Miotto Benoit, Struhl Kevin
Department of Biological Chemistry and Molecular Pharmacology, Harvard Medical School, Boston, MA 02115, USA.
Mol Cell Biol. 2006 Aug;26(16):5969-82. doi: 10.1128/MCB.00696-06.
bZIP DNA-binding domains are targets for viral and cellular proteins that function as transcriptional coactivators. Here, we show that MBF1 and the related Chameau and HBO1 histone acetylases interact with distinct subgroups of bZIP proteins, whereas pX does not discriminate. Selectivity of Chameau and MBF1 for bZIP proteins is mediated by residues in the basic region that lie on the opposite surface from residues that contact DNA. Chameau functions as a specific coactivator for the AP-1 class of bZIP proteins via two arginine residues. A conserved glutamic acid/glutamine in the linker region underlies MBF1 specificity for a subgroup of bZIP factors. Chameau and MBF1 cannot synergistically coactivate transcription due to competitive interactions with the basic region, but either protein can synergistically coactivate with pX. Analysis of Jun derivatives that selectively interact with these coactivators reveals that MBF1 is crucial for the response to oxidative stress, whereas Chameau is important for the response to chemical and osmotic stress. Thus, the bZIP domain mediates selective interactions with coactivators and hence differential regulation of gene expression.
bZIP DNA结合结构域是作为转录共激活因子发挥作用的病毒和细胞蛋白的作用靶点。在此,我们表明MBF1以及相关的Chameau和HBO1组蛋白乙酰转移酶与不同亚组的bZIP蛋白相互作用,而pX则没有选择性。Chameau和MBF1对bZIP蛋白的选择性是由碱性区域中与接触DNA的残基位于相反表面的残基介导的。Chameau通过两个精氨酸残基作为AP-1类bZIP蛋白的特异性共激活因子。连接区中保守的谷氨酸/谷氨酰胺是MBF1对bZIP因子一个亚组具有特异性的基础。由于与碱性区域的竞争性相互作用,Chameau和MBF1不能协同共激活转录,但这两种蛋白中的任何一种都可以与pX协同共激活转录。对与这些共激活因子选择性相互作用的Jun衍生物的分析表明,MBF1对氧化应激反应至关重要,而Chameau对化学和渗透应激反应很重要。因此,bZIP结构域介导了与共激活因子的选择性相互作用,从而对基因表达进行差异调节。