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Mycobacteria infect different cell types in the human lung and cause species dependent cellular changes in infected cells

机译:分枝杆菌感染人肺中的不同细胞类型,并导致受感染细胞的物种依赖性细胞变化

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Mycobacterial infections remain a significant cause of morbidity and mortality worldwide. Due to limitations of the currently available model systems, there are still comparably large gaps in the knowledge about the pathogenesis of these chronic inflammatory diseases in particular with regard to the human host. Therefore, we aimed to characterize the initial phase of mycobacterial infections utilizing a human ex vivo lung tissue culture model designated STST (Short-Term Stimulation of Tissues). Human lung tissues from 65 donors with a size of 0.5–1?cm3 were infected each with two strains of three different mycobacterial species (M. tuberculosis, M. avium, and M. abscessus), respectively. In order to preserve both morphology and nucleic acids, the HOPE? fixation technique was used. The infected tissues were analyzed using histo- and molecular-pathological methods. Immunohistochemistry was applied to identify the infected cell types. Morphologic comparisons between ex vivo incubated and non-incubated lung specimens revealed no noticeable differences. Viability of ex vivo stimulated tissues demonstrated by TUNEL-assay was acceptable. Serial sections verified sufficient diffusion of the infectious agents deep into the tissues. Infection was confirmed by Ziel Neelsen-staining and PCR to detect mycobacterial DNA. We observed the infection of different cell types, including macrophages, neutrophils, monocytes, and pneumocytes-II, which were critically dependent on the mycobacterial species used. Furthermore, different forms of nuclear alterations (karyopyknosis, karyorrhexis, karyolysis) resulting in cell death were detected in the infected cells, again with characteristic species-dependent differences. We show the application of a human ex vivo tissue culture model for mycobacterial infections. The immediate primary infection of a set of different cell types and the characteristic morphologic changes observed in these infected human tissues significantly adds to the current understanding of the initial phase of human pulmonary tuberculosis. Further studies are ongoing to elucidate the molecular mechanisms involved in the early onset of mycobacterial infections in the human lung.
机译:分枝杆菌感染仍然是全世界发病率和死亡率的重要原因。由于当前可用的模型系统的局限性,关于这些慢性炎性疾病的发病机理的知识,尤其是关于人类宿主的知识,仍然存在相当大的空白。因此,我们旨在利用人类离体肺组织培养模型STST(组织的短期刺激)来表征分枝杆菌感染的初始阶段。来自65个供体的人肺组织的大小为0.5-1?cm3,分别用两种菌株感染了三种不同的分枝杆菌种(结核分枝杆菌,鸟分枝杆菌和脓肿分枝杆菌)。为了保留形态和核酸,希望?使用固定技术。使用组织和分子病理学方法分析感染的组织。应用免疫组织化学鉴定感染的细胞类型。离体培养的肺和未培养的肺标本之间的形态学比较显示没有明显的差异。通过TUNEL测定证实的离体刺激组织的活力是可以接受的。系列切片证实了传染原充分扩散到组织深处。通过Ziel Neelsen染色和PCR检测分枝杆菌DNA证实感染。我们观察到了不同细胞类型的感染,包括巨噬细胞,嗜中性粒细胞,单核细胞和肺细胞-II,它们严重依赖于所使用的分枝杆菌菌种。此外,在受感染的细胞中检测到导致细胞死亡的不同形式的核改变(核融合,核转移,核溶解),再次具有特征性的物种依赖性。我们展示了人类离体组织培养模型用于分枝杆菌感染的应用。立即感染一系列不同细胞类型的原发性感染以及在这些被感染的人类组织中观察到的特征性形态变化,大大增加了对人类肺结核初始阶段的当前了解。正在进行进一步的研究以阐明与人肺中分支杆菌感染的早期发作有关的分子机制。

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