首页> 外文期刊>Molecular Carcinogenesis >Mammary glands of sexually immature rats are more susceptible than those of mature rats to the carcinogenic, lethal, and mutagenic effects of N-nitroso-N-methylurea.
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Mammary glands of sexually immature rats are more susceptible than those of mature rats to the carcinogenic, lethal, and mutagenic effects of N-nitroso-N-methylurea.

机译:性未成熟大鼠的乳腺比成熟大鼠的乳腺更易受到N-亚硝基-N-甲基脲的致癌,致死和致突变作用。

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摘要

Knowing that the prepubertal period is a time of enhanced susceptibility for radiation-induced human breast cancer, we used the Fischer 344 rat model to explore the age-differential susceptibility of the mammary gland to the carcinogenic, lethal, and mutagenic effects of two structurally diverse chemical carcinogens, N-nitroso-N-methylurea (NMU), and 7,12-dimethylbenz(a)anthracene (DMBA). Mammary carcinoma incidences and multiplicities were significantly greater in immature than mature NMU-treated rats while mammary carcinoma incidences and multiplicities were significantly lower in immature than mature DMBA-treated rats. The survival of mammary clonogens of mature NMU-treated rats in limiting dilution transplantation assays was greater than that of the survival of mammary clonogens of immature NMU-treated rats. No differences were found in the survival of mammary cells from immature and mature rats exposed to DMBA. Although there were no mutation spectra differences, mammary epithelial cells of immature NMU-treated rats had greater mutation frequencies than those of mature NMU-treated rats. Together these results support the hypothesis that the mammary gland of immature rats is more susceptible to the carcinogenic, lethal, and mutagenic effects of alkylating agents represented by NMU in a carcinogen-class-specific manner. Further, the results suggest the importance of mechanistic and epidemiological studies of the susceptibility of the prepubertal breast to specific carcinogens such as alkylating agents.
机译:知道青春期前是辐射诱发的人类乳腺癌易感性增强的时期,我们使用Fischer 344大鼠模型探索了乳腺对两种结构多样的致癌,致死和诱变作用的年龄差异敏感性。化学致癌物,N-亚硝基-N-甲基脲(NMU)和7,12-二甲基苯并(a)蒽(DMBA)。未成熟的乳腺癌的发病率和多重性显着高于成熟的NMU处理的大鼠,而未成熟的乳腺癌的发病率和多重性显着低于成熟的DMBA处理的大鼠。在有限稀释移植试验中,成熟的NMU处理的大鼠的乳腺克隆形成物的存活率大于未成熟的NMU处理的大鼠的乳腺克隆形成物的存活率。暴露于DMBA的未成熟和成熟大鼠的乳腺细胞存活率无差异。尽管没有突变谱差异,但是未成熟的NMU处理的大鼠的乳腺上皮细胞具有比成熟的NMU处理的大鼠更大的突变频率。这些结果共同支持了以下假设:未成熟大鼠的乳腺更易受以NMU代表的致癌物类特异性方式的烷化剂的致癌,致死和致突变作用。此外,结果表明青春期前乳房对特定致癌物(如烷化剂)敏感性的机械和流行病学研究的重要性。

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