Reactions of pyrimidine nucleosides with aqueous alkalies: kinetics and mechanisms.

H Lönnberg, P Suokas, R Käppi, E Darzynkiewicz
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引用次数: 7

Abstract

Kinetics for the reactions of various cytosine and uracil nucleosides and their alkyl derivatives with aqueous sodium hydroxide have been studied by liquid chromatography. Blocking of the glycosyl hydroxyl groups with alkyl groups and changes in the glycon moiety configuration have been observed to exert only moderate effects on the rate of deamination of cytosine nucleosides. Methylation of the 4-amino group retards deamination considerably, while a methyl substituent at C5 is rate accelerating and at C6 only moderately rate retarding. These findings have been accounted for by a mechanism involving a rate limiting bimolecular displacement of the 4-amino group by a hydroxide ion. Analogous comparisons with uracil nucleosides suggest that the decomposition of uridine is initiated by an intermolecular attack of hydroxide ion on the C5 atom of the base moiety. In contrast, beta-D-arabino- and beta-D-lyxo-furanosyl derivatives appear to be cleaved via an intramolecular nucleophilic attack of the ionized 2'-hydroxyl group.

嘧啶核苷与水溶液的反应:动力学和机理。
用液相色谱法研究了各种胞嘧啶和尿嘧啶核苷及其烷基衍生物与氢氧化钠水溶液的反应动力学。已观察到用烷基阻断糖基羟基和改变糖基部分构型对胞嘧啶核苷脱氨速率只有中等影响。4-氨基甲基化显著延缓脱胺反应,而甲基取代基在C5上加速脱胺反应,而在C6上仅适度延缓脱胺反应。这些发现是由一种机制来解释的,这种机制涉及到氢氧根离子对4-氨基的限速双分子位移。与尿嘧啶核苷类似的比较表明尿嘧啶的分解是由氢氧根离子对碱基部分的C5原子的分子间攻击引起的。相反,β - d -阿拉伯糖和β - d -羟基呋喃基衍生物似乎是通过电离的2'-羟基的分子内亲核攻击而被切割的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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