首页> 美国卫生研究院文献>Nucleic Acids Research >The Drosophila transcription factor tramtrack (TTK) interacts with Trithorax-like (GAGA) and represses GAGA-mediated activation
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The Drosophila transcription factor tramtrack (TTK) interacts with Trithorax-like (GAGA) and represses GAGA-mediated activation

机译:果蝇转录因子电轨(TTK)与类胸甲藻(GAGA)相互作用并抑制GAGA介导的活化。

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摘要

In this study, we report the interaction of the Drosophila transcription factors Trithorax-like (GAGA) and tramtrack (TTK). This interaction is documented both in vitro, through GST pull-down assays, as well as in vivo, in yeast and Schneider S2 cells. GAGA and TTK share in common the presence of an N-terminal POZ/BTB domain that was found to be necessary and sufficient for GAGA–TTK interaction. Structural models that could account for this interaction are discussed. GAGA is known to activate the expression of many genes in Drosophila. On the other hand, TTK was proposed to act as a maternally provided repressor of several pair-rule genes, such as even-skipped (eve). As with many Drosophila genes, eve contains at its promoter region binding sites for GAGA and TTK. Here, in transient expression experiments, we showed that GAGA activates transcription from the eve stripe 2 promoter element and that TTK inhibits this GAGA-dependent activation. Repression by TTK of the eve promoter requires its activation by GAGA and depends on the presence of the POZ/BTB domains of TTK and GAGA. These results indicate that GAGA–TTK interaction contributes to the regulation of gene expression in Drosophila.
机译:在这项研究中,我们报告了果蝇转录因子类胸脯肉样(GAGA)和电车轨道(TTK)的相互作用。通过酵母和施耐德S2细胞的体外,通过GST下拉分析以及体内的这种相互作用都得到了证明。 GAGA和TTK共有一个N末端POZ / BTB域,这对于GAGA-TTK相互作用是必要的和充分的。讨论了可以解释这种相互作用的结构模型。已知GAGA可激活果蝇中许多基因的表达。另一方面,有人提议将TTK用作几对规则基因的母体提供的阻遏物,例如偶数跳过(eve)。与许多果蝇基因一样,eve在其启动子区域包含GAGA和TTK的结合位点。在这里,在瞬时表达实验中,我们表明GAGA激活了前夕条纹2启动子元件的转录,而TTK抑制了这种GAGA依赖性激活。 TTT对前夕启动子的抑制需要被GAGA激活,并取决于TTK和GAGA的POZ / BTB域的存在。这些结果表明,GAGA–TTK相互作用有助于果蝇中基因表达的调节。

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