Liu Yun, Gregersen Brent A, Lopez Xabier, York Darrin M
Department of Chemistry, University of Minnesota, 207 Pleasant St. SE, Minneapolis, Minnesota 55455-0431, USA.
J Phys Chem B. 2005 Oct 27;109(42):19987-20003. doi: 10.1021/jp053146z.
Density functional calculations of thio effects on the in-line mechanism of methanolysis of ethylene phosphate (a reverse reaction model for RNA phosphate transesterification) are presented. A total of 12 reaction mechanisms are examined using the B3LYP functional with large basis sets, and the effects of solvation were treated using the PCM, CPCM, and SM5 solvation models. Single thio substitutions at all of the distinct phosphoryl oxygen positions (2', 3', 5', pro-R) and a double thio substitution at the nonbridging (pro-R/pro-S) positions were considered. Profiles for each reaction were calculated in the dianionic and monoanionic/monoprotic states, corresponding to reaction models under alkaline and nonalkaline conditions, respectively. These models provide insight into the mechanisms of RNA transesterification thio effects and serve as a set of high-level quantum data that can be used in the design of new semiempirical quantum models for hybrid quantum mechanical/molecular mechanical simulations and linear-scaling electronic structure calculations.
本文介绍了硫对磷酸乙烯酯甲醇解的内型机理(RNA磷酸酯酯交换的逆反应模型)影响的密度泛函计算。使用具有大基组的B3LYP泛函研究了总共12种反应机理,并使用PCM、CPCM和SM5溶剂化模型处理溶剂化效应。考虑了在所有不同的磷酰氧位置(2'、3'、5'、前-R)的单硫取代以及在非桥连(前-R/前-S)位置的双硫取代。在双阴离子和单阴离子/单质子状态下计算了每个反应的剖面图,分别对应于碱性和非碱性条件下的反应模型。这些模型有助于深入了解RNA酯交换硫效应的机理,并作为一组高级量子数据,可用于设计用于混合量子力学/分子力学模拟和线性缩放电子结构计算的新半经验量子模型。
