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首页> 外文期刊>Molecular Microbiology >Membrane localization of the ToxR winged-helix domain is required for TcpP-mediated virulence gene activation in Vibrio cholerae
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Membrane localization of the ToxR winged-helix domain is required for TcpP-mediated virulence gene activation in Vibrio cholerae

机译:TcpP介导的霍乱弧菌毒力基因激活需要ToxR翼螺旋结构域的膜定位。

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摘要

ToxR is a bitopic membrane protein that controls virulence gene expression in Vibrio cholerae. Its cytoplasmic domain is homologous to the winged helix-turn-helix ('winged helix') DNA-binding/transcription activation domain found in a variety of prokaryotic and eukaryotic regulators, whereas its periplasmic domain is of ill-defined function. Several genes in V. cholerae are regulated by ToxR, but by apparently different mechanisms. Whereas ToxR directly controls the transcription of genes encoding two outer membrane proteins, OmpU and OmpT, it co-operates with a second membrane-localized transcription factor called TcpP to activate transcription of the gene encoding ToxT, which regulates transcription of cholera toxin (ctxAB) and the toxin-co-regulated pilus (tcp). To determine the requirements for gene activation by ToxR, different domains of the protein were analysed for their ability to control expression of toxT, ompU and ompT. Soluble forms of the cytoplasmic winged-helix domain regulated ompU and ompT gene expression properly but did not activate toxT transcription. Membrane localization of the winged helix was sufficient for both omp gene regulation and TcpP-dependent toxT transcription, irrespective of the type of periplasmic domain or even the presence of a periplasmic domain. These results suggest that (i) the major function for membrane localization of ToxR is for its winged-helix domain to co-operate with TcpP to activate transcription; (ii) the periplasmic domain of ToxR is not required for TcpP-dependent activation of toxT transcription; and (iii) membrane localization is not a strict requirement for DNA binding and transcription activation by ToxR. [References: 66]
机译:ToxR是一种双向膜蛋白,可控制霍乱弧菌中的毒力基因表达。其胞质结构域与在各种原核和真核调节子中发现的有翼螺旋-转-螺旋('有翼螺旋')DNA结合/转录激活域同源,而其周质结构域功能不清楚。霍乱弧菌的几个基因受ToxR调控,但受明显不同的机制调控。 ToxR直接控制编码两个外膜蛋白OmpU和OmpT的基因的转录,而ToxR与称为TcpP的第二个膜定位转录因子协同激活编码ToxT的基因的转录,后者调节霍乱毒素(ctxAB)的转录和毒素共调节菌毛(tcp)。为了确定通过ToxR激活基因的要求,分析了蛋白质的不同结构域控制toxT,ompU和ompT表达的能力。胞质有翼螺旋结构域的可溶性形式适当地调节了ompU和ompT基因的表达,但并未激活toxT转录。有翼螺旋的膜定位对于omp基因调控和TcpP依赖的toxT转录都是足够的,而与周质结构域的类型甚至周质结构域的存在无关。这些结果表明:(i)ToxR膜定位的主要功能是其有翼螺旋结构域与TcpP协同激活转录; (ii)依赖TcpP的toxT转录激活不需要ToxR的周质结构域; (iii)膜定位不是ToxR对DNA结合和转录激活的严格要求。 [参考:66]

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