首页> 外文期刊>Human and Experimental Toxicology >Role of iron-dextran on 7,12-dimethylbenz(a) anthracene-initiated and croton oil-promoted cutaneous tumorigenesis in normal and pregnant mice.
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Role of iron-dextran on 7,12-dimethylbenz(a) anthracene-initiated and croton oil-promoted cutaneous tumorigenesis in normal and pregnant mice.

机译:右旋糖酐铁在正常小鼠和妊娠小鼠中对7,12-二甲基苯并(a)蒽引发和巴豆油促进的皮肤肿瘤发生的作用。

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摘要

Skin chemical carcinogenesis has been divided into the process of initiation, promotion and progression. Earlier, we showed the role of iron overload in the promotion stage of skin carcinogenesis. In this communication, we report that iron overload does not augment croton oil-mediated tumor promotion in 7,12-dimethylbenz(a)anthracene (DMBA)-initiated pregnant mice skin tumorigenesis. Virgin female Swiss mice were given 1 mg iron/mouse/day parenterally for 2 weeks to induce iron overload. After the last injection, a group of mice was left with male mice for 10 days. These animals showed an increase in cutaneous iron concentration as compared to normal mice. Papillomas were induced in mice skin by a single topical application of DMBA as initiator. A week after the initiation, promoting agent, croton oil was applied twice per week for 20 weeks. The appearance of the first tumor (papilloma), number of tumors/mouse and percentage incidence were recorded. When compared to the iron unloaded control and iron overload pregnant groups, the iron overload virgin animals showed an increased incidence of tumors. In iron overload virgin animals, tumors appeared earlier and also the numbers of tumors/mouse were significantly higher. However, in iron overload pregnant animals, diminished tumor incidence was observed and the numbers of tumors matched the result of normal pregnant animals. Our results show that iron overload in pregnant mice does not participate in the augmentation of DMBA- and croton oil-induced skin tumorigenesis.
机译:皮肤化学致癌作用已分为起始,促进和发展过程。之前,我们显示了铁超负荷在皮肤癌变促进阶段的作用。在此通讯中,我们报道了铁超负荷不会增加巴豆油介导的7,12-二甲基苯并(a)蒽(DMBA)引发的妊娠小鼠皮肤肿瘤发生。初次给瑞士的雌性小鼠经肠胃外注射1毫克铁/小鼠/天,持续2周,以诱导铁超负荷。最后一次注射后,将一组小鼠与雄性小鼠放置10天。与正常小鼠相比,这些动物表现出皮肤铁浓度的增加。通过单次局部应用DMBA作为引发剂在小鼠皮肤中诱导乳头状瘤。引发后一周,促进剂巴豆油每周两次应用20周。记录第一个肿瘤(乳头状瘤)的出现,肿瘤/小鼠数和发生率。与无铁对照组和铁超负荷孕妇组相比,处女铁超重动物的肿瘤发生率增加。在铁超负荷的原始动物中,肿瘤出现较早,并且肿瘤/小鼠的数量明显更高。然而,在铁超负荷的怀孕动物中,观察到肿瘤发生率降低,并且肿瘤数目与正常怀孕动物的结果相符。我们的结果表明,妊娠小鼠体内铁超载不参与DMBA和巴豆油诱导的皮肤肿瘤发生的增强。

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