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首页> 美国卫生研究院文献>ACS AuthorChoice >Differential Base Stacking Interactions Induced by Trimethylene Interstrand DNA Cross-Links in the 5′-CpG-3′ and 5′-GpC-3′ Sequence Contexts
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Differential Base Stacking Interactions Induced by Trimethylene Interstrand DNA Cross-Links in the 5′-CpG-3′ and 5′-GpC-3′ Sequence Contexts

机译:在5-CpG-3和5-GpC-3序列背景下由三亚甲基链间DNA交联诱导的差异碱基堆积相互作用。

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Synthetically derived trimethylene interstrand DNA cross-links have been used as surrogates for the native cross-links that arise from the 1,N2-deoxyguanosine adducts derived from α,β-unsaturated aldehydes. The native enal-mediated cross-linking occurs in the 5′-CpG-3′ sequence context but not in the 5′-GpC-3′ sequence context. The ability of the native enal-derived 1,N2-dG adducts to induce interstrand DNA cross-links in the 5′-CpG-3′ sequence as opposed to the 5′-GpC-3′ sequence is attributed to the destabilization of the DNA duplex in the latter sequence context. Here, we report higher accuracy solution structures of the synthetically derived trimethylene cross-links, which are refined from NMR data with the AMBER force field. When the synthetic trimethylene cross-links are placed into either the 5′-CpG-3′ or the 5′-GpC-3′ sequence contexts, the DNA duplex maintains B-DNA geometry with structural perturbations confined to the cross-linked base pairs. Watson−Crick hydrogen bonding is conserved throughout the duplexes. Although different from canonical B-DNA stacking, the cross-linked and the neighbor base pairs stack in the 5′-CpG-3′ sequence. In contrast, the stacking at the cross-linked base pairs in the 5′-GpC-3′ sequence is greatly perturbed. The π-stacking interactions between the cross-linked and the neighbor base pairs are reduced. This is consistent with remarkable chemical shift perturbations of the C5 H5 and H6 nucleobase protons that shifted downfield by 0.4−0.5 ppm. In contrast, these chemical shift perturbations in the 5′-CpG-3′ sequence are not remarkable, consistent with the stacked structure. The differential stacking of the base pairs at the cross-linking region probably explains the difference in stabilities of the trimethylene cross-links in the 5′-CpG-3′ and 5′-GpC-3′ sequence contexts and might, in turn, account for the sequence selectivity of the interstrand cross-link formation induced by the native enal-derived 1,N2-dG adducts.
机译:合成衍生的三亚甲基链间DNA交联已被用作天然交联的替代物,该天然交联源自α,β-不饱和醛的1,N 2 -脱氧鸟苷加合物。天然的enal介导的交联发生在5'-CpG-3'序列中,但不在5'-GpC-3'序列中。与5'-GpC-3'相反,天然的源自烯醛的1,N 2 -dG加合物诱导5'-CpG-3'序列中链间DNA交联的能力序列归因于后一序列上下文中DNA双链体的不稳定。在这里,我们报告了合成衍生的三亚甲基交联的更高精确度的溶液结构,该结构已通过NMR数据和AMBER力场进行了精炼。当将合成的三亚甲基交联键置于5'-CpG-3'或5'-GpC-3'序列环境中时,DNA双链体会维持B-DNA的几何形状,其结构扰动仅限于交联的碱基对。沃森-克里克氢键在整个双链体中均保持保守。尽管与规范的B-DNA堆叠不同,但交联的和相邻的碱基对以5'-CpG-3'序列堆叠。相反,在5'-GpC-3'序列中的交联碱基对处的堆积受到极大干扰。减少了交联的碱基对和相邻碱基对之间的π堆积相互作用。这与C 5 H5和H6核碱基质子的显着化学位移扰动相一致,该质子向低场偏移了0.4-0.5 ppm。相反,在5'-CpG-3'序列中的这些化学位移扰动并不明显,与堆叠结构一致。碱基对在交联区域的差异堆积可能解释了5'-CpG-3'和5'-GpC-3'序列上下文中三亚甲基交联稳定性的差异,进而可能解释了解释天然烯醛衍生的1,N 2 -dG加合物诱导的链间交联形成的序列选择性。

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