小肠结肠炎耶尔森菌O:8主要分泌性耶尔森菌外膜蛋白(Yops)对小鼠感染模型致病性的贡献
Contribution of the major secreted yops of Yersinia enterocolitica O:8 to pathogenicity in the mouse infection model.
作者信息
Trülzsch Konrad, Sporleder Thorsten, Igwe Emeka I, Rüssmann Holger, Heesemann Jürgen
机构信息
Max von Pettenkofer Institute for Hygiene and Medical Microbiology, Ludwig Maximilians University, Munich, Germany.
出版信息
Infect Immun. 2004 Sep;72(9):5227-34. doi: 10.1128/IAI.72.9.5227-5234.2004.
Pathogenic yersiniae (Yersinia pestis, Y. pseudotuberculosis, and Y. enterocolitica) harbor a 70-kb virulence plasmid (pYV) that encodes a type III secretion system and a set of at least six effector proteins (YopH, YopO, YopP, YopE, YopM, and YopT) that are injected into the host cell cytoplasm. Yops (Yersinia outer proteins) disturb the dynamics of the cytoskeleton, inhibit phagocytosis by macrophages, and downregulate the production of proinflammatory cytokines, which makes it possible for yersiniae to multiply extracellularly in lymphoid tissue. Y. enterocolitica serotype O:8 belongs to the highly mouse-pathogenic group of yersiniae in contrast to Y. enterocolitica serotype O:9. However, there has been no systematic study of the contribution of Yops to the pathogenicity of Y. enterocolitica O:8 in mice. We generated a set of yop gene deletion mutants of Y. enterocolitica O:8 by using the novel Red cloning procedure. We subsequently analyzed the contribution of yopH, -O, -P, -E, -M, -T, and -Q deletions to pathogenicity after oral and intravenous infection of mice. Here we showed for the first time that a DeltayopT deletion mutant colonizes mouse tissues to a greater extent than the parental strain. The DeltayopO, DeltayopP, and DeltayopE mutants were only slightly attenuated after oral infection since they were still able to colonize the spleen and liver and cause systemic infection. The DeltayopO mutant was lethal for mice, whereas DeltayopP and DeltayopE mutants were successfully eliminated from the spleen and liver 2 weeks after infection. In contrast the DeltayopH, DeltayopM, and DeltayopQ mutants were highly attenuated and not able to colonize the spleen and liver on any of the days tested. The DeltayopH, DeltayopO, DeltayopP, DeltayopE, DeltayopM, and DeltayopQ mutants had only modest defects in the colonization of the small intestine and Peyer's patches. The DeltayopE mutant was eliminated from the small intestine 3 weeks after infection, whereas the DeltayopH, DeltayopP, DeltayopM, and DeltayopQ mutants continued to colonize the small intestine at this time.
致病性耶尔森菌(鼠疫耶尔森菌、假结核耶尔森菌和小肠结肠炎耶尔森菌)携带一个70kb的毒力质粒(pYV),该质粒编码一个III型分泌系统和一组至少六种效应蛋白(YopH、YopO、YopP、YopE、YopM和YopT),这些蛋白被注入宿主细胞质中。Yops(耶尔森菌外膜蛋白)扰乱细胞骨架动力学,抑制巨噬细胞的吞噬作用,并下调促炎细胞因子的产生,这使得耶尔森菌能够在淋巴组织中进行胞外增殖。与小肠结肠炎耶尔森菌O:9血清型相比,小肠结肠炎耶尔森菌O:8血清型属于对小鼠致病性很强的耶尔森菌群。然而,尚未有关于Yops对小肠结肠炎耶尔森菌O:8在小鼠中致病性贡献的系统性研究。我们利用新型Red克隆程序构建了一组小肠结肠炎耶尔森菌O:8的yop基因缺失突变体。随后,我们分析了yopH、-O、-P、-E、-M、-T和-Q缺失对小鼠经口和静脉感染后致病性的影响。在此,我们首次表明,ΔyopT缺失突变体在小鼠组织中的定殖程度高于亲本菌株。ΔyopO、ΔyopP和ΔyopE突变体经口感染后仅略有减毒,因为它们仍能定殖于脾脏和肝脏并引起全身感染。ΔyopO突变体对小鼠具有致死性,而ΔyopP和ΔyopE突变体在感染后2周从脾脏和肝脏中被成功清除。相比之下,ΔyopH、ΔyopM和ΔyopQ突变体高度减毒,在任何测试日都无法定殖于脾脏和肝脏。ΔyopH、ΔyopO、ΔyopP、ΔyopE、ΔyopM和ΔyopQ突变体在小肠和派尔集合淋巴结定殖方面仅有适度缺陷。ΔyopE突变体在感染后3周从小肠中被清除,而此时ΔyopH、ΔyopP、ΔyopM和ΔyopQ突变体仍继续定殖于小肠。
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