洋地黄素通过抑制活化t细胞驱动的c-MYC表达的核因子诱导癌细胞凋亡。

Q1 Environmental Science Journal of Carcinogenesis Pub Date : 2013-05-20 Print Date: 2013-01-01 DOI:10.4103/1477-3163.112268
Qing Feng Yang, Clifton L Dalgard, Ofer Eidelman, Catherine Jozwik, Bette S Pollard, Meera Srivastava, Harvey B Pollard
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引用次数: 20

摘要

背景:在体内和体外实验中,心脏苷类药物如洋地黄毒素可直接导致癌细胞凋亡。然而,连接心脏糖苷作用与细胞凋亡的机制尚不清楚。据报道,类似洋地黄毒素的化合物能够降低c-MYC的表达。此外,先前的研究表明,c-MYC的转录依赖于c-MYC启动子中的活化t细胞核因子(NFAT)结合位点。因此,我们假设NFAT可能介导洋地黄毒素对c-MYC mRNA信息的影响。材料和方法:我们选择在HeLa细胞中研究这一过程,其中8q24结构完整的c-MYC基因与人乳头瘤病毒18在所有整合位点共定位。结果:我们发现在洋地黄素治疗后的1(st) h内,c-MYC mRNA显著降低。随后是c-MYC蛋白的急剧丧失,caspase 3的激活,以及随后的凋亡细胞死亡。为了测试NFAT依赖机制,我们分析了洋地黄毒素对NFAT-荧光素酶表达系统的NFAT亚型依赖的自激活的影响。四种典型的NFAT异构体(1、2、3或4)对表达的药物依赖作用各不相同。对地黄霉素最敏感的NFAT异构体是NFAT1。利用c-MYC染色质免疫沉淀,我们发现洋地黄毒素抑制NFAT1与近端c-MYC启动子的相互作用。结论:这些结果表明洋地黄毒素的致癌活性包括抑制nfat驱动的c-MYC表达。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Digitoxin induces apoptosis in cancer cells by inhibiting nuclear factor of activated T-cells-driven c-MYC expression.

Background: Cardiac glycosides such as digitoxin have been shown to directly cause apoptotic death of cancer cells both in vitro, and in vivo. However, the mechanism connecting cardiac glycoside action to apoptosis is not known. It has been reported that compounds resembling digitoxin are able to reduce c-MYC expression. Furthermore, it has been previously shown that the transcription of c-MYC depends on nuclear factor of activated T-cells (NFAT) binding sites in the c-MYC promoter. We have therefore hypothesized that NFAT might mediate digitoxin effects on c-MYC mRNA message.

Materials and methods: We have chosen to study this process in HeLa cells where structurally intact c-MYC genes in 8q24 co-localize with human papilloma virus 18 at all integration sites.

Results: Here we show that within the 1(st) h following treatment with digitoxin, a significant reduction in c-MYC mRNA occurs. This is followed by a precipitous loss of c-MYC protein, activation of caspase 3, and subsequent apoptotic cell death. To test the NFAT-dependence mechanism, we analyzed the effects of digitoxin on NFAT isoform-dependent auto-activation of a NFAT-luciferase expression system. Drug dependent effects on expression varied according to each of the four canonical NFAT isoforms (1, 2, 3 or 4). The most digitoxin-sensitive NFAT isoform was NFAT1. Using c-MYC chromatin immune precipitation, we find that digitoxin inhibits interaction of NFAT1 with the proximal c-MYC promoter.

Conclusions: These results suggest that the carcinotoxic activity of digitoxin includes suppression of NFAT-driven c-MYC expression.

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来源期刊
Journal of Carcinogenesis
Journal of Carcinogenesis Environmental Science-Health, Toxicology and Mutagenesis
CiteScore
7.50
自引率
0.00%
发文量
0
审稿时长
15 weeks
期刊介绍: Journal of Carcinogenesis considers manuscripts in many areas of carcinogenesis and Chemoprevention. Primary areas of interest to the journal include: physical and chemical carcinogenesis and mutagenesis; processes influencing or modulating carcinogenesis, such as DNA repair; genetics, nutrition, and metabolism of carcinogens; the mechanism of action of carcinogens and modulating agents; epidemiological studies; and, the formation, detection, identification, and quantification of environmental carcinogens. Manuscripts that contribute to the understanding of cancer prevention are especially encouraged for submission
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