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食蟹猴感染结核分枝杆菌的早期事件。

Early events in Mycobacterium tuberculosis infection in cynomolgus macaques.

作者信息

Lin Philana Ling, Pawar Santosh, Myers Amy, Pegu Amarenda, Fuhrman Carl, Reinhart Todd A, Capuano Saverio V, Klein Edwin, Flynn Joanne L

机构信息

Department of Molecular Genetics and Biochemistry, University of Pittsburgh School of Medicine, W1157 Biomedical Science Tower, 200 Lothrop Street, Pittsburgh, PA 15261, USA.

出版信息

Infect Immun. 2006 Jul;74(7):3790-803. doi: 10.1128/IAI.00064-06.

Abstract

Little is known regarding the early events of infection of humans with Mycobacterium tuberculosis. The cynomolgus macaque is a useful model of tuberculosis, with strong similarities to human tuberculosis. In this study, eight cynomolgus macaques were infected bronchoscopically with low-dose M. tuberculosis; clinical, immunologic, microbiologic, and pathologic events were assessed 3 to 6 weeks postinfection. Gross pathological abnormalities were observed as early as 3 weeks, including Ghon complex formation by 5 weeks postinfection. Caseous granulomas were observed in the lung as early as 4 weeks postinfection. Only caseous granulomas were observed in the lungs at these early time points, reflecting a rigorous initial response. T-cell activation (CD29 and CD69) and chemokine receptor (CXCR3 and CCR5) expression appeared localized to different anatomic sites. Activation markers were increased on cells from airways and only at modest levels on cells in peripheral blood. The priming of mycobacterium-specific T cells, characterized by the production of gamma interferon occurred slowly, with responses seen only after 4 weeks of infection. These responses were observed from T lymphocytes in blood, airways, and hilar lymph node, with responses predominantly localized to the site of infection. From these studies, we conclude that immune responses to M. tuberculosis are relatively slow in the local and peripheral compartments and that necrosis occurs surprisingly quickly during granuloma formation.

摘要

关于人类感染结核分枝杆菌的早期事件,目前所知甚少。食蟹猕猴是一种有用的结核病模型,与人类结核病有很强的相似性。在本研究中,八只食蟹猕猴通过支气管镜感染低剂量结核分枝杆菌;在感染后3至6周评估临床、免疫、微生物和病理事件。早在3周时就观察到大体病理异常,包括感染后5周出现原发综合征。早在感染后4周就在肺部观察到干酪样肉芽肿。在这些早期时间点,肺部仅观察到干酪样肉芽肿,这反映了一种严格的初始反应。T细胞活化(CD29和CD69)和趋化因子受体(CXCR3和CCR5)表达似乎定位于不同的解剖部位。活化标志物在气道细胞上增加,而在外周血细胞上仅适度增加。以γ干扰素产生为特征的分枝杆菌特异性T细胞的启动过程缓慢,仅在感染4周后才出现反应。在血液、气道和肺门淋巴结中的T淋巴细胞中观察到这些反应,且反应主要定位于感染部位。从这些研究中,我们得出结论,在局部和外周区域,对结核分枝杆菌的免疫反应相对较慢,并且在肉芽肿形成过程中坏死发生得惊人地快。

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