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Cyclic AMP Receptor Protein Regulates Pheromone-Mediated Bioluminescence at Multiple Levels in Vibrio fischeri ES114

机译:环AMP受体蛋白在费氏弧菌ES114的多个水平上调节信息素介导的生物发光。

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摘要

Bioluminescence in Vibrio fischeri ES114 is activated by autoinducer pheromones, and this regulation serves as a model for bacterial cell-cell signaling. As in other bacteria, pheromone concentration increases with cell density; however, pheromone synthesis and perception are also modulated in response to environmental stimuli. Previous studies suggested that expression of the pheromone-dependent bioluminescence activator LuxR is regulated in response to glucose by cyclic AMP (cAMP) receptor protein (CRP) (P. V. Dunlap and E. P. Greenberg, J. Bacteriol. 164:45–50, 1985; P. V. Dunlap and E. P. Greenberg, J. Bacteriol. 170:4040–4046, 1988; P. V. Dunlap, J. Bacteriol. 171:1199–1202, 1989; and W. F. Friedrich and E. P. Greenberg, Arch. Microbiol. 134:87–91, 1983). Consistent with this model, we found that bioluminescence in V. fischeri ES114 is modulated by glucose and stimulated by cAMP. In addition, a Δcrp mutant was ∼100-fold dimmer than ES114 and did not increase luminescence in response to added cAMP, even though cells lacking crp were still metabolically capable of producing luminescence. We further discovered that CRP regulates not only luxR but also the alternative pheromone synthase gene ainS. We found that His-tagged V. fischeri CRP could bind sequences upstream of both luxR and ainS, supporting bioinformatic predictions of direct regulation at both promoters. Luminescence increased in response to cAMP if either the ainS or luxR system was under native regulation, suggesting cAMP-CRP significantly increases luminescence through both systems. Finally, using transcriptional reporters in transgenic Escherichia coli, we elucidated two additional regulatory connections. First, LuxR-independent basal transcription of the luxI promoter was enhanced by CRP. Second, the effect of CRP on the ainS promoter depended on whether the V. fischeri regulatory gene litR was also introduced. These results suggest an integral role for CRP in pheromone signaling that goes beyond sensing cell density.
机译:费氏弧菌ES114中的生物发光被自动诱导素信息素激活,这种调节作用可作为细菌细胞信号传导的模型。像其他细菌一样,信息素的浓度随着细胞密度的增加而增加。然而,信息素的合成和感知也响应于环境刺激而被调节。先前的研究表明,信息素依赖性生物发光激活剂LuxR的表达受环状AMP(cAMP)受体蛋白(CRP)的葡萄糖调节(PV Dunlap和EP Greenberg,细菌学杂志164:45-50,1985; PV) Dunlap和EP Greenberg,J. Bacteriol。170:4040–4046,1988; PV Dunlap,J.Bacteriol。171:1199–1202,1989; WF Friedrich和EP Greenberg,Arch.Microbiol。134:87-91,1983 )。与该模型一致,我们发现费氏弧菌ES114中的生物发光受葡萄糖调节,并受cAMP刺激。此外,Δcrp突变体的亮度比ES114高约100倍,即使添加了cAMP的细胞也不能增加发光,即使缺少crp的细胞仍具有代谢能力,也可以产生发光。我们进一步发现,CRP不仅调节luxR,而且调节其他信息素合酶基因ainS。我们发现,His标记的费氏弧菌CRP可以结合luxR和ainS上游的序列,支持在两个启动子上直接调控的生物信息学预测。如果ainS或luxR系统处于天然调控下,则响应cAMP的发光会增加,这表明cAMP-CRP会显着增加通过这两个系统的发光。最后,使用转基因大肠杆菌中的转录报告基因,我们阐明了另外两个调控连接。首先,CRP增强了luxI启动子的不依赖LuxR的基础转录。其次,CRP对ainS启动子的影响取决于是否还引入了费氏弧菌调节基因litR。这些结果表明,CRP在信息素信号传导中起着不可或缺的作用,其作用超出了检测细胞密度。

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