首页> 美国卫生研究院文献>The EMBO Journal >Co-operative DNA binding by GAGA transcription factor requires the conserved BTB/POZ domain and reorganizes promoter topology.
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Co-operative DNA binding by GAGA transcription factor requires the conserved BTB/POZ domain and reorganizes promoter topology.

机译:通过GAGA转录因子进行的合作DNA结合需要保守的BTB / POZ结构域并重组启动子拓扑。

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摘要

The POZ domain is a conserved protein-protein interaction motif present in a variety of transcription factors involved in development, chromatin remodelling and human cancers. Here, we study the role of the POZ domain of the GAGA transcription factor in promoter recognition. Natural target promoters for GAGA typically contain multiple GAGA-binding elements. Our results show that the POZ domain mediates strong co-operative binding to multiple sites but inhibits binding to single sites. Protein cross-linking and gel filtration chromatography experiments established that the POZ domain is required for GAGA oligomerization into higher order complexes. Thus, GAGA oligomerization increases binding specificity by selecting only promoters with multiple sites. Electron microscopy revealed that GAGA binds to multiple sites as a large oligomer and induces bending of the promoter DNA. Our results indicate a novel mode of DNA binding by GAGA, in which a large GAGA complex binds multiple GAGA elements that are spread out over a region of a few hundred base pairs. We suggest a model in which the promoter DNA is wrapped around a GAGA multimer in a conformation that may exclude normal nucleosome formation.
机译:POZ结构域是存在于涉及发育,染色质重塑和人类癌症的各种转录因子中的保守的蛋白质-蛋白质相互作用基序。在这里,我们研究了GAGA转录因子的POZ域在启动子识别中的作用。 GAGA的天然靶标启动子通常包含多个GAGA结合元件。我们的结果表明,POZ域介导了对多个位点的强合作结合,但抑制了对单个位点的结合。蛋白质交联和凝胶过滤色谱实验确定,GAGA寡聚为高阶复合物需要POZ域。因此,GAGA寡聚通过仅选择具有多个位点的启动子来增加结合特异性。电子显微镜显示GAGA以大寡聚物形式结合到多个位点,并诱导启动子DNA弯曲。我们的结果表明了GAGA结合DNA的新模式,其中大型GAGA复合物结合了多个GAGA元素,这些元素分布在数百个碱基对的区域上。我们建议一个模型,其中启动子DNA以可能排除正常核小体形成的构象包裹在GAGA多聚体周围。

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