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土拉热弗朗西斯菌活疫苗株感染的免疫后果:天然免疫反应在感染和免疫中的作用

Immunologic consequences of Francisella tularensis live vaccine strain infection: role of the innate immune response in infection and immunity.

作者信息

Cole Leah E, Elkins Karen L, Michalek Suzanne M, Qureshi Nilofer, Eaton Linda J, Rallabhandi Prasad, Cuesta Natalia, Vogel Stefanie N

机构信息

Department of Microbiology and Immunology, University of Maryland, Baltimore, School of Medicine, Baltimore, MD 21201, USA.

出版信息

J Immunol. 2006 Jun 1;176(11):6888-99. doi: 10.4049/jimmunol.176.11.6888.

Abstract

Francisella tularensis (Ft), a Gram-negative intracellular bacterium, is the etiologic agent of tularemia. Although attenuated for humans, i.p. infection of mice with <10 Ft live vaccine strain (LVS) organisms causes lethal infection that resembles human tularemia, whereas the LD50 for an intradermal infection is >10(6) organisms. To examine the immunological consequences of Ft LVS infection on the innate immune response, the inflammatory responses of mice infected i.p. or intradermally were compared. Mice infected i.p. displayed greater bacterial burden and increased expression of proinflammatory genes, particularly in the liver. In contrast to most LPS, highly purified Ft LVS LPS (10 microg/ml) was found to be only minimally stimulatory in primary murine macrophages and in HEK293T cells transiently transfected with TLR4/MD-2/CD14, whereas live Ft LVS bacteria were highly stimulatory for macrophages and TLR2-expressing HEK293T cells. Despite the poor stimulatory activity of Ft LVS LPS in vitro, administration of 100 ng of Ft LVS LPS 2 days before Ft LVS challenge severely limited both bacterial burden and cytokine mRNA and protein expression in the absence of detectable Ab at the time of bacterial challenge, yet these mice developed a robust IgM Ab response within 2 days of infection and survived. These data suggest that prior administration of Ft LVS LPS protects the host by diminishing bacterial burden and blunting an otherwise overwhelming inflammatory response, while priming the adaptive immune response for development of a strong Ab response.

摘要

土拉弗朗西斯菌(Ft)是一种革兰氏阴性胞内细菌,是兔热病的病原体。尽管对人类毒性减弱,但用少于10个Ft活疫苗株(LVS)感染小鼠腹腔会导致致命感染,类似于人类兔热病,而皮内感染的半数致死量大于10⁶个细菌。为了研究Ft LVS感染对先天免疫反应的免疫后果,比较了腹腔感染或皮内感染小鼠的炎症反应。腹腔感染的小鼠表现出更高的细菌载量和促炎基因表达增加,特别是在肝脏中。与大多数脂多糖不同,高度纯化的Ft LVS脂多糖(10微克/毫升)在原代小鼠巨噬细胞和瞬时转染TLR4/MD-2/CD14的HEK293T细胞中仅具有最小的刺激作用,而活的Ft LVS细菌对巨噬细胞和表达TLR2的HEK293T细胞具有高度刺激作用。尽管Ft LVS脂多糖在体外刺激活性较差,但在Ft LVS攻击前2天给予100纳克Ft LVS脂多糖,在细菌攻击时没有可检测到的抗体的情况下,严重限制了细菌载量以及细胞因子mRNA和蛋白质表达,但这些小鼠在感染后2天内产生了强烈的IgM抗体反应并存活下来。这些数据表明,预先给予Ft LVS脂多糖可通过减少细菌载量和减弱原本压倒性的炎症反应来保护宿主,同时启动适应性免疫反应以产生强烈的抗体反应。

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