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用乙基亚硝基脲诱导经处理的DBA/2品系小鼠精原细胞中的正向和反向特异性位点突变以及显性白内障突变。

The induction of forward and reverse specific-locus mutations and dominant cataract mutations in spermatogonia of treated strain DBA/2 mice by ethylnitrosourea.

作者信息

Favor J, Neuhäuser-Klaus A, Ehling U H

机构信息

GSF-Institut für Säugetiergenetik, Neuherberg, F.R.G.

出版信息

Mutat Res. 1991 Aug;249(2):293-300. doi: 10.1016/0027-5107(91)90003-7.

Abstract

The mutagenic effectiveness of ethylnitrosurea (ENU) was assessed in treated spermatogonia of DBA/2 mice. In a total of 17,515 offspring examined following 160 mg ENU/kg body weight treatment of parental males, 26 forward specific-locus mutations, 2 reverse specific-locus mutations and 9 dominant cataract mutations were recovered. ENU increased the mutation rate to all 3 genetic endpoints. However, ENU was less effective in treated DBA/2 mice than in the standard experimental protocol employing treated hybrid (102 X C3H)F1 male mice. This observed difference for a direct-acting mutagen such as ENU may result from differences in the detoxification of ENU or from differences in the DNA-repair capabilities of strain DBA/2. The first documented reverse mutation of the b allele is reported. The reversion was shown to be due to an AT to GC transition. To date, in addition to the reverse mutation of the b allele, 5 independent ENU-induced mutations recovered in germ cells of the mouse have been molecularly characterized and all have been shown to be base substitutions at an AT site. This is in contrast to the expected mechanism of ENU mutation induction due to O6-ethylguanine adduct formation which results in a GC to AT base-pair substitution and emphasizes the complexities of mutagenesis in germ cells of mammals.

摘要

在经处理的DBA/2小鼠精原细胞中评估了乙基亚硝基脲(ENU)的诱变效力。在用160 mg ENU/ kg体重处理亲代雄性小鼠后,总共检查了17,515只后代,发现了26个正向特异性位点突变、2个反向特异性位点突变和9个显性白内障突变。ENU增加了所有3个遗传终点的突变率。然而,ENU在处理过的DBA/2小鼠中的效果不如在使用处理过的杂种(102×C3H)F1雄性小鼠的标准实验方案中有效。对于像ENU这样的直接作用诱变剂所观察到的这种差异,可能是由于ENU解毒的差异或DBA/2品系DNA修复能力的差异所致。报道了首次记录的b等位基因的反向突变。该反向突变显示是由于AT到GC的转换。迄今为止,除了b等位基因的反向突变外,在小鼠生殖细胞中回收的5个独立的ENU诱导突变已进行了分子表征,并且所有这些突变均显示为AT位点的碱基替换。这与由于O6-乙基鸟嘌呤加合物形成导致GC到AT碱基对替换的ENU突变诱导预期机制形成对比,并强调了哺乳动物生殖细胞诱变的复杂性。

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