Robert Koch-Institut, Research Group P26, Nosocomial Infections of the Elderly, Nordufer 20, 13353 Berlin, Germany.
Int J Med Microbiol. 2010 Jun;300(5):313-23. doi: 10.1016/j.ijmm.2010.01.002. Epub 2010 Feb 12.
We previously identified Legionella pneumophila PlaB as the major cell-associated phospholipase A/lysophospholipase A with contact-dependent hemolytic activity. In this study, we further characterized this protein and found it to be involved in the virulence of L. pneumophila. PlaB was mainly expressed and active during exponential growth. Active PlaB was outer membrane-associated and at least in parts surface-exposed. Transport to the outer membrane was not dependent on the type I (T1SS), II (T2SS), IVB (T4BSS) or Tat secretion pathways. Furthermore, PlaB activity was not dependent on the presence of the macrophage infectivity potentiator (Mip) or the major secreted zinc metalloproteinase A (MspA). Despite the fact that PlaB is not essential for replication in protozoa or macrophage cell lines, we found that plaB mutants were impaired for replication in the lungs and dissemination to the spleen in the guinea pig infection model. Histological sections monitored less inflammation and destruction of the lung tissue after infection with the plaB mutants compared to L. pneumophila wild type. Taken together, PlaB is the first phospholipase A/lysophospholipase A with a confirmed role in the establishment of Legionnaires' disease.
我们之前鉴定出嗜肺军团菌 PlaB 是主要的细胞相关磷脂酶 A/溶血磷脂酶 A,具有接触依赖性溶血活性。在这项研究中,我们进一步对该蛋白进行了表征,发现它与嗜肺军团菌的毒力有关。PlaB 在指数生长期主要表达和活跃。活性 PlaB 与外膜相关,至少部分表面暴露。向外膜的转运不依赖于 I 型(T1SS)、II 型(T2SS)、IVB(T4BSS)或 Tat 分泌途径。此外,PlaB 活性不依赖于巨噬细胞感染增强因子(Mip)或主要分泌的锌金属蛋白酶 A(MspA)的存在。尽管 PlaB 对于原生动物或巨噬细胞系中的复制不是必需的,但我们发现 PlaB 突变体在豚鼠感染模型中的肺部复制和向脾脏的传播受损。与野生型嗜肺军团菌相比,感染 PlaB 突变体后,组织学切片显示肺部炎症和组织破坏较少。总之,PlaB 是第一个被证实与军团病的建立有关的磷脂酶 A/溶血磷脂酶 A。
