低浓度的葡萄糖或胰岛素通过增加p27Kip1(一种细胞周期抑制蛋白)的表达,降低了长寿的Ames矮鼠罹患多种癌症的风险

I. Eto
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引用次数: 0

摘要

介绍。近年来,啮齿动物或人类肥胖或2型糖尿病中各种类型癌症发病率增加的分子生物学机制已基本得到解决。相比之下,纯合子长寿命Ames矮子小鼠中各种类型癌症发病率降低而不是增加的分子生物学机制仍未得到解决。目标。本研究的第一个目的是调查纯合子长寿艾姆斯矮小鼠癌症发病率的降低是否由于细胞周期抑制蛋白p27Kip1的表达增加而不是减少。第二个目标是调查纯合子长寿艾姆斯矮鼠癌症发病率的下降是否是由于葡萄糖或胰岛素水平的下降而不是增加。方法。为了达到这些目的,我们首先对p27Kip1蛋白的肝脏表达进行了免疫印迹分析。然后,我们使用体外培养的人乳腺癌细胞系进行荧光素酶报告质粒测定,以确定当葡萄糖或胰岛素浓度降低时,p27Kip1 mRNA的翻译起始活性是否增加。结果与结论。第一个目的的结果表明,p27Kip1蛋白在纯合子长寿Ames矮子小鼠的肝脏表达如预期的那样上调。我们还发现,较低浓度的葡萄糖或胰岛素增加了p27Kip1 mRNA的翻译起始活性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Lower Concentrations of Glucose or Insulin Decrease the Risk of Various Types of Cancer in the Long-Lived Ames Dwarf Mouse by Increasing the Expression of p27Kip1, a Cell-Cycle Repressor Protein
Introduction. The molecular biological mechanism of the increased incidence of the various types of cancer in obesity or type 2 diabetes in rodents or humans has largely been resolved in recent years. By contrast, the molecular biological mechanism of the decreased, not increased, incidence of the various types of cancer in the homozygous long-lived Ames dwarf mice still remains unresolved. Objective. The first objective of the present study was to investigate whether the decrease in the incidence of cancer in the homozygous long-lived Ames dwarf mice is due to the increase, not decrease, in the expression of p27Kip1, a cell cycle repressor protein. The second objective was to investigate whether the decrease in the incidence of cancer in the homozygous long-lived Ames dwarf mice is due to the decrease, not increase, in the levels of glucose or insulin. Methods. To achieve these objectives, we first performed western immunoblot analysis of the hepatic expression of p27Kip1 protein. We then performed, using a human breast cancer cell line in vitro, the luciferase reporter plasmid assay to determine whether the translation initiation activity of the p27Kip1 mRNA is increased when the concentrations of either glucose or insulin are decreased. Results and Conclusion. The results of the first objective indicated that the hepatic expression of p27Kip1 protein was up-regulated in the homozygous long-lived Ames dwarf mice as expected. We also found that the lower concentrations of glucose or insulin increased the translation initiation activity of the p27Kip1 mRNA.
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