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3-甲基-1-苯基三氮烯对胎儿、母体及正常大鼠组织核酸的体内烷基化作用

In vivo alkylation of foetal, maternal and normal rat tissue nucleic acids by 3-methyl-1-phenyltriazene.

作者信息

Margison G P, Likhachev A J, Kolar G F

出版信息

Chem Biol Interact. 1979 May;25(2-3):345-53. doi: 10.1016/0009-2797(79)90056-5.

Abstract

The carcinogen 3-methyl-1-phenyltriazene (MPT) was administered subcutaneously to normal or pregnant BD VI rats and DNA and RNA were isolated from various tissues after 8 h or 15 h, respectively. Sephadex G-10 chromatography of DNA hydrolysates showed the presence of 7-methylguanine in all tissues examined including that of the brain, one of the target organs for tumour induction. The amounts of the minor product, O6-methylguanine, were characteristic of an SN1 reaction mechanism. Dowex-50 chromatography of RNA hydrolysates showed the presence of 7-methylguanine and of the minor product, 3-methylcytosine. The relative amounts, both of the methylated bases in the individual nucleic acids and of 7-methylguanine in DNA and RNA, were similar to those found previously after administration of 3,3-dimethyl-1-phenyltriazene (DMPT). This suggests the involvment of a common alkylating intermediate. De novo incorporation of radioactivity into purine bases was detected in both DNA and RNA although the levels were not related to the amounts of methylation. The results show that MPT is sufficiently stable to alkylate nucleic acids in vivo and are consistent with the hypothesis that this reaction is a prerequisite for tumour induction. Futhermore, they support the proposal that MPT is the active intermediate in the induction of tumours by DMPT.

摘要

将致癌物3-甲基-1-苯基三氮烯(MPT)皮下注射给正常或怀孕的BD VI大鼠,分别在8小时或15小时后从各种组织中分离出DNA和RNA。DNA水解产物的葡聚糖G-10色谱分析表明,在所有检测的组织中都存在7-甲基鸟嘌呤,包括作为肿瘤诱导靶器官之一的脑。次要产物O6-甲基鸟嘌呤的量具有SN1反应机制的特征。RNA水解产物的Dowex-50色谱分析表明存在7-甲基鸟嘌呤和次要产物3-甲基胞嘧啶。单个核酸中甲基化碱基的相对量以及DNA和RNA中7-甲基鸟嘌呤的相对量,与先前给予3,3-二甲基-1-苯基三氮烯(DMPT)后发现的相似。这表明涉及一种共同的烷基化中间体。在DNA和RNA中均检测到放射性重新掺入嘌呤碱基,尽管其水平与甲基化量无关。结果表明,MPT在体内足够稳定以烷基化核酸,并且与该反应是肿瘤诱导的先决条件这一假设一致。此外,它们支持MPT是DMPT诱导肿瘤的活性中间体这一观点。

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