首页> 美国卫生研究院文献>Journal of Bacteriology >Suppressible base substitution mutations induced by angelicin (isopsoralen) in the Escherichia coli lacI gene: implications for the mechanism of SOS mutagenesis.
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Suppressible base substitution mutations induced by angelicin (isopsoralen) in the Escherichia coli lacI gene: implications for the mechanism of SOS mutagenesis.

机译:在大肠杆菌lacI基因中由当归霉素(异补骨脂素)诱导的可抑制碱基取代突变:对SOS诱变机制的影响。

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摘要

Angelicin- plus near-UV-induced mutations were umuC dependent in Escherichia coli K-12. Angelicin, a monofunctional psoralen derivative, is believed to damage DNA almost exclusively at pyrimidine bases. To broaden our knowledge about the mutagenic specificity of SOS-dependent mutagens, we determined the mutational specificity of 233 suppressible lacI mutations induced by angelicin. More than 90% of the nonsense mutations arose via transversion substitutions. The three most frequently mutated sites were at A-T base pairs and accounted for more than one-third of all induced nonsense mutations. The two hottest sites were at the only occurrences of the 5'-TATA-3' tetranucleotide in lacI, a sequence expected to be a preferred binding site for a psoralen. Both A-T-to-T-A and A-T-to-C-G transversions were well induced by angelicin treatment, but the frequency of each transversion depended on the particular site. We also detected significant induction of transversion mutations at G-C sites. The induction of transversions by an SOS-dependent mutagen that generates lesions at pyrimidines supports the idea that DNA lesions influence the selection of bases that are incorporated via the process of SOS repair.
机译:Angelicin加近紫外线诱导的突变在大肠杆菌K-12中是umuC依赖性的。据信安吉利辛是一种单功能补骨脂素衍生物,几乎只能在嘧啶碱基处破坏DNA。为了拓宽我们对SOS依赖性诱变剂诱变特异性的认识,我们确定了当归霉素诱导的233种可抑制lacI突变的突变特异性。超过90%的无义突变是通过颠换取代产生的。三个最频繁突变的位点位于A-T碱基对,占所有诱导的无义突变的三分之一以上。这两个最热的位点是lacI中唯一出现的5'-TATA-3'四核苷酸,该序列被认为是补骨脂素的优选结合位点。当归霉素处理可以很好地诱导A-T到T-A和A-T到C-G的转化,但是每个转化的频率都取决于特定的位点。我们还在G-C位点检测到明显的颠换突变诱导。 SOS依赖性诱变剂在嘧啶上产生损伤,从而引起转化,这支持了DNA损伤影响通过SOS修复过程结合的碱基选择的想法。

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