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HrcU and HrpP are pathogenicity factors in the fire blight pathogen Erwinia amylovora required for the type III secretion of DspA/E

机译:HrcU和HrpP是DspA / E的III型分泌所必需的火疫病病原体小球藻欧文氏菌的致病因素

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Background Many Gram-negative bacterial pathogens mediate host-microbe interactions via utilization of the type III secretion (T3S) system. The T3S system is a complex molecular machine consisting of more than 20 proteins. Collectively, these proteins translocate effectors across extracellular space and into the host cytoplasm. Successful translocation requires timely synthesis and allocation of both structural and secreted T3S proteins. Based on amino acid conservation in animal pathogenic bacteria, HrcU and HrpP were examined for their roles in regulation of T3S hierarchy. Results Both HrcU and HrpP were shown to be required for disease development in an immature pear infection model and respective mutants were unable to induce a hypersensitive response in tobacco. Using in vitro western blot analyses, both proteins were also shown to be required for the secretion of DspA/E, a type 3 effector and an important pathogenicity factor. Via yeast-two hybridization (Y2H), HrpP and HrcU were revealed to exhibit protein-protein binding. Finally, all HrcU and HrpP phenotypes identified were shown to be dependent on a conserved amino acid motif in the cytoplasmic tail of HrcU. Conclusions Collectively, these data demonstrate roles for HrcU and HrpP in regulating T3S and represent the first attempt in understanding T3S heirarchy in E. amylovora .
机译:背景技术许多革兰氏阴性细菌病原体通过利用III型分泌(T3S)系统来介导宿主-微生物相互作用。 T3S系统是由20多种蛋白质组成的复杂分子机器。这些蛋白质共同地将效应子跨细胞外空间转运并进入宿主细胞质。成功的易位需要结构和分泌的T3S蛋白的及时合成和分配。基于动物病原细菌中的氨基酸保守性,检查了HrcU和HrpP在调节T3S层次中的作用。结果显示,在不成熟的梨感染模型中,HrcU和HrpP都是疾病发展所必需的,并且各自的突变体均不能在烟草中诱导超敏反应。使用体外蛋白质印迹分析,这两种蛋白质也被证明是DspA / E,3型效应子和重要的致病因子的分泌所必需的。通过酵母两次杂交(Y2H),HrpP和HrcU被发现表现出蛋白质-蛋白质结合。最后,所有鉴定出的HrcU和HrpP表型均显示为依赖于HrcU胞质尾中的保守氨基酸基序。结论总体而言,这些数据证明了HrcU和HrpP在调节T3S中的作用,并代表了首次了解淀粉状支原体中T3S层次结构的尝试。

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