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碱基对的生物平衡。

The biological equilibrium of base pairs.

作者信息

Strazewski P

机构信息

Institut für organische Chemie Universität, Basel, Switzerland.

出版信息

J Mol Evol. 1990 Feb;30(2):116-24. doi: 10.1007/BF02099938.

Abstract

An inherent feature of double-stranded DNA is the possible replacement of any base pair by another one upon replication. A replication-dependent substitution mutation of a matched base pair requires the temporary formation of a mismatched base pair (mispair). A functionally complementary pair of mispairs is ascribed to each of the four types of substitution mutations. Provided that all types of mispairs can be formed, a dynamic biological equilibrium between the four matched base pairs must exist in all DNA, which is directly related to the formation and stability of the corresponding eight mispairs in vivo. Each nucleotide position in a genome can therefore be described as a system of six dynamic equilibria between the four matched base pairs. After a sufficient number of replications, these equilibrium states will express an overall mutation-selection balance for each individual base pair. In a thermodynamic context, the mispairs represent intermediate states on the transformation pathways between the matched base pairs. Catalysts change the stability and probability of formation of intermediate states. Mutagenic proteins are proposed as hypothetical substitution mutation catalysts in vivo. Functionally, they would be capable of recognizing a particular DNA sequence, tautomerizing a nucleotide base thereof, and hence efficiently inducing a specific misincorporation. Phenomenologically such catalysts would accelerate the rates of substitution mutations and provide pathways for directional mutation pressure.

摘要

双链DNA的一个固有特征是在复制过程中任何碱基对都有可能被另一个碱基对取代。匹配碱基对的复制依赖性替代突变需要暂时形成错配碱基对(错配)。四种类型的替代突变中的每一种都有一对功能互补的错配。如果所有类型的错配都能形成,那么在所有DNA中,四种匹配碱基对之间必然存在动态生物平衡,这与体内相应的八种错配的形成和稳定性直接相关。因此,基因组中的每个核苷酸位置都可以描述为四种匹配碱基对之间六个动态平衡的系统。经过足够数量的复制后,这些平衡状态将表现出每个碱基对的整体突变-选择平衡。在热力学背景下,错配代表了匹配碱基对之间转化途径上的中间状态。催化剂会改变中间状态形成的稳定性和概率。诱变蛋白被认为是体内假设的替代突变催化剂。从功能上讲,它们能够识别特定的DNA序列,使其核苷酸碱基互变异构,从而有效地诱导特定的错误掺入。从现象学上讲,这种催化剂会加速替代突变的速率,并为定向突变压力提供途径。

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