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首页> 外文期刊>Nutrition and Cancer: An International Journal >beta-Carotene fails to act as a tumor promoter, induces RAR expression, and prevents carcinoma formation in a two-stage model of skin carcinogenesis in male Sencar mice.
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beta-Carotene fails to act as a tumor promoter, induces RAR expression, and prevents carcinoma formation in a two-stage model of skin carcinogenesis in male Sencar mice.

机译:在雄性Sencar小鼠的皮肤癌变的两阶段模型中,β-胡萝卜素不能充当肿瘤启动子,诱导RAR表达并阻止癌的形成。

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Clinical trials have shown a significant increase in incidence of lung cancer among smokers and asbestos workers supplemented with beta-carotene, suggesting a tumor-promoting activity for this agent. We set out to test possible tumor-promoting and chemopreventive activities of dietary and topical beta-carotene in the two-stage 7,12-dimethylbenz[a]anthracene-12-O-tetradecanoylphorbol 13-acetate (TPA) model of mouse skin carcinogenesis. In the first study, the effects of three levels of dietary beta-carotene (6, 60, and 600 micrograms/g purified diet containing no other retinoid or carotenoid) were assessed over a period of 42 weeks. Carcinoma yield was reduced by approximately 50% in the 600 micrograms/g diet group (mean 0.22 carcinomas/mouse) compared with the 6 micrograms/g diet group (mean 0.44 carcinomas/mouse, p = 0.003). The 60 micrograms/g diet group showed a pattern of inhibition similar to the 600 micrograms/g diet group. A protective effect (25% reduction) of beta-carotene (in the 600 micrograms/g diet group) on papilloma formation was also found. However, the intermediate 60 micrograms/g diet group showed the same incidence as the low 6 micrograms/g diet group. This points to a lack of correlation between papilloma and carcinoma incidence, as we also found in previous work on dietary retinoids and carotenoids. The purpose of the second study was to assess whether topical beta-carotene (2 micrograms) has tumor-promoting or chemopreventive activity in the two-stage protocol. In the absence of TPA, beta-carotene had no significant tumor-promoting activity. Instead, papilloma yield induced by TPA was decreased by topical beta-carotene from an average of 20 to approximately 10 papillomas/mouse (p = 2.5 x 10(-7)). The effect of topical beta-carotene persisted beyond the treatment period (Week 24) until the termination of the study at Week 42. Western blot analysis of mouse skin extracts showed that topical beta-carotene upregulated retinoic acid receptor-alpha and -gamma expression in the dorsal skin. This finding suggests that beta-carotene may work as a chemopreventive agent by upregulating the expression of retinoid receptors in mouse skin. In conclusion, our data show that beta-carotene prevents skin carcinoma formation, induces retinoic acid receptor expression, and fails to act as a tumor promoter in the two-stage model of skin tumorigenesis.
机译:临床试验表明,在吸烟者和石棉工人中,补充了β-胡萝卜素的肺癌发病率显着增加,表明该药具有促进肿瘤的活性。我们着手测试两阶段的7,12-二甲基苯并[a]蒽-12-O-十四烷酰佛波醇13-乙酸(TPA)模型在小鼠皮肤癌变中的饮食和局部β-胡萝卜素的促肿瘤和化学预防活性。 。在第一个研究中,在42周的时间内评估了三种饮食水平的β-胡萝卜素(6、60和600微克/克不含其他类维生素A或类胡萝卜素的纯饮食)的影响。与6微克/克饮食组(平均0.44癌/小鼠,p = 0.003)相比,600微克/克饮食组(平均0.22癌/小鼠)的癌变率降低了约50%。 60微克/克饮食组显示出与600微克/克饮食组相似的抑制模式。还发现了β-胡萝卜素(在600微克/克饮食组中)对乳头状瘤的形成有保护作用(降低了25%)。但是,中度60毫克/克饮食组与低6毫克/克饮食组的发病率相同。这表明乳头状瘤和癌的发病率之间缺乏相关性,正如我们在以前关于饮食类维生素A和类胡萝卜素的研究中也发现的那样。第二项研究的目的是评估局部β-胡萝卜素(2微克)在两个阶段的方案中是否具有促肿瘤或化学预防活性。在没有TPA的情况下,β-胡萝卜素没有明显的促肿瘤活性。取而代之的是,局部β-胡萝卜素将TPA诱导的乳头状瘤产量从平均20降低到大约10个乳头状瘤/小鼠(p = 2.5 x 10(-7))。局部β-胡萝卜素的作用一直持续到治疗期(第24周),直到研究在第42周终止。小鼠皮肤提取物的Western印迹分析表明,局部β-胡萝卜素上调了视黄酸受体α和γ的表达。背部皮肤。这一发现表明,β-胡萝卜素可能通过上调小鼠皮肤中类维生素A受体的表达而起到化学预防剂的作用。总之,我们的数据表明,β-胡萝卜素可预防皮肤癌的形成,诱导视黄酸受体的表达,并且在皮肤肿瘤发生的两阶段模型中不能充当肿瘤的启动子。

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