG和C的氨基质子的共振可以清楚地分辨和观察到,但G和iC的氨基质子的共振非常宽且难以观察。几种具有不同复杂度的插入剂,包括乙锭,柔红霉素和诺霉素,已被用来探测含(iG,iC)PS双链体骨架的柔韧性。当与B-DNA结合时,所有这些药物产生的药物诱导的UV / vis光谱与其各自的光谱相同,这表明这些药物使用相似的嵌入过程与包含(iG,iC)的PS双链体结合。该结果对于反义应用中插入物-缀合的寡核苷酸的设计可能是有用的。本文提出的研究增强了我们对越来越多的平行链DNA结构的理解,包括G四重唱,i-基序和不寻常的同源碱基对平行链双螺旋。讨论了它们可能的相关性。

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