脱氧核苷的内在构象性质:胞嘧啶在DNA的A、B和Z型之间平衡中的潜在作用。
Intrinsic conformational properties of deoxyribonucleosides: implicated role for cytosine in the equilibrium among the A, B, and Z forms of DNA.
作者信息
Foloppe N, MacKerell A D
机构信息
Department of Pharmaceutical Sciences, School of Pharmacy, University of Maryland, Baltimore, Maryland 21201, USA.
出版信息
Biophys J. 1999 Jun;76(6):3206-18. doi: 10.1016/S0006-3495(99)77472-2.
Structural properties of biomolecules are dictated by their intrinsic conformational energetics in combination with environmental contributions. Calculations using high-level ab initio methods on the deoxyribonucleosides have been performed to investigate the influence of base on the intrinsic conformational energetics of nucleosides. Energy minima in the north and south ranges of the deoxyribose pseudorotation surfaces have been located, allowing characterization of the influence of base on the structures and energy differences between those minima. With all bases, chi values associated with the south energy minimum are lower than in canonical B-DNA, while chi values associated with the north energy minimum are close to those in canonical A-DNA. In deoxycytidine, chi adopts an A-DNA conformation in both the north and south energy minima. Energy differences between the A and B conformations of the nucleosides are <0.5 kcal/mol in the present calculations, except with deoxycytidine, where the A form is favored by 2.3 kcal/mol, leading the intrinsic conformational energetics of GC basepairs to favor the A form of DNA by 1.5 kcal/mol as compared with AT pairs. This indicates that the intrinsic conformational properties of cytosine at the nucleoside level contribute to the A form of DNA containing predominately GC-rich sequences. In the context of a B versus Z DNA equilibrium, deoxycytidine favors the Z form over the B form by 1.6 kcal/mol as compared with deoxythymidine, suggesting that the intrinsic conformational properties of cytosine also contribute to GC-rich sequences occurring in Z DNA with a higher frequency than AT-rich sequences. Results show that the east pseudorotation energy barrier involves a decrease in the furanose amplitude and is systematically lower than the inversion barrier, with the energy differences influenced by the base. Energy barriers going from the south (B form) sugar pucker to the east pseudorotation barrier are lower in pyrimidines as compared with purines, indicating that the intrinsic conformational properties associated with base may also influence the sugar pseudorotational population distribution seen in DNA crystal structures and the kinetics of B to A transitions. The present work provides evidence that base composition, in addition to base sequence, can influence DNA conformation.
生物分子的结构特性由其内在的构象能量学以及环境因素共同决定。已使用高级从头算方法对脱氧核糖核苷进行计算,以研究碱基对核苷内在构象能量学的影响。已确定脱氧核糖假旋转表面南北范围内的能量最小值,从而能够表征碱基对这些最小值之间结构和能量差异的影响。对于所有碱基,与南方能量最小值相关的χ值低于经典B-DNA中的值,而与北方能量最小值相关的χ值接近经典A-DNA中的值。在脱氧胞苷中,χ在南北能量最小值处均采用A-DNA构象。在当前计算中,核苷A和B构象之间的能量差异小于0.5千卡/摩尔,但脱氧胞苷除外,其中A形式比B形式更有利2.3千卡/摩尔,这使得GC碱基对的内在构象能量学与AT碱基对相比,使DNA的A形式更有利1.5千卡/摩尔。这表明核苷水平上胞嘧啶的内在构象特性有助于富含GC序列的DNA呈现A形式。在B与Z DNA平衡的背景下,与脱氧胸苷相比,脱氧胞苷对Z形式的偏好比对B形式的偏好高1.6千卡/摩尔,这表明胞嘧啶的内在构象特性也导致富含GC的序列在Z DNA中出现的频率高于富含AT的序列。结果表明,向东假旋转能垒涉及呋喃糖振幅的降低,并且系统地低于反转能垒,能量差异受碱基影响。与嘌呤相比,嘧啶从南方(B形式)糖构象到向东假旋转能垒的能垒更低,这表明与碱基相关的内在构象特性也可能影响DNA晶体结构中观察到的糖假旋转群体分布以及B到A转变的动力学。目前的工作提供了证据,表明除了碱基序列外,碱基组成也可以影响DNA构象。
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