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Genomic screening for genes upregulated by demethylation revealed novel targets of epigenetic silencing in breast cancer

机译:通过去甲基化上调基因的基因组筛选揭示了乳腺癌表观遗传沉默的新靶标

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Breast cancer arises through the accumulation of multiple genetic alterations and epigenetic changes such as methylation, which silences gene expression in a variety of cancers. In the present study, we applied genomic screening to identify genes upregulated by the demethylating agent 5-aza-2′-deoxycytidine (DAC) in a human breast cancer cell line (MCF7). We identified 288 genes upregulated and 29 genes downregulated more than fivefold after treatment with DAC, and gene ontology analyses revealed the genes to be involved in immune responses, apoptosis, and cell differentiation. In addition, real-time PCR analysis of ten genes silenced in MCF7 cells confirmed that they are upregulated by DAC, while bisulfite-pyrosequencing analysis confirmed that nine of those genes were silenced by methylation. We also found that treating MCF7 cells with DAC restored induction of DFNA5 by p53, as well as by two other p53 family genes, p63γ and p73β. Introduction of NTN4 into MCF7 cells suppressed cell growth, indicating that NTN4 has tumor suppressive activity. In primary breast cancers, we detected cancer-specific methylation of NTN4, PGP9.5, and DKK3, suggesting that methylation of these genes could be useful markers for diagnosis of breast cancer. Thus, DNA methylation appears to be a common event in breast cancer, and the genes silenced by methylation could be useful targets for both diagnosis and therapy.
机译:乳腺癌是通过多种遗传变异和表观遗传变化(例如甲基化)的积累而产生的,而甲基化使多种癌症中的基因表达沉默。在本研究中,我们应用基因组筛选来鉴定人乳腺癌细胞系(MCF7)中由脱甲基剂5-氮杂2'-脱氧胞苷(DAC)上调的基因。我们发现DAC处理后,有288个基因被上调,而29个基因被下调了5倍以上,而基因本体分析显示这些基因与免疫反应,细胞凋亡和细胞分化有关。此外,实时PCR分析了MCF7细胞中沉默的10个基因,证实它们被DAC上调,而亚硫酸氢盐-焦磷酸测序分析证实了其中9个基因被甲基化沉默。我们还发现,用DAC处理MCF7细胞可恢复p53以及其他两个p53家族基因p63γ和p73β对DFNA5的诱导。 NTN4导入MCF7细胞抑制细胞生长,表明NTN4具有肿瘤抑制活性。在原发性乳腺癌中,我们检测到了NTN4,PGP9.5和DKK3的癌症特异性甲基化,这表明这些基因的甲基化可能是诊断乳腺癌的有用标记。因此,DNA甲基化似乎是乳腺癌中的常见事件,而甲基化沉默的基因可能是诊断和治疗的有用靶标。

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