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普氏立克次体感染的小鼠模型:对流行性斑疹伤寒发病机制的启示

A murine model of infection with Rickettsia prowazekii: implications for pathogenesis of epidemic typhus.

作者信息

Bechah Yassina, Capo Christian, Grau Georges E, Raoult Didier, Mege Jean-Louis

机构信息

Unité des Rickettsies, CNRS UMR 6020, Université de la Méditerranée, Faculté de Médecine, 27 Bld. J. Moulin, 13385 Marseille Cedex 05, France.

出版信息

Microbes Infect. 2007 Jun;9(7):898-906. doi: 10.1016/j.micinf.2007.03.008. Epub 2007 Mar 21.

DOI:10.1016/j.micinf.2007.03.008
PMID:17537665
Abstract

Epidemic typhus remains a major disease threat, furthermore, its etiologic agent, Rickettsia prowazekii, is classified as a bioterrorism agent. We describe here a murine model of epidemic typhus that reproduced some features of the human disease. When BALB/c mice were inoculated intravenously with R. prowazekii (Breinl strain), they survived but did not clear R. prowazekii infection. Immunohistological analysis of tissues and quantitative PCR showed that R. prowazekii was present in blood, liver, lungs and brain 1 day after infection and persisted for at least 9 days. Importantly, infected mice developed interstitial pneumonia, with consolidation of the alveoli, hemorrhages in lungs, multifocal granulomas in liver, and hemorrhages in brain, as seen in humans. Circulating antibodies directed against R. prowazekii were detected at day 4 post-infection and steadily increased for up to 21 days, demonstrating that R. prowazekii lesions were independent of humoral immune response. R. prowazekii-induced lesions were associated with inflammatory response, as demonstrated by elevated levels of inflammatory cytokines including interferon-gamma, tumor necrosis factor and the CC chemokine RANTES in the lesions. We concluded that the BALB/c mouse strain provides a useful model for studying the pathogenic mechanisms of epidemic typhus and its control by the immune system.

摘要

流行性斑疹伤寒仍然是一种主要的疾病威胁,此外,其病原体普氏立克次体被列为生物恐怖主义制剂。我们在此描述一种流行性斑疹伤寒的小鼠模型,该模型再现了人类疾病的一些特征。当用普氏立克次体(布雷因尔菌株)静脉接种BALB/c小鼠时,它们存活下来但未清除普氏立克次体感染。组织的免疫组织学分析和定量PCR显示,感染后1天普氏立克次体存在于血液、肝脏、肺和脑中,并持续至少9天。重要的是,感染的小鼠出现间质性肺炎,伴有肺泡实变、肺部出血、肝脏多灶性肉芽肿和脑部出血,这与人类所见相同。感染后第4天检测到针对普氏立克次体的循环抗体,并持续稳定增加长达21天,表明普氏立克次体病变独立于体液免疫反应。普氏立克次体诱导的病变与炎症反应相关,病变中包括干扰素-γ、肿瘤坏死因子和CC趋化因子RANTES在内的炎症细胞因子水平升高证明了这一点。我们得出结论,BALB/c小鼠品系为研究流行性斑疹伤寒的致病机制及其由免疫系统控制提供了一个有用的模型。

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