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Modulation of DNA binding properties of CCAAT/enhancer binding protein epsilon by heterodimer formation and interactions with NFkappaB pathway

机译:异源二聚体的形成以及与NFkappaB途径的相互作用调节CCAAT /增强子结合蛋白ε的DNA结合特性

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摘要

C/EBP epsilon is a transcription factor involved in myeloid cell differentiation. Along with C/EBP-α, -β, -γ, -δ, and -ζ, C/EBP-ϵ belongs to the family of CCAAT/enhancer binding proteins that are implicated in control of growth and differentiation of several cell lineages in inflammation and stress response. We have previously shown that C/EBP-ϵ preferentially binds DNA as a heterodimer with other C/EBP family members such as C/EBP-δ, CHOP (C/EBP-ζ), and the b-zip family protein ATF4. In this study, we define the consensus binding sites for C/EBP-ϵ dimers and C/EBP-ϵ–ATF4 heterodimers. We show that the activated NFkappaB pathway promotes interaction of the C/EBP-ϵ subunit with its cognate DNA binding site via interaction with RelA. RelA-C/EBP interaction is enhanced by phosphorylation of threonine at amino acid 75 and results in increased DNA binding compared with the wild-type nonphosphorylated C/EBP both in vitro and in vivo. We suggest that interaction of the activated NFkappaB pathway and C/EBP-ϵ may be important in selective activation of a subset of C/EBP-ϵ–responsive genes.
机译:C / EBP epsilon是参与髓样细胞分化的转录因子。与C /EBP-α,-β,-γ,-δ和-ζ一样,C / EBP- of属于CCAAT /增强子结合蛋白家族,与控制某些细胞系的生长和分化有关。炎症和压力反应。先前我们已经表明,C /EBP-β优先与其他C / EBP家族成员(例如C /EBP-δ,CHOP(C /EBP-ζ)和b-zip家族蛋白ATF4)结合作为异二聚体的DNA。在这项研究中,我们定义了C / EBP-ϵ二聚体和C / EBP-ϵATF4异二聚体的共有结合位点。我们表明,激活的NFkappaB途径通过与RelA的相互作用促进C /EBP-β亚基与其同源DNA结合位点的相互作用。与野生型非磷酸化C / EBP相比,在体内和体外,苏氨酸在氨基酸75处的磷酸化增强了RelA-C / EBP相互作用,并导致DNA结合增加。我们建议激活的NFkappaB途径与C / EBP-ϵ的相互作用可能对选择性激活C / EBP-ϵ反应基因的一个子集很重要。

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