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与HIV-1 κB位点相关的非回文16碱基对DNA的溶液结构:BI-BII平衡诱导双链体整体动态曲率的证据

Solution structure of a non-palindromic 16 base-pair DNA related to the HIV-1 kappa B site: evidence for BI-BII equilibrium inducing a global dynamic curvature of the duplex.

作者信息

Tisné C, Hantz E, Hartmann B, Delepierre M

机构信息

Laboratoire de RMN, Institut Pasteur, CNRS URA, Paris, France.

出版信息

J Mol Biol. 1998 May 29;279(1):127-42. doi: 10.1006/jmbi.1998.1757.

Abstract

1H and 31P NMR spectroscopy have been used together with molecular modelling to determine the fine structure of a non-palindromic 16 bp DNA containing the NF-kappa B binding site. Much emphasis has been placed upon NMR optimization of both two-dimensional 31P NMR techniques to extract structural information defining the phosphodiester backbone conformation and selective homonuclear 2D COSY experiments to determine sugar conformations. NMR data show evidence for a dynamic behaviour of steps flanking the ten base-pairs of the NF-kappa B binding site. A BI-BII equilibrium at these steps is demonstrated and two models for each extreme conformation are proposed in agreement with NMR data. In the refined BII structures, the NF-kappa B binding site exhibits an intrinsic curvature towards the major groove that is magnified by the four flanking steps in the BII conformation. Furthermore, the base-pairs are translated into the major groove. Thus, we present a novel mode of dynamic intrinsic curvature compatible with the DNA curvature observed in the X-ray structure of the p50-DNA complex.

摘要

1H和31P核磁共振光谱已与分子建模一起用于确定包含NF-κB结合位点的非回文16bp DNA的精细结构。人们非常重视二维31P NMR技术的NMR优化,以提取定义磷酸二酯主链构象的结构信息,以及用于确定糖构象的选择性同核二维COSY实验。NMR数据显示了NF-κB结合位点十个碱基对两侧步骤的动态行为证据。证明了这些步骤处的BI-BII平衡,并根据NMR数据为每个极端构象提出了两个模型。在优化的BII结构中,NF-κB结合位点向大沟呈现固有曲率,该曲率在BII构象中被四个侧翼步骤放大。此外,碱基对向大沟平移。因此,我们提出了一种与p50-DNA复合物X射线结构中观察到的DNA曲率兼容的动态固有曲率新模式。

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