Hatada E N, Nieters A, Wulczyn F G, Naumann M, Meyer R, Nucifora G, McKeithan T W, Scheidereit C
Max-Planck-Institut fuer Molekulare Genetik, Otto-Warburg-Laboratorium, Berlin-Dahlem, Federal Republic of Germany.
Proc Natl Acad Sci U S A. 1992 Mar 15;89(6):2489-93. doi: 10.1073/pnas.89.6.2489.
The inducible pleiotropic transcription factor NF-kappa B is composed of two subunits, p50 and p65. The p50 subunit is encoded on the N-terminal half of a 105-kDa open reading frame and contains a rel-like domain. To date, no function has been described for the C-terminal portion. We show here that the C-terminal half of p105, when expressed as a separate molecule, binds to p50 and can rapidly disrupt protein-DNA complexes of p50 or native NF-kappa B. Deletion analysis of this precursor-derived inhibitor activity indicated a domain containing ankyrin-like repeats as necessary for inhibition. The protooncogene bcl-3, which contains seven ankyrin repeats, can equally inhibit p50 DNA binding. These observations identify bcl-3 as an inhibitor of NF-kappa B and strongly suggest that the ankyrin repeats in these factors are involved in protein-protein interactions with the rel-like domain of p50. Comparison with other ankyrin repeat-containing proteins suggests that a subclass of these proteins acts as regulators of rel-like transcription factors.
可诱导的多效转录因子核因子-κB由两个亚基p50和p65组成。p50亚基由一个105 kDa开放阅读框的N端一半编码,并包含一个类rel结构域。迄今为止,尚未描述其C端部分的功能。我们在此表明,p105的C端一半作为一个单独的分子表达时,可与p50结合,并能迅速破坏p50或天然核因子-κB的蛋白质-DNA复合物。对这种前体衍生的抑制活性进行缺失分析表明,一个含有锚蛋白样重复序列的结构域是抑制所必需的。原癌基因bcl-3含有七个锚蛋白重复序列,同样可抑制p50与DNA的结合。这些观察结果确定bcl-3为核因子-κB的一种抑制剂,并强烈表明这些因子中的锚蛋白重复序列参与了与p50类rel结构域的蛋白质-蛋白质相互作用。与其他含锚蛋白重复序列的蛋白质进行比较表明,这些蛋白质的一个亚类作为类rel转录因子的调节因子发挥作用。
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