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Human maintenance DNA (cytosine-5)-methyltransferase and p53 modulate expression of p53-repressed promoters

机译:人类维持DNA(胞嘧啶5)-甲基转移酶和p53调节p53抑制型启动子的表达

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摘要

DNA (cytosine-5)-methyltransferase (DNMT) 1 participates in transcriptional repression of genes by methylation-dependent and -independent mechanisms. Here, DNMT1 is shown to bind p53 and colocalize in the nucleus. DNMT1-mediated methylation is stimulated by p53 in vitro. Upon p53 induction, a reporter construct containing the antiapoptotic gene survivin promoter, which contains a natural p53 binding site, was methylated in WT HCT116 cells but not in DNMT1 null or p53 null cells. Endogenous survivin gene repression involves cooperation between DNMT1 and p53 and is relieved by introduction of DNMT1- or p53-specific small inhibitory RNA. DNMT1 null cells did not exhibit a significant repressive effect for p53 responsive survivin and cdc25C gene expression compared with the parental cells. Normal human fibroblasts also exhibited similar DNMT1- and p53-mediated methylation of the survivin promoter, suggesting cooperation between p53 and DNMT1 in gene silencing.
机译:DNA(cytosine-5)-methyltransferase(DNMT)1通过甲基化依赖性和非依赖性机制参与基因的转录抑制。在这里,DNMT1被显示与p53结合并在细胞核中共定位。 DNMT1介导的甲基化在体外受p53刺激。在p53诱导后,含有抗凋亡基因survivin启动子的报告基因构建体在野生型HCT116细胞中被甲基化,而在DNMT1 null或p53 null细胞中未被甲基化。内源性survivin基因抑制涉及DNMT1和p53之间的合作,并且通过引入DNMT1或p53特异性小抑制RNA得以缓解。与亲代细胞相比,DNMT1空细胞对p53反应性survivin和cdc25C基因表达没有明显的抑制作用。正常人成纤维细胞还表现出相似的DNMT1和p53介导的survivin启动子甲基化,表明p53和DNMT1在基因沉默中具有协同作用。

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