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Assembly of the Hap2p/Hap3p/Hap4p/Hap5p-DNA Complex in Saccharomyces cerevisiae

机译:在酿酒酵母中的Hap2p / Hap3p / Hap4p / Hap5p-DNA复合体的组装

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The CCAAT-binding factor (CBF) is an evolutionarily conserved multimeric transcriptional activator in eukaryotes. In Saccharomyces cerevisiae, the CCAAT-binding factor is composed of four subunits, termed Hap2p, Hap3p, Hap4p, and Hap5p. The Hap2p/Hap3p/Hap5p heterotrimer is the DNA-binding component of the complex that binds to the consensus 5′-CCAAT-3′ sequence in the promoter of target genes. The Hap4p subunit contains the transcriptional activation domain necessary for stimulating transcription after interacting with Hap2p/Hap3p/Hap5p. In this report, we demonstrate that Hap2p, Hap3p, and Hap5p assemble via a one-step pathway requiring all three subunits simultaneously, as opposed to the mammalian CCAAT-binding factor which has been shown to assemble via a two-step pathway with CBF-A (Hap3p homolog) and CBF-C (Hap5p homolog) forming a stable dimer before CBF-B (Hap2p homolog) can interact. We have also found that the interaction of Hap4p with Hap2p/Hap3p/Hap5p requires DNA binding as a prerequisite. To further understand the protein-protein and protein-DNA interactions of this transcription factor, we identified the minimal domain of Hap4p necessary for interaction with the Hap2p/Hap3p/Hap5p-DNA complex, and we demonstrate that this domain is sufficient to complement the respiratory deficiency of a hap4Δ mutant and activate transcription when fused with the VP16 activation domain. These studies provide a further understanding of the assembly of the yeast CCAAT-binding factor at target promoters and raise a number of questions concerning the protein-protein and protein-DNA interactions of this multisubunit transcription factor.
机译:CCAAT结合因子(CBF)是真核生物中进化保守的多聚体转录激活因子。在酿酒酵母中,CCAAT结合因子由四个亚基组成,分别称为Hap2p,Hap3p,Hap4p和Hap5p。 Hap2p / Hap3p / Hap5p异源三聚体是复合物的DNA结合成分,可与靶基因启动子中的共有5'-CCAAT-3'序列结合。 Hap4p亚基包含与Hap2p / Hap3p / Hap5p相互作用后刺激转录所必需的转录激活域。在这份报告中,我们证明了Hap2p,Hap3p和Hap5p通过一步途径同时需要所有三个亚基进行组装,而哺乳动物CCAAT结合因子已被证明通过CBF-的两步途径进行组装A(Hap3p同源物)和CBF-C(Hap5p同源物)在CBF-B(Hap2p同源物)可以相互作用之前形成稳定的二聚体。我们还发现,Hap4p与Hap2p / Hap3p / Hap5p的相互作用需要结合DNA作为先决条件。为了进一步了解该转录因子的蛋白质-蛋白质和蛋白质-DNA相互作用,我们鉴定了与Hap2p / Hap3p / Hap5p-DNA复合体相互作用所必需的Hap4p最小域,并且我们证明了该域足以补充呼吸道突变体缺乏hap4Δ,并在与VP16激活域融合时激活转录。这些研究提供了对酵母CCAAT结合因子在靶标启动子处的组装的进一步理解,并引起了有关该多亚基转录因子的蛋白质-蛋白质和蛋白质-DNA相互作用的许多问题。

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