利用结核分枝杆菌 H37Ra 感染的免疫功能健全小鼠作为顽固病菌的体内模型

IF 2.8 3区 医学 Q3 IMMUNOLOGY Tuberculosis Pub Date : 2024-01-18 DOI:10.1016/j.tube.2024.102479
Neetu Kumari , Romil Sharma , Juned Ali , Gyan Chandra , Sarika Singh , Manju Y. Krishnan
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引用次数: 0

摘要

结核分枝杆菌(Mtb)的持续存在是成功治疗结核病(TB)的挑战之一。非复制 Mtb 的体外模型被用来测试新分子对 Mtb 持久体的疗效。H37Ra 菌株在巨噬细胞和小鼠体内的生长能力减弱。我们验证了 H37Ra 感染免疫功能健全的小鼠,用于测试抗结核分子对慢速/非复制 Mtb 的体内疗效。瑞士小鼠经静脉感染 H37Ra,并在 12 周内监测其 CFU 负担和组织病理学。细菌以缓慢的速度繁殖,根据感染剂量的不同,在 8-12 周内达到最大负荷量 106 ∼106,同时肺部组织病理学变化与时间和剂量有关。令人惊讶的是,使用异烟肼-利福平-乙胺丁醇-吡嗪酰胺复方制剂治疗 4 周后,肺部和脾脏中的 CFU 只分别减少了 0.4 log10 和 1 log10。结果表明,经过 4 周的抗结核治疗后,肺部有 40% 的 H37Ra 杆菌是宿主。异烟肼/利福平单一疗法也显示出类似的结果。贝达喹啉和异烟肼联合使用可将CFU数量减少到200(检测限),而单用异烟肼则可减少到5000 CFU。该研究展示了一种用于使用 BSL-2 菌株测试新线索的 Mtb 持久病菌体内模型。
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The use of Mycobacterium tuberculosis H37Ra-infected immunocompetent mice as an in vivo model of persisters

Persistence of Mycobacterium tuberculosis (Mtb) is one of the challenges to successful treatment of tuberculosis (TB). In vitro models of non-replicating Mtb are used to test the efficacy of new molecules against Mtb persisters. The H37Ra strain is attenuated for growth in macrophages and mice. We validated H37Ra-infected immunocompetent mice for testing anti-TB molecules against slow/non-replicating Mtb in vivo. Swiss mice were infected intravenously with H37Ra and monitored for CFU burden and histopathology for a period of 12 weeks. The bacteria multiplied at a slow pace reaching a maximum load of ∼106 in 8–12 weeks depending on the infection dose, accompanied by time and dose-dependent histopathological changes in the lungs. Surprisingly, four-weeks of treatment with isoniazid-rifampicin-ethambutol-pyrazinamide combination caused only 0.4 log10 and 1 log10 reduction in CFUs in lungs and spleen respectively. The results show that ∼40 % of the H37Ra bacilli in lungs are persisters after 4 weeks of anti-TB therapy. Isoniazid/rifampicin monotherapy also showed similar results. A combination of bedaquiline and isoniazid reduced the CFU counts to <200 (limit of detection), compared to ∼5000 CFUs by isoniazid alone. The study demonstrates an in vivo model of Mtb persisters for testing new leads using a BSL-2 strain.

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来源期刊
Tuberculosis
Tuberculosis 医学-呼吸系统
CiteScore
4.60
自引率
3.10%
发文量
87
审稿时长
49 days
期刊介绍: Tuberculosis is a speciality journal focusing on basic experimental research on tuberculosis, notably on bacteriological, immunological and pathogenesis aspects of the disease. The journal publishes original research and reviews on the host response and immunology of tuberculosis and the molecular biology, genetics and physiology of the organism, however discourages submissions with a meta-analytical focus (for example, articles based on searches of published articles in public electronic databases, especially where there is lack of evidence of the personal involvement of authors in the generation of such material). We do not publish Clinical Case-Studies. Areas on which submissions are welcomed include: -Clinical TrialsDiagnostics- Antimicrobial resistance- Immunology- Leprosy- Microbiology, including microbial physiology- Molecular epidemiology- Non-tuberculous Mycobacteria- Pathogenesis- Pathology- Vaccine development. This Journal does not accept case-reports. The resurgence of interest in tuberculosis has accelerated the pace of relevant research and Tuberculosis has grown with it, as the only journal dedicated to experimental biomedical research in tuberculosis.
期刊最新文献
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