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High Susceptibility of Analbuminemic Rats to Neurogenic Tumor Induction by Transplacental Administration of N‐Ethyl‐N‐nitrosourea

机译:N-乙基-N-亚硝基脲经胎盘给药对神经性肿瘤诱导的神经过敏性肿瘤的高度敏感性

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摘要

The susceptibilities of Nagase analbuminemic rats (NAR) and control Sprague‐Dawley rats (SDR) to N‐ethyl‐N‐nitrosourea (ENU) were compared. In Experiment I, the rats were given daily subcutaneous injections of 10 mg/kg of ENU for a week from 4 weeks of age. In Experiment II, mother rats were given a single subcutaneous injection of 60 mg/kg of ENU on day 17 of pregnancy and tumor development in their offspring was examined. In Experiment I, the incidence of neurogenic tumors was slightly, but not significantly, higher in NAR than in control rats. In Experiment II, the incidence of total tumors including neurogenic tumors was significantly higher in NAR (40/43, 93.0%) than in SDR (13/61, 21.3%). NAR showed particularly high susceptibility to induction of nenrogenic tumors (34/43, 79.1%) and renal tumors (15/43, 34.9%). In an attempt to elucidate the underlying mechanisms of the increased susceptibility of NAR to ENU, O6‐ethylguanine, a major premutagenic ethylated DNA adduct, was quantitated in fetal brain DNA of NAR and SDR after a pulse exposure to 60 mg/kg ENU. No significant difference in the initial formation or subsequent repair of O6‐ethylguanine was observed in the two strains, indicating that abnormality at some later stage(s) of chemical carcinogenesis may lead to the increased susceptibility of NAR to induction of neurogenic tumors.
机译:比较了Nagase贫血症大鼠(NAR)和对照Sprague-Dawley大鼠(SDR)对N-乙基-N-亚硝基脲(ENU)的敏感性。在实验I中,从4周龄开始,每天向大鼠皮下注射10 mg / kg ENU。在实验II中,在怀孕第17天给母鼠皮下注射60 mg / kg ENU,并检查其子代的肿瘤发展。在实验一中,NAR中神经源性肿瘤的发生率比对照组大鼠略高,但不明显。在实验II中,NAR(40/43,93.0%)中包括神经源性肿瘤在内的全部肿瘤的发生率显着高于SDR(13/61,21.3%)。 NAR对诱导神经原性肿瘤(34/43,79.1%)和肾肿瘤(15/43,34.9%)的敏感性特别高。为了阐明NAR对ENU敏感性增加的潜在机制,在脉冲暴露后,对NAR和SDR的胎儿脑DNA定量了主要的诱变前乙基化DNA加合物O 6 -乙基鸟嘌呤。至60 mg / kg ENU。在两个菌株中未观察到O 6 -乙基鸟嘌呤的初始形成或后续修复的显着差异,表明化学致癌作用的某些后期异常可能导致NAR敏感性增加。诱导神经源性肿瘤。

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