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Dynamic hydroxymethylation of deoxyribonucleic acid marks differentiation-associated enhancers

机译:脱氧核糖核酸的动态羟甲基化标志着分化相关的增强子

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Enhancers are developmentally controlled transcriptional regulatory regions whose activities are modulated through histone modifications or histone variant deposition. In this study, we show by genome-wide mapping that the newly discovered deoxyribonucleic acid (DNA) modification 5-hydroxymethylcytosine (5hmC) is dynamically associated with transcription factor binding to distal regulatory sites during neural differentiation of mouse P19 cells and during adipocyte differentiation of mouse 3T3-L1 cells. Functional annotation reveals that regions gaining 5hmC are associated with genes expressed either in neural tissues when P19 cells undergo neural differentiation or in adipose tissue when 3T3-L1 cells undergo adipocyte differentiation. Furthermore, distal regions gaining 5hmC together with H3K4me2 and H3K27ac in P19 cells behave as differentiation-dependent transcriptional enhancers. Identified regions are enriched in motifs for transcription factors regulating specific cell fates such as Meis1 in P19 cells and PPARγ in 3T3-L1 cells. Accordingly, a fraction of hydroxymethylated Meis1 sites were associated with a dynamic engagement of the 5-methylcytosine hydroxylase Tet1. In addition, kinetic studies of cytosine hydroxymethylation of selected enhancers indicated that DNA hydroxymethylation is an early event of enhancer activation. Hence, acquisition of 5hmC in cell-specific distal regulatory regions may represent a major event of enhancer progression toward an active state and participate in selective activation of tissue-specific genes.
机译:增强子是发育控制的转录调节区域,其活性通过组蛋白修饰或组蛋白变体沉积来调节。在这项研究中,我们通过全基因组图谱显示,新发现的脱氧核糖核酸(DNA)修饰5-羟甲基胞嘧啶(5hmC)在小鼠P19细胞的神经分化和脂肪细胞分化过程中与远端调节位点的转录因子动态相关。小鼠3T3-L1细胞。功能注释显示,获得5hmC的区域与P19细胞进行神经分化时在神经组织中表达的基因或3T3-L1细胞进行脂肪细胞分化时在脂肪组织中表达的基因相关。此外,在P19细胞中与H3K4me2和H3K27ac一起获得5hmC的远端区域起着分化依赖性转录增强子的作用。识别出的区域富含转录因子,这些转录因子可调控特定的细胞命运,例如P19细胞中的Meis1和3T3-L1细胞中的PPARγ。因此,一部分羟甲基化的Meis1位点与5-甲基胞嘧啶羟化酶Tet1的动态结合有关。另外,对选定的增强子的胞嘧啶羟甲基化的动力学研究表明,DNA羟甲基化是增强子激活的早期事件。因此,在细胞特异性远端调控区中获得5hmC可能代表增强子向活动状态发展并参与组织特异性基因的选择性激活的主要事件。

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