Hatt J K, Youngman P
Department of Genetics, University of Georgia, Athens, Georgia 30602, USA.
J Bacteriol. 2000 Dec;182(24):6975-82. doi: 10.1128/JB.182.24.6975-6982.2000.
The Spo0A protein of Bacillus subtilis is a DNA-binding protein that is required for the expression of genes involved in the initiation of sporulation. Spo0A binds directly to and both activates and represses transcription from the promoters of several genes required during the onset of endospore formation. The C-terminal 113 residues are known to contain the DNA-binding activity of Spo0A. Previous studies identified a region of the C-terminal half of Spo0A that is highly conserved among species of endospore-forming Bacillus and Clostridium and which encodes a putative helix-turn-helix DNA-binding domain. To test the functional significance of this region and determine if this motif is involved in DNA binding, we changed three conserved residues, S210, E213, and R214, to Gly and/or Ala by site-directed mutagenesis. We then isolated and analyzed the five substitution-containing Spo0A proteins for DNA binding and sporulation-specific gene activation. The S210A Spo0A mutant exhibited no change from wild-type binding, although it was defective in spoIIA and spoIIE promoter activation. In contrast, both the E213G and E213A Spo0A variants showed decreased binding and completely abolished transcriptional activation of spoIIA and spoIIE, while the R214G and R214A variants completely abolished both DNA binding and transcriptional activation. These data suggest that these conserved residues are important for transcriptional activation and that the E213 residue is involved in DNA binding.
枯草芽孢杆菌的Spo0A蛋白是一种DNA结合蛋白,它是芽孢形成起始过程中相关基因表达所必需的。Spo0A直接结合并激活和抑制芽孢形成开始时所需的几个基因启动子的转录。已知C末端的113个残基包含Spo0A的DNA结合活性。先前的研究确定了Spo0A C末端一半的一个区域,该区域在形成芽孢的芽孢杆菌和梭菌物种中高度保守,并且编码一个假定的螺旋-转角-螺旋DNA结合结构域。为了测试该区域的功能重要性并确定该基序是否参与DNA结合,我们通过定点诱变将三个保守残基S210、E213和R214替换为甘氨酸和/或丙氨酸。然后,我们分离并分析了五种含替换的Spo0A蛋白的DNA结合和芽孢形成特异性基因激活情况。S210A Spo0A突变体与野生型结合没有变化,尽管它在spoIIA和spoIIE启动子激活方面存在缺陷。相比之下,E213G和E213A Spo0A变体的结合能力下降,spoIIA和spoIIE的转录激活完全丧失,而R214G和R214A变体则完全消除了DNA结合和转录激活。这些数据表明,这些保守残基对转录激活很重要,并且E213残基参与DNA结合。