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Pre-marked chromatin and transcription factor co-binding shape the pioneering activity of Foxa2

机译:预先标记的染色质和转录因子共同结合形成Foxa2的开拓性活动

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摘要

Pioneer transcription factors (PTF) can recognize their binding sites on nucleosomal DNA and trigger chromatin opening for recruitment of other non-pioneer transcription factors. However, critical properties of PTFs are still poorly understood, such as how these transcription factors selectively recognize cell type-specific binding sites and under which conditions they can initiate chromatin remodelling. Here we show that early endoderm binding sites of the paradigm PTF Foxa2 are epigenetically primed by low levels of active chromatin modifications in embryonic stem cells (ESC). Priming of these binding sites is supported by preferential recruitment of Foxa2 to endoderm binding sites compared to lineage-inappropriate binding sites, when ectopically expressed in ESCs. We further show that binding of Foxa2 is required for chromatin opening during endoderm differentiation. However, increased chromatin accessibility was only detected on binding sites which are synergistically bound with other endoderm transcription factors. Thus, our data suggest that binding site selection of PTFs is directed by the chromatin environment and that chromatin opening requires collaboration of PTFs with additional transcription factors.
机译:先锋转录因子(PTF)可以识别它们在核小体DNA上的结合位点,并触发染色质开放以募集其他非先锋转录因子。但是,对PTF的关键特性仍然知之甚少,例如这些转录因子如何选择性识别细胞类型特异性结合位点,以及它们在何种条件下可以引发染色质重塑。在这里,我们显示了范式PTF Foxa2的早期内胚层结合位点是通过胚胎干细胞(ESC)中低水平的活性染色质修饰在表观遗传上引发的。当在胚胎干细胞中异位表达时,与谱系不适当的结合位点相比,Foxa2优先募集到内胚层结合位点可以支持这些结合位点的启动。我们进一步表明Foxa2的结合是内胚层分化过程中染色质开放所必需的。然而,仅在与其他内胚层转录因子协同结合的结合位点上检测到染色质可及性增加。因此,我们的数据表明,PTF的结合位点选择受染色质环境的控制,染色质开放需要PTF与其他转录因子的协同作用。

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