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Characterization of a Novel Two-Component Regulatory System HptRS the Regulator for the Hexose Phosphate Transport System in Staphylococcus aureus

机译:新型的两组分调节系统HptRS金黄色葡萄球菌中的磷酸磷酸盐运输系统调节剂的表征

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摘要

Hexose phosphate is an important carbon source within the cytoplasm of host cells. Bacterial pathogens that invade, survive, and multiply within various host epithelial cells exploit hexose phosphates from the host cytoplasm through the hexose phosphate transport (HPT) system to gain energy and synthesize cellular components. In Escherichia coli, the HPT system consists of a two-component regulatory system (UhpAB) and a phosphate sensor protein (UhpC) that tightly regulate expression of a hexose phosphate transporter (UhpT). Although growing evidence suggests that Staphylococcus aureus also can invade, survive, and multiply within various host epithelial cells, the genetic elements involved in the HPT system in S. aureus have not been characterized yet. In this study, we identified and characterized the HPT system in S. aureus that includes the hptRS (a novel two-component regulatory system), the hptA (a putative phosphate sensor), and the uhpT (a hexose phosphate transporter) genes. The hptA, hptRS, and uhpT markerless deletion mutants were generated by an allelic replacement method using a modified pMAD-CM-GFPuv vector system. We demonstrated that both hptA and hptRS are required to positively regulate transcription of uhpT in response to extracellular phosphates, such as glycerol-3-phosphate (G3P), glucose-6-phosphate (G6P), and fosfomycin. Mutational studies revealed that disruption of the hptA, hptRS, or uhpT gene impaired the growth of bacteria when the available carbon source was limited to G6P, impaired survival/multiplication within various types of host cells, and increased resistance to fosfomycin. The results of this study suggest that the HPT system plays an important role in adaptation of S. aureus within the host cells and could be an important target for developing novel antistaphylococcal therapies.
机译:磷酸己糖是宿主细胞胞质内的重要碳源。在各种宿主上皮细胞内侵袭,存活和繁殖的细菌病原体通过磷酸己糖转运(HPT)系统利用宿主细胞质中的磷酸己糖来获取能量并合成细胞成分。在大肠杆菌中,HPT系统由两组分调节系统(UhpAB)和磷酸盐传感器蛋白(UhpC)组成,后者可以严格调节磷酸己糖转运蛋白(UhpT)的表达。尽管越来越多的证据表明,金黄色葡萄球菌也可以在各种宿主上皮细胞中侵袭,生存和繁殖,但尚未鉴定出金黄色葡萄球菌HPT系统中涉及的遗传元件。在这项研究中,我们鉴定并鉴定了金黄色葡萄球菌中的HPT系统,该系统包括hptRS(新颖的两组分调节系统),hptA(假定的磷酸盐传感器)和uhpT(磷酸己糖转运蛋白)基因。使用改良的pMAD-CM-GFPuv载体系统,通过等位基因置换方法生成了hptA,hptRS和uhpT无标记缺失突变体。我们证明了hptA和hptRS都需要积极调节uhpT的转录,以响应细胞外磷酸盐,例如3-磷酸甘油(G3P),6-磷酸葡萄糖(G6P)和磷霉素。突变研究表明,当可利用的碳源仅限于G6P时,对hptA,hptRS或uhpT基因的破坏会损害细菌的生长,会损害各种宿主细胞内的存活/繁殖,并增加对磷霉素的抗性。这项研究的结果表明,HPT系统在适应 S“中起着重要作用。金黄色葡萄球菌在宿主细胞中可能是开发新型抗葡萄球菌疗法的重要靶标。

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