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在存在大鼠肝脏S9和去甲哈尔满的情况下,硝基苯及其衍生物的诱变性对鼠伤寒沙门氏菌酶的依赖性。

Dependence on Salmonella typhimurium enzymes of mutagenicities of nitrobenzene and its derivatives in the presence of rat-liver S9 and norharman.

作者信息

Suzuki J, Takahashi N, Kobayashi Y, Miyamae R, Ohsawa M, Suzuki S

出版信息

Mutat Res. 1987 Jun;178(2):187-93. doi: 10.1016/0027-5107(87)90268-5.

Abstract

Dependence on S. typhimurium enzymes of mutagenicities of nitrobenzene (NB) and o-, p-chloronitrobenzenes (o-, p-CNBs), which are only mutagenic in the presence of S9 and norharman (NOH), was investigated using a nitroreductase-deficient strain TA98NR and an esterifying enzyme-deficient strain TA98/1,8-DNP6. NB exhibited mutagenicity towards TA98 but did not towards TA98NR strain in spite of the presence of S9 in the assay system. The mutagenicity of o-CNB towards TA98NR was significantly lower than that of o-CNB towards TA98. In contrast to NB and o-CNB, synthesized phenylhydroxylamine (PHA) and o-chlorophenylhydroxylamine (o-CPHA) exhibited approximately the same mutagenicity towards both tester strains. These results indicate that the nitroreduction required for the appearance of mutagenicity of the nitrobenzene derivatives in the presence of S9 and NOH is dependent on the nitroreductase of the tester strain. In addition, the mutagenicities of PHA and p-CPHA were significantly higher towards TA98/1,8-DNP6 than towards TA98, suggesting that the esterification of their hydroxylamines produced inactivation rather than activation. From these results, it was concluded that S9 and NOH play a role in metabolic activation other than the reduction of the nitro group to hydroxylamine and subsequent esterification for the mutagenesis of NB and its derivatives.

摘要

利用硝基还原酶缺陷型菌株TA98NR和酯化酶缺陷型菌株TA98/1,8 - DNP6,研究了硝基苯(NB)以及邻、对氯硝基苯(o -、p - CNBS)在仅存在S9和去甲哈尔满(NOH)时的致突变性对鼠伤寒沙门氏菌酶的依赖性。NB对TA98表现出致突变性,但尽管检测系统中存在S9,对TA98NR菌株却没有致突变性。o - CNBS对TA98NR的致突变性明显低于对TA98的致突变性。与NB和o - CNBS不同,合成的苯羟胺(PHA)和邻氯苯羟胺(o - CPHA)对两种测试菌株表现出大致相同的致突变性。这些结果表明,在S9和NOH存在下硝基苯衍生物致突变性出现所需的硝基还原依赖于测试菌株的硝基还原酶。此外,PHA和p - CPHA对TA98/1,8 - DNP6的致突变性明显高于对TA98的致突变性,这表明它们的羟胺酯化产生的是失活而非激活。从这些结果可以得出结论,S9和NOH在代谢激活中发挥作用,而不是将硝基还原为羟胺以及随后的酯化作用,以实现NB及其衍生物的致突变性。

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