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首页> 外文期刊>Journal of bacteriology >In Vivo DNA-Binding and Oligomerization Properties of the Shigella flexneri AraC-Like Transcriptional Regulator VirF as Identified by Random and Site-Specific Mutagenesis
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In Vivo DNA-Binding and Oligomerization Properties of the Shigella flexneri AraC-Like Transcriptional Regulator VirF as Identified by Random and Site-Specific Mutagenesis

机译:弗氏志贺氏菌AraC样转录调节因子VirF的体内DNA结合和低聚特性,通过随机和定点诱变确定

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摘要

In Shigella flexneri expression of the plasmid-encoded virulence genes is regulated via a complex mechanism involving both environmental signals and specific transactivators. The primary regulator protein, VirF, is a member of the AraC family of transcription factors and shares with other AraC-like proteins a conserved carboxy-terminal domain thought to be important for DNA binding. Random and site-directed mutagenesis of the virF gene encoding VirF yielded a number of mutations along the length of the protein which severely affected the ability of VirF to activate gene expression. The mutant proteins were shown to be affected in their ability to activate the virulence genes virB and icsA, both known to be regulated directly by VirF, as well as the virB-dependent virulence gene mxiC. Mutating key residues predicted to be important for DNA recognition had a significant negative effect, thereby suggesting that VirF interacts with its target sequence via two helix-turn-helix motifs. Two mutants that were dominant negative when coexpressed with the wild-type VirF protein were also isolated, indicating a role for protein-protein oligomerization in normal VirF function.
机译:志贺氏志贺菌中,质粒编码的毒力基因的表达是通过复杂的机制调节的,该机制涉及环境信号和特定的反式激活因子。主要的调节蛋白VirF是AraC转录因子家族的成员,与其他AraC样蛋白共享一个保守的羧基末端结构域,被认为对DNA结合很重要。编码VirF的 virF 基因的随机和定点诱变沿蛋白质长度产生许多突变,这严重影响了VirF激活基因表达的能力。突变蛋白的激活毒力基因 virB icsA 的能力受到影响,这两个基因都直接受VirF调控,而 virB 依赖性毒力基因 mxiC 。预测对DNA识别很重要的关键残基突变具有明显的负面影响,从而表明VirF通过两个螺旋-转-螺旋基序与其靶序列相互作用。还分离了两个与野生型VirF蛋白共表达时显性阴性的突变体,表明蛋白质-蛋白质寡聚在正常VirF功能中起作用。

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