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沙眼衣原体慢性生殖道感染在γ干扰素基因敲除小鼠中的传播

Dissemination of Chlamydia trachomatis chronic genital tract infection in gamma interferon gene knockout mice.

作者信息

Cotter T W, Ramsey K H, Miranpuri G S, Poulsen C E, Byrne G I

机构信息

Department of Medical Microbiology and Immunology, University of Wisconsin School of Medicine, Madison 53706, USA.

出版信息

Infect Immun. 1997 Jun;65(6):2145-52. doi: 10.1128/iai.65.6.2145-2152.1997.

Abstract

Mice (C57BL/6), treated with progesterone and infected intravaginally with the mouse pneumonitis strain of Chlamydia trachomatis (MoPn), acquired genital tract disease that ascended from the endocervix to the uterine horns, oviducts, and ovaries in a temporal fashion before the occurrence of spontaneous microbiological resolution by about 28 days after infection. Surprisingly, dissemination of MoPn in small numbers to draining lymph nodes, the peritoneal cavity, spleen, liver, kidneys, and lungs occurred in normal mice during the early stages of disease (7 to 14 days) in a portion of infected animals but resolved from these tissues, by microbiological criteria, prior to resolution of genital tract involvement. In contrast, gamma interferon knockout (IFN-gamma KO) mice exhibited dissemination of infection to a greater extent and for longer periods in a variety of tissues, and a portion of infected IFN-gamma KO mice failed to microbiologically resolve their genital tract disease. By comparison, C57BL/6 SCID mice uniformly failed to resolve their genital tract disease and exhibited high levels of dissemination to all tissues tested for extended (50-day) periods of times. Interestingly, although IFN-gamma KO mice failed to completely clear organisms from their genital tracts, they exhibited an attenuated infection indistinguishable from that of heterozygous littermates when challenged 112 days after primary infection. These data support a role for IFN-gamma in containing dissemination of MoPn from the genital tract to extragenital sites and in the microbiological resolution of infection. Data also indicate that IFN-gamma is not required for modulating reinfections, which normally follow a shorter and less dramatic course.

摘要

用孕酮处理的C57BL/6小鼠经阴道感染沙眼衣原体小鼠肺炎株(MoPn)后,在感染后约28天自然微生物清除发生之前,以时间顺序从子宫颈上升至子宫角、输卵管和卵巢,获得了生殖道疾病。令人惊讶的是,在疾病早期(7至14天),一小部分感染动物的正常小鼠中,少量的MoPn会扩散到引流淋巴结、腹腔、脾脏、肝脏、肾脏和肺部,但在生殖道受累症状消除之前,根据微生物学标准,这些组织中的感染就已消除。相比之下,γ干扰素基因敲除(IFN-γ KO)小鼠在多种组织中表现出更大程度和更长时间的感染扩散,并且一部分感染的IFN-γ KO小鼠未能通过微生物学方法消除其生殖道疾病。相比之下,C57BL/6 SCID小鼠始终未能消除其生殖道疾病,并且在长达50天的时间内,在所有测试组织中均表现出高水平的扩散。有趣的是,尽管IFN-γ KO小鼠未能从其生殖道中完全清除病原体,但在初次感染112天后受到攻击时,它们表现出与杂合子同窝小鼠难以区分的减弱感染。这些数据支持IFN-γ在控制MoPn从生殖道扩散到生殖道外部位以及在感染的微生物学清除中发挥作用。数据还表明,调节再次感染不需要IFN-γ,再次感染通常病程较短且不那么严重。

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