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Insights into GATA-1-mediated gene activation versus repression via genome-wide chromatin occupancy analysis.

机译:通过全基因组染色质占有率分析了解GATA-1介导的基因激活与抑制之间的关系。

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The transcription factor GATA-1 is required for terminal erythroid maturation and functions as an activator or repressor depending on gene context. Yet its in vivo site selectivity and ability to distinguish between activated versus repressed genes remain incompletely understood. In this study, we performed GATA-1 ChIP-seq in erythroid cells and compared it to GATA-1-induced gene expression changes. Bound and differentially expressed genes contain a greater number of GATA-binding motifs, a higher frequency of palindromic GATA sites, and closer occupancy to the transcriptional start site versus nondifferentially expressed genes. Moreover, we show that the transcription factor Zbtb7a occupies GATA-1-bound regions of some direct GATA-1 target genes, that the presence of SCL/TAL1 helps distinguish transcriptional activation versus repression, and that polycomb repressive complex 2 (PRC2) is involved in epigenetic silencing of a subset of GATA-1-repressed genes. These data provide insights into GATA-1-mediated gene regulation in vivo.
机译:转录因子GATA-1是终端红系成熟所必需的,并根据基因的情况起激活剂或阻遏物的作用。然而,其体内位点选择性和区分激活基因与抑制基因的能力仍未完全了解。在这项研究中,我们在类红细胞中进行了GATA-1 ChIP-seq,并将其与GATA-1诱导的基因表达变化进行了比较。与非差异表达的基因相比,结合和差异表达的基因包含更多数量的GATA结合基序,回文GATA位点的频率更高,并且更接近转录起始位点。此外,我们表明转录因子Zbtb7a占据一些直接GATA-1靶基因的GATA-1结合区域,SCL / TAL1的存在有助于区分转录激活与抑制,并且涉及多梳抑制复合物2(PRC2) GATA-1抑制基因子集的表观遗传沉默这些数据提供了对体内GATA-1介导的基因调节的见解。

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