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各种烷基和不饱和取代基对某些硝基苯硫醚致突变性的影响。

Effect of various alkyl and unsaturated substituents on the mutagenicity of some nitrophenyl thioethers.

作者信息

Juneja T R, Talukdar A, Mehta N, Gupta R L

机构信息

University Institute of Pharmaceutical Sciences, Punjab University, Chandigarh 160014, India.

出版信息

Mutat Res. 2001 Aug 22;495(1-2):97-102. doi: 10.1016/s1383-5718(01)00201-7.

Abstract

A variety of nitro-substituted phenyl alkyl/aryl thioethers and nitroso-substituted phenyl alkyl/aryl thioethers have been synthesized and tested for their mutagenicity towards Salmonella typhimurium strain TA100, TA98, TA98NR and TA98/1,8-DNP(6) in the absence of S9 mix. The relative order of mutagenicity in TA98 and TA100 among p-nitrophenyl thioethers having alkyl or aryl substituents is allyl>phenyl>benzyl>butyl>propyl>ethyl>methyl. Compounds having an alkyl chain C(6) to C(12) were found to be non-mutagenic. Among the various positional isomers (ortho, meta and para) of nitro-substituted diphenyl thioethers only the compounds having the -NO(2) function at the para position is mutagenic, whereas compounds having a -NO(2) function at ortho and meta are non-mutagenic. However, the reduced intermediate, ortho-nitroso derivative was found to be mutagenic in all the four strains but the meta-nitroso derivative was found to be non-mutagenic. All mutagens were found to be non-mutagenic when tested in nitroreductase deficient strain TA98NR, whereas their nitroso intermediates are found to be mutagenic. A substantial fall in the mutagenic activity is observed when some mutagens are tested in O-acetyltransferase deficient strain TA98/1,8-DNP(6).

摘要

已经合成了多种硝基取代的苯基烷基/芳基硫醚和亚硝基取代的苯基烷基/芳基硫醚,并在无S9混合液的情况下测试了它们对鼠伤寒沙门氏菌TA100、TA98、TA98NR和TA98/1,8 - DNP(6)菌株的致突变性。在具有烷基或芳基取代基的对硝基苯基硫醚中,TA98和TA100中的致突变性相对顺序为烯丙基>苯基>苄基>丁基>丙基>乙基>甲基。发现具有C(6)至C(12)烷基链的化合物无致突变性。在硝基取代的二苯基硫醚的各种位置异构体(邻位、间位和对位)中,只有在对位具有 -NO(2)官能团的化合物具有致突变性,而在邻位和间位具有 -NO(2)官能团的化合物无致突变性。然而,还原中间体邻亚硝基衍生物在所有四种菌株中均具有致突变性,而间亚硝基衍生物无致突变性。在硝基还原酶缺陷菌株TA98NR中测试时,所有诱变剂均无致突变性,而它们的亚硝基中间体具有致突变性。当在O - 乙酰转移酶缺陷菌株TA98/1,8 - DNP(6)中测试一些诱变剂时,观察到致突变活性大幅下降。

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