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Human cancer stem cells are a target for cancer prevention using (?)-epigallocatechin gallate

机译:人类癌症干细胞是使用(?) - Epigallocatechin Gallate的癌症预防靶标

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Abstract Purpose Our previous experiments show that the main constituent of green-tea catechins, (?)-epigallocatechin gallate (EGCG), completely prevents tumor promotion on mouse skin initiated with 7,12-dimethylbenz(a)anthracene followed by okadaic acid and that EGCG and green tea extract prevent cancer development in a wide range of target organs in rodents. Therefore, we focused our attention on human cancer stem cells (CSCs) as targets of cancer prevention and treatment with EGCG. Methods The numerous reports concerning anticancer activity of EGCG against human CSCs enriched from cancer cell lines were gathered from a search of PubMed, and we hope our review of the literatures will provide a broad selection for the effects of EGCG on various human CSCs. Results Based on our theoretical study, we discuss the findings as follows: (1) Compared with the parental cells, human CSCs express increased levels of the stemness markers Nanog, Oct4, Sox2, CD44, CD133, as well as the EMT markers, Twist, Snail, vimentin, and also aldehyde dehydrogenase. They showed decreased levels of E-cadherin and cyclin D1. (2) EGCG inhibits the transcription and translation of genes encoding stemness markers, indicating that EGCG generally inhibits the self-renewal of CSCs. (3) EGCG inhibits the expression of the epithelial-mesenchymal transition phenotypes of human CSCs. (4) The inhibition of EGCG of the stemness of CSCs was weaker compared with parental cells. (5) The weak inhibitory activity of EGCG increased synergistically in combination with anticancer drugs. Conclusions Green tea prevents human cancer, and the combination of EGCG and anticancer drugs confers cancer treatment with tissue-agnostic efficacy.
机译:摘要目的我们以前的实验表明,绿茶儿茶素的主要成分(?) - EpigallocateChin Gallate(EGCG),完全防止了用7,12-二甲基(A)蒽的小鼠皮肤上的肿瘤促进,然后是冈田酸及此EGCG和绿茶提取物可防止啮齿动物中各种靶器官中的癌症发育。因此,我们将注意力集中在人体癌症干细胞(CSC)中作为癌症预防和用EGCG治疗的靶标。方法从癌细胞系中富集富含人类CSC的抗癌活动的大量报告都收集了对Pubmed的搜索,我们希望我们的文献审查将为EGCG对各种人类CSC的影响提供广泛的选择。结果基于我们的理论研究,我们讨论如下结果:(1)与亲本细胞相比,人类CSCs表达茎秆标志物纳米,Oct4,Sox2,CD44,CD133以及EMT标记的增加程度,以及EMT标记,蜗牛,皮蛋白,以及醛脱氢酶。它们显示出e-cadherin和cyclin d1水平降低。 (2)EGCG抑制编码茎标记物的基因的转录和翻译,表明EGCG通常抑制CSC的自我更新。 (3)EGCG抑制人CSCs的上皮 - 间充质转换表型的表达。 (4)与亲本细胞相比,CSCs茎茎的EGCG的抑制性较弱。 (5)EGCG的弱抑制活性与抗癌药物组合协同增长。结论绿茶可防止人类癌症,EGCG和抗癌药物的结合赋予癌症治疗组织 - 无症效果。

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