Liptay S, Schmid R M, Nabel E G, Nabel G J
Department of Internal Medicine, University of Michigan Medical Center, Ann Arbor 48109-0650.
Mol Cell Biol. 1994 Dec;14(12):7695-703. doi: 10.1128/mcb.14.12.7695-7703.1994.
NF-kappa B is an inducible transcription factor complex which regulates the expression of a variety of genes which are involved in the immune, inflammatory, and acute-phase responses. The maintenance of NF-kappa B activity in stimulated cells requires ongoing protein synthesis, suggesting several modes of regulation. In this report, we have characterized the transcriptional regulation of one family member, NF-kappa B2. The genomic structure and sequence of NF-kappa B2 revealed the presence of two promoters and at least four kappa B regulatory elements, which mediate responsiveness to phorbol myristate acetate and tumor necrosis factor alpha. Similar to other NF-kappa B family members, NF-kappa B2 is positively autoregulated. In contrast to other family members, we find that kappa B elements in the NFKB2 promoter can also mediate transcriptional repression in the absence of NF-kappa B. We identified a nuclear complex which binds specifically to a subset of kappa B-related sites but not to the canonical kappa B element. Because of its putative inhibitory or repressive effect, this binding activity has been termed Rep-kappa B. This mechanism of repressing basal NF-kappa B2 transcription in an inactivated state enables the cell to tightly control NF-kappa B2 activity. These data demonstrate that a novel mode of kappa B-dependent regulation is mediated by specific kappa B sites in the NFKB2 promoter.
核因子κB是一种可诱导的转录因子复合物,它调控多种参与免疫、炎症和急性期反应的基因的表达。在受刺激的细胞中维持核因子κB的活性需要持续的蛋白质合成,这提示了几种调控模式。在本报告中,我们对一个家族成员核因子κB2的转录调控进行了表征。核因子κB2的基因组结构和序列显示存在两个启动子和至少四个κB调控元件,它们介导对佛波酯肉豆蔻酸酯和肿瘤坏死因子α的反应。与其他核因子κB家族成员相似,核因子κB2存在正向自身调节。与其他家族成员不同的是,我们发现核因子κB2启动子中的κB元件在没有核因子κB的情况下也能介导转录抑制。我们鉴定出一种核复合物,它能特异性结合κB相关位点的一个子集,但不结合典型的κB元件。由于其假定的抑制作用,这种结合活性被称为Rep-κB。这种在失活状态下抑制基础核因子κB2转录的机制使细胞能够严格控制核因子κB2的活性。这些数据表明,核因子κB2启动子中的特定κB位点介导了一种新的κB依赖性调控模式。
