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The wing of the ToxR winged helix-turn-helix domain is required for DNA binding and activation of toxT and ompU

机译:DNA结合以及toxT和ompU的激活需要ToxR有翼螺旋-转-螺旋结构域的翼

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摘要

ToxR and TcpP, two winged helix-turn-helix (w-HTH) family transcription factors, co-activate expression of the toxT promoter in Vibrio cholerae. ToxT then directly regulates a number of genes required for virulence. In addition to co-activation of toxT, ToxR can directly activate the ompU promoter and repress the ompT promoter. Based on a previous study suggesting that certain wing residues of ToxR are preferentially involved in toxT co-activation compared to direct ompU activation, we employed alanine-scanning mutagenesis to determine which residues in the wing of ToxR are required for activation of each promoter. All of the ToxR wing residues tested that were critical for transcriptional activation of toxT and/or ompU were also critical for DNA binding. While some ToxR wing mutants had reduced interaction with TcpP, that reduced interaction did not correlate with a specific defect in toxT activation. Rather, such mutants also affected ompU activation and DNA binding. Based on these findings we conclude that the primary role of the wing of ToxR is to bind DNA, along with the DNA recognition helix of ToxR, and this function is required both for direct activation of ompU and co-activation of toxT.
机译:ToxR和TcpP,两个有翼螺旋转螺旋(w-HTH)家族转录因子,共同激活霍乱弧菌中toxT启动子的表达。然后,ToxT直接调节毒力所需的许多基因。除了共激活toxT,ToxR可以直接激活ompU启动子并抑制ompT启动子。根据先前的研究表明,与直接ompU激活相比,ToxR的某些侧翼残基优先参与toxT共激活,我们采用丙氨酸扫描诱变来确定ToxR侧翼中的哪些残基需要激活每个启动子。测试的对ToxT和/或ompU转录激活至关重要的所有ToxR侧翼残基对DNA结合也至关重要。尽管某些ToxR机翼突变体与TcpP的相互作用降低,但这种相互作用的降低与toxT激活中的特定缺陷无关。相反,此类突变体也影响了ompU激活和DNA结合。根据这些发现,我们得出结论,ToxR机翼的主要作用是结合DNA以及ToxR的DNA识别螺旋,并且该功能对于ompU的直接激活和toxT的共激活都是必需的。

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