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中介复合物亚基 Med19 直接结合 GATA 转录因子,并且与 Med1 一起调控 GATA 驱动的基因表达。

Mediator complex subunit Med19 binds directly GATA transcription factors and is required with Med1 for GATA-driven gene regulation .

机构信息

Centre de Biologie Integrative CBD, UMR5547 CNRS/UPS, Université de Toulouse, Toulouse Cedex, France.

Inserm, CHU Lille, Institut Pasteur de Lille, CNRS ERL 9002 Integrative Structural Biology, Université Lille, Lille, France.

出版信息

J Biol Chem. 2020 Sep 25;295(39):13617-13629. doi: 10.1074/jbc.RA120.013728. Epub 2020 Jul 31.

Abstract

The evolutionarily conserved multiprotein Mediator complex (MED) serves as an interface between DNA-bound transcription factors (TFs) and the RNA Pol II machinery. It has been proposed that each TF interacts with a dedicated MED subunit to induce specific transcriptional responses. But are these binary partnerships sufficient to mediate TF functions? We have previously established that the Med1 Mediator subunit serves as a cofactor of GATA TFs in , as shown in mammals. Here, we observe mutant phenotype similarities between another subunit, Med19, and the GATA TF Pannier (Pnr), suggesting functional interaction. We further show that Med19 physically interacts with the Drosophila GATA TFs, Pnr and Serpent (Srp), and through their conserved C-zinc finger domains. Moreover, Med19 loss of function experiments or indicate that it is required for Pnr- and Srp-dependent gene expression, suggesting general GATA cofactor functions. Interestingly, Med19 but not Med1 is critical for the regulation of all tested GATA target genes, implying shared or differential use of MED subunits by GATAs depending on the target gene. Lastly, we show a direct interaction between Med19 and Med1 by GST pulldown experiments indicating privileged contacts between these two subunits of the MED middle module. Together, these findings identify Med19/Med1 as a composite GATA TF interface and suggest that binary MED subunit-TF partnerships are probably oversimplified models. We propose several mechanisms to account for the transcriptional regulation of GATA-targeted genes.

摘要

进化保守的多蛋白 Mediator 复合物 (MED) 作为 DNA 结合转录因子 (TFs) 和 RNA Pol II 机器之间的接口。有人提出,每个 TF 都与特定的 MED 亚基相互作用,以诱导特定的转录反应。但是这些二元伙伴关系是否足以介导 TF 的功能?我们之前已经证明,Med1 Mediator 亚基在果蝇中充当 GATA TF 的辅助因子,正如在哺乳动物中所观察到的。在这里,我们观察到另一个亚基 Med19 与 GATA TF Pannier (Pnr) 之间存在类似的突变表型,表明存在功能相互作用。我们进一步表明,Med19 与果蝇 GATA TFs Pnr 和 Serpent (Srp) 物理相互作用,并且通过它们保守的 C-锌指结构域。此外,Med19 功能丧失实验表明,它是 Pnr 和 Srp 依赖的基因表达所必需的,这表明它具有普遍的 GATA 辅助因子功能。有趣的是,Med19 而不是 Med1 对于所有测试的 GATA 靶基因的调控都是必需的,这意味着 GATAs 根据靶基因共享或差异地使用 MED 亚基。最后,我们通过 GST 下拉实验显示了 Med19 和 Med1 之间的直接相互作用,表明这两个 MED 中间模块的亚基之间存在特权接触。总之,这些发现确定了 Med19/Med1 作为一个复合的 GATA TF 界面,并表明二元 MED 亚基-TF 伙伴关系可能过于简化。我们提出了几种机制来解释 GATA 靶向基因的转录调控。

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