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Effect of Metabolic Imbalance on Expression of Type III Secretion Genes in Pseudomonas aeruginosa

机译:代谢失衡对铜绿假单胞菌Ⅲ型分泌基因表达的影响

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The type III secretion system is a dedicated machinery used by many pathogens to deliver toxins directly into the cytoplasm of a target cell. Expression and secretion of the type III effectors are triggered by cell contact. In Pseudomonas aeruginosa and Yersinia spp., expression can be triggered in vitro by removing calcium from the medium. The mechanism underlying either mode of regulation is unclear. Here we characterize a transposon insertion mutant of P. aeruginosa PAO1 that displays a marked defect in cytotoxicity. The insertion is located upstream of several genes involved in histidine utilization and impedes the ability of PAO1 to intoxicate eukaryotic cells effectively in a type III-dependent fashion. This inhibition depends on the presence of histidine in the medium and appears to depend on the excessive uptake and catabolism of histidine. The defect in cytotoxicity is mirrored by a decrease in exoS expression. Other parameters such as growth or piliation are unaffected. The cytotoxicity defect is partially complemented by an insertion mutation in cbrA that also causes overexpression of cbrB. The cbrAB two-component system has been implicated in sensing and responding to a carbon-nitrogen imbalance. Taken together, these results suggest that the metabolic state of the cell influences expression of the type III regulon.
机译:III型分泌系统是许多病原体用来将毒素直接传递到靶细胞的细胞质中的专用设备。细胞接触触发III型效应子的表达和分泌。在铜绿假单胞菌耶尔森氏菌 spp。中,可以通过从培养基中去除钙来触发表达。两种调节方式的机制尚不清楚。在这里,我们表征了 P的转座子插入突变体。铜绿假单胞菌PAO1具有明显的细胞毒性缺陷。该插入位于与组氨酸利用有关的几个基因的上游,并阻碍了PAO1以III型依赖的方式有效地使真核细胞中毒的能力。这种抑制作用取决于培养基中组氨酸的存在,并且似乎取决于组氨酸的过度摄取和分解代谢。细胞毒性的缺陷反映在 exoS 表达的减少上。其他参数,例如生长或毛羽不受影响。细胞毒性缺陷部分由 cbrA 中的插入突变所弥补,这也会导致 cbrB 的过表达。 cbrAB 两组分系统与感测和响应碳氮不平衡有关。综上所述,这些结果表明细胞的代谢状态影响III型调节子的表达。

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