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首页> 外文期刊>Nucleic Acids Research >c-Jun/c-Fos heterodimers regulate cellular genes via a newly identified class of methylated DNA sequence motifs
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c-Jun/c-Fos heterodimers regulate cellular genes via a newly identified class of methylated DNA sequence motifs

机译:c-Jun / c-Fos异二聚体通过新鉴定的一类甲基化DNA序列基序来调控细胞基因

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摘要

CpG methylation in mammalian DNA is known to interfere with gene expression by inhibiting the binding of transactivators to their cognate sequence motifs or recruiting proteins involved in gene repression. An Epstein-Barr virus-encoded transcription factor, Zta, was the first example of a sequence-specific transcription factor that preferentially recognizes and selectively binds DNA sequence motifs with methylated CpG residues, reverses epigenetic silencing and activates gene transcription. The DNA binding domain of Zta is homologous to c-Fos, a member of the cellular AP-1 (activator protein 1) transcription factor family, which regulates cell proliferation and survival, apoptosis, transformation and oncogenesis. We have identified a novel AP-1 binding site termed meAP-1, which contains a CpG dinucleotide. If methylated, meAP-1 sites are preferentially bound by the AP-1 heterodimer c-Jun/c-Fos in vitro and in cellular chromatin in vivo. In activated human primary B cells, c-Jun/c-Fos locates to these methylated elements in promoter regions of transcriptionally activated genes. Reminiscent of the viral Zta protein, c-Jun/c-Fos is the first identified cellular member of the AP-1 family of transactivators that can induce expression of genes with methylated, hence repressed promoters, reversing epigenetic silencing.
机译:已知哺乳动物DNA中的CpG甲基化可通过抑制反式激活因子与其同源序列基序的结合或募集参与基因抑制的蛋白质来干扰基因表达。用爱泼斯坦-巴尔病毒编码的转录因子Zta是序列特异性转录因子的第一个例子,该序列优先识别并选择性地结合具有甲基化CpG残基的DNA序列基序,逆转表观遗传沉默并激活基因转录。 Zta的DNA结合结构域与c-Fos(细胞AP-1(激活蛋白1)转录因子家族的成员)同源,后者调节细胞的增殖和存活,凋亡,转化和癌变。我们已经确定了一个新的AP-1结合位点,称为meAP-1,其中包含一个CpG二核苷酸。如果甲基化,则meAP-1位点在体外和体内细胞染色质中优先被AP-1异二聚体c-Jun / c-Fos结合。在激活的人原代B细胞中,c-Jun / c-Fos位于转录激活基因的启动子区域中的这些甲基化元件上。 c-Jun / c-Fos使人联想到病毒Zta蛋白,它是AP-1反式激活因子家族中第一个鉴定出的细胞成员,可以诱导甲基化的基因表达,从而抑制了启动子,从而逆转了表观遗传沉默。

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