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化学诱变机制IV:三亚乙基蜜胺与核酸成分之间的反应

MECHANISM OF CHEMICAL MUTAGENESIS IV. : Reaction between Triethylene Melamine and Nucleic Acid Components.

作者信息

Lorkiewicz Z, Szybalski W

机构信息

McArdle Memorial Laboratory, University of Wisconsin, Madison, Wisconsin.

出版信息

J Bacteriol. 1961 Aug;82(2):195-201. doi: 10.1128/jb.82.2.195-201.1961.

Abstract

Lorkiewicz, Z. (University of Wisconsin, Madison), and Waclaw Szybalski. Mechanism of chemical mutagenesis. IV. Reaction between triethylene melamine and nucleic acid components. J. Bacteriol. 82: 195-201. 1961.-Triethylene melamine interacts primarily with phosphorylated intracellular deoxyribonucleic acid (DNA) precursors and not with DNA. It was found by direct chemical and chromatographic analysis that only pyrimidine precursors of nucleic acids are attacked by triethylene melamine. In the course of the triethylene melamine-deoxycytidine reaction the mutagenicity of the reaction mixture is lost, but the mutagenicity of the triethylene melamine-thymidine reaction products significantly increases above that of the reaction substrates. Several steps are postulated to explain the mechanism of the triethylene melamine-initiated mutagenic reaction: (i) Reaction I, semireversible uptake of triethylene melamine; (ii) reaction II, chemical interaction between triethylene melamine and intracellular thymidine mono- or triphosphate with the production of a functional analogue of the latter; (iii) incorporation of this fraudulent analogue into the newly formed DNA strand; (iv) occurrence of self-perpetuating errors in the sequence of natural bases during subsequent rounds of replication of the analogue-containing DNA strand. It is postulated that the mechanism of mutagenic responses to different types of mutagens can fit either a simplified (mutagenic base analogues) or extended version (radiation) of this schema.

摘要

洛尔基维茨,Z.(威斯康星大学麦迪逊分校)和瓦茨瓦夫·希巴尔斯基。化学诱变机制。IV.三亚乙基三聚氰胺与核酸成分之间的反应。《细菌学杂志》82: 195 - 201。1961年。——三亚乙基三聚氰胺主要与磷酸化的细胞内脱氧核糖核酸(DNA)前体相互作用,而非与DNA相互作用。通过直接化学分析和色谱分析发现,核酸的嘧啶前体是三亚乙基三聚氰胺唯一攻击的对象。在三亚乙基三聚氰胺 - 脱氧胞苷反应过程中,反应混合物的致突变性丧失,但三亚乙基三聚氰胺 - 胸苷反应产物的致突变性比反应底物显著增加。推测了几个步骤来解释三亚乙基三聚氰胺引发的诱变反应机制:(i)反应I,三亚乙基三聚氰胺的半可逆摄取;(ii)反应II,三亚乙基三聚氰胺与细胞内胸苷单磷酸或三磷酸之间的化学相互作用,产生后者的功能类似物;(iii)将这种欺诈性类似物掺入新形成的DNA链中;(iv)在随后含类似物的DNA链复制轮次中,天然碱基序列中出现自我延续的错误。据推测,对不同类型诱变剂的诱变反应机制可以符合该模式的简化版(诱变碱基类似物)或扩展版(辐射)。

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