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链和方向不对称性对双螺旋DNA中碱基对耦合和电荷转移的影响。

Effects of strand and directional asymmetry on base-base coupling and charge transfer in double-helical DNA.

作者信息

O'Neill Melanie A, Barton Jacqueline K

机构信息

Division of Chemistry and Chemical Engineering, California Institute of Technology, Pasadena, CA 91125, USA.

出版信息

Proc Natl Acad Sci U S A. 2002 Dec 24;99(26):16543-50. doi: 10.1073/pnas.012669599. Epub 2002 Dec 16.

Abstract

Mechanistic models of charge transfer (CT) in macromolecules often focus on CT energetics and distance as the chief parameters governing CT rates and efficiencies. However, in DNA, features unique to the DNA molecule, in particular, the structure and dynamics of the DNA base stack, also have a dramatic impact on CT. Here we probe the influence of subtle structural variations on base-base CT within a DNA duplex by examining photoinduced quenching of 2-aminopurine (Ap) as a result of hole transfer (HT) to guanine (G). Photoexcited Ap is used as a dual reporter of variations in base stacking and CT efficiency. Significantly, the unique features of DNA, including the strandedness and directional asymmetry of the double helix, play a defining role in CT efficiency. For an (AT)n bridge, the orientation of the base pairs is critical; the yield of intrastrand HT is markedly higher through (A)n compared with (T)n bridges, whereas HT via intrastrand pathways is more efficient than through interstrand pathways. Remarkably, for reactions through the same DNA bridge, over the same distance, and with the same driving force, HT from photoexcited Ap to G in the 5' to 3' direction is more efficient and less dependent on distance than HT from 3' to 5'. We attribute these differences in HT efficiency to variations in base-base coupling within the DNA assemblies. Thus base-base coupling is a critical parameter in DNA CT and strongly depends on subtle structural nuances of duplex DNA.

摘要

大分子中电荷转移(CT)的机理模型通常将CT能量学和距离作为控制CT速率和效率的主要参数。然而,在DNA中,DNA分子特有的特征,特别是DNA碱基堆积的结构和动力学,也对CT有显著影响。在这里,我们通过研究2-氨基嘌呤(Ap)由于空穴转移(HT)到鸟嘌呤(G)而产生的光诱导猝灭,来探究DNA双链体内细微结构变化对碱基间CT的影响。光激发的Ap用作碱基堆积和CT效率变化的双重报告分子。值得注意的是,DNA的独特特征,包括双螺旋的链状结构和方向不对称性,在CT效率中起决定性作用。对于(AT)n桥,碱基对的方向至关重要;通过(A)n的链内HT产率明显高于通过(T)n桥的产率,而通过链内途径的HT比通过链间途径更有效。值得注意的是,对于通过相同DNA桥、在相同距离且具有相同驱动力的反应,从光激发的Ap到G在5'到3'方向的HT比从3'到5'的HT更有效且对距离的依赖性更小。我们将这些HT效率的差异归因于DNA组装体内碱基间耦合的变化。因此,碱基间耦合是DNA CT中的一个关键参数,并且强烈依赖于双链DNA的细微结构细微差别。

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