首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >The mutagenic effects of 7,12-dimethylbenz(a)anthacene, 3-methylcholanthrene and benzo(a)pyrene to the developing Syrian hamster fetus measured by an in vivo/in vitro mutation assay.
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The mutagenic effects of 7,12-dimethylbenz(a)anthacene, 3-methylcholanthrene and benzo(a)pyrene to the developing Syrian hamster fetus measured by an in vivo/in vitro mutation assay.

机译:通过体内/体外突变测定法测定了7,12-二甲基苯并(a)并蒽,3-甲基胆and和苯并(a)py对发育中的叙利亚仓鼠胎儿的诱变作用。

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摘要

The transplacental mutagenicity of three polycylic aromatic hydrocarbons, 7,12-dimethylbenz[a]anthacene (DMBA), 3-methylcholanthrene (MC) and benzo[a]pyrene (BP), was measured by an in vivo/in vitro mutation assay. Fetal sensitivity and dose-response characteristics with regard to transplacental mutagenesis by these compounds have never been quantified. In the current experiment, pregnant Syrian hamsters were exposed to these compounds at day 12 of gestation. Twenty-four hours later the fetuses were removed and their cells were allowed a 5-day expression time in culture. They were then seeded for colony formation and also for mutation selection by diphtheria toxin. DMBA at 0.2 mmol/kg (51.3 mg/kg) had an induced mutant frequency of 1.56 x 10(-4) mutants per surviving cell. This was 598 times the historical control. DMBA at 0.2 mmol/kg was 3.6 times more potent than the highly mutagenic positive control, ethylnitrosourea, at 1 mmol/kg. DMBA also caused a dose-dependent increase in cloning efficiency, which was highly correlated with mutation rate. BP and MC were less effective than DMBA, causing increased mutations that were 31.6 and 17.7 times the historical control, respectively, and for neither was there any correlation of mutation rate with cloning efficiency. The special effectiveness of DMBA as a transplacental mutagen may relate to its ability to cause increased cell division and fixation of DNA lesions as mutations.
机译:通过体内/体外突变测定法测量了三种多环芳香烃,7,12-二甲基苯并[a]蒽(DMBA),3-甲基胆碱(MC)和苯并[a] py(BP)的胎盘致突变性。关于这些化合物经胎盘诱变的胎儿敏感性和剂量反应特性从未量化。在目前的实验中,怀孕的叙利亚仓鼠在妊娠第12天就暴露于这些化合物中。二十四小时后,取出胎儿,并使其细胞在培养中表达5天。然后将它们播种以形成菌落,并通过白喉毒素进行突变选择。 0.2 mmol / kg(51.3 mg / kg)的DMBA诱导的突变频率为每个存活细胞1.56 x 10(-4)个突变体。这是历史控制值的598倍。 0.2 mmol / kg的DMBA的效力是1 mmol / kg的高度致突变性阳性对照乙基亚硝基脲的3.6倍。 DMBA还引起克隆效率的剂量依赖性增加,这与突变率高度相关。 BP和MC的效果不如DMBA,导致突变的增加分别是历史对照的31.6和17.7倍,而且突变率与克隆效率均无相关性。 DMBA作为胎盘诱变剂的特殊功效可能与它引起细胞分裂增加和DNA损伤固定突变的能力有关。

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