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Yersinia pestis Endowed with Increased Cytotoxicity Is Avirulent in a Bubonic Plague Model and Induces Rapid Protection against Pneumonic Plague

机译:鼠疫耶尔森氏菌具有更高的细胞毒性,在鼠疫鼠疫模型中是无毒的,可诱导针对肺炎鼠疫的快速保护。

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摘要

An important virulence strategy evolved by bacterial pathogens to overcome host defenses is the modulation of host cell death. Previous observations have indicated that Yersinia pestis, the causative agent of plague disease, exhibits restricted capacity to induce cell death in macrophages due to ineffective translocation of the type III secretion effector YopJ, as opposed to the readily translocated YopP, the YopJ homologue of the enteropathogen Yersinia enterocolitica O∶8. This led us to suggest that reduced cytotoxic potency may allow pathogen propagation within a shielded niche, leading to increased virulence. To test the relationship between cytotoxic potential and virulence, we replaced Y. pestis YopJ with YopP. The YopP-expressing Y. pestis strain exhibited high cytotoxic activity against macrophages in vitro. Following subcutaneous infection, this strain had reduced ability to colonize internal organs, was unable to induce septicemia and exhibited at least a 107-fold reduction in virulence. Yet, upon intravenous or intranasal infection, it was still as virulent as the wild-type strain. The subcutaneous administration of the cytotoxic Y. pestis strain appears to activate a rapid and potent systemic, CTL-independent, immunoprotective response, allowing the organism to overcome simultaneous coinfection with 10,000 LD50 of virulent Y. pestis. Moreover, three days after subcutaneous administration of this strain, animals were also protected against septicemic or primary pneumonic plague. Our findings indicate that an inverse relationship exists between the cytotoxic potential of Y. pestis and its virulence following subcutaneous infection. This appears to be associated with the ability of the engineered cytotoxic Y. pestis strain to induce very rapid, effective and long-lasting protection against bubonic and pneumonic plague. These observations have novel implications for the development of vaccines/therapies against Y. pestis and shed new light on the virulence strategies of Y. pestis in nature.
机译:由细菌病原体进化以克服宿主防御的重要毒力策略是宿主细胞死亡的调节。先前的观察结果表明,鼠疫耶尔森氏菌是鼠疫疾病的病原体,由于III型分泌效应因子YopJ易位,与巨噬细胞的易位YopP(肠道病原体的YopJ同源物)相比,其诱导巨噬细胞死亡的能力有限。小肠结肠炎耶尔森菌O∶8。这导致我们提出降低细胞毒性的潜能可能会导致病原体在受保护的生态位内繁殖,从而增加毒力。为了测试细胞毒性潜力和毒力之间的关系,我们用YopP替代了鼠疫耶尔森氏菌YopJ。表达YopP的鼠疫耶尔森氏菌菌株在体外对巨噬细胞表现出高的细胞毒性活性。皮下感染后,该菌株的内脏定植能力降低,无法诱导败血病,毒力降低至少107倍。然而,在静脉或鼻内感染后,它仍具有与野生型毒株一样的毒性。皮下施用细胞毒性鼠疫耶尔森氏菌菌株似乎可以激活快速有效的全身性,不依赖CTL的免疫保护反应,从而使该生物体能够同时克服10,000 LD50毒性鼠疫耶尔森氏菌的同时感染。而且,在该菌株的皮下给药三天后,还保护了动物免于败血病或原发性肺炎鼠疫。我们的发现表明,在皮下感染后,鼠疫耶尔森氏菌的细胞毒性潜力与其毒力之间存在反比关系。这似乎与工程改造的细胞毒性鼠疫耶尔森氏菌菌株诱导针对豚鼠和肺炎鼠疫的非常快速,有效和持久的保护能力有关。这些发现对抵抗鼠疫耶尔森氏菌的疫苗/疗法的发展具有新的意义,并为自然界中的鼠疫耶尔森氏菌的毒力策略提供了新的思路。

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