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甲基苄基亚硝胺及其α-乙酰氧基衍生物的致突变性。

The mutagenicity of methylbenzylnitrosamine and its alpha-acetoxy derivatives.

作者信息

Tannenbaum S R, Kraft P, Baldwin J, Branz S

出版信息

Cancer Lett. 1977 May;2(6):305-10. doi: 10.1016/s0304-3835(77)80009-8.

Abstract

Biological activity of the alpha-acetoxy derivatives of methylbenzylnitrosamine was evaluated using tester strains of Salmonella typhimurium. Compound III, oxidized on the benzyl moiety, was more toxic and more mutagenic than Compound IV, oxidized on the methyl side chain. Compound IV was weakly toxic and was non-mutagenic at the concentrations tested. The presence or absence of the uvrB repair system had no effect on the toxicity of either Compound II or IV. Neither the alpha-oxidized compounds nor the parent nitrosamine reverted the frameshift mutants. As a mutagen, Compound III was approximately as active as N-nitroso compounds not requiring metabolic activation, more active than alpha-acetoxy dialkylnitrosamines and less active than the cyclic alpha-acetoxynitrosopyrrolidine.

摘要

使用鼠伤寒沙门氏菌测试菌株评估了甲基苄基亚硝胺的α-乙酰氧基衍生物的生物活性。在苄基部分被氧化的化合物III比在甲基侧链被氧化的化合物IV毒性更大且致突变性更强。化合物IV毒性较弱,在所测试的浓度下无致突变性。uvrB修复系统的存在与否对化合物II和IV的毒性均无影响。α-氧化化合物和母体亚硝胺均未使移码突变体回复突变。作为诱变剂,化合物III的活性与不需要代谢活化的N-亚硝基化合物大致相当,比α-乙酰氧基二烷基亚硝胺更具活性,比环状α-乙酰氧基亚硝基吡咯烷活性更低。

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