Guangdong Provincial Key Laboratory of Regional Immunity and Diseases, Department of Pathogen Biology, School of Medicine, Shenzhen Universitygrid.263488.3, Shenzhen, China.
Department of Respiratory Medicine, Children's Hospital of Chongqing Medical University, Chongqing Key Laboratory of Pediatrics, Chongqing, China.
mBio. 2022 Oct 26;13(5):e0200422. doi: 10.1128/mbio.02004-22. Epub 2022 Aug 24.
Tuberculosis (TB), which is caused by the single pathogenic bacterium, Mycobacterium tuberculosis, is among the top 10 lethal diseases worldwide. This situation has been exacerbated by the increasing number of cases of multidrug-resistant TB (MDR-TB) and extensively drug-resistant TB (XDR-TB). Histamine is an organic nitrogenous compound that mediates a plethora of cell processes via different receptors. The expression of histamine receptor H1 (HRH1), one of the four histamine receptors identified to date was previously reported to be augmented by M. tuberculosis infection, although the underlying mechanism is unclear. In the present study, we applied confocal microscopy, flow cytometry, and Western blotting to show that HRH1 expression was enhanced in macrophages following mycobacterial infection. Furthermore, by combining techniques of gene knockdown, immunoprecipitation, intracellular bacterial burden analysis, fluorescence labeling, and imaging, we found that M. tuberculosis targeted the host HRH1 to suppress NOX2-mediated cROS production and inhibit phagosome maturation and acidification via the GRK2-p38MAPK signaling pathway. Our findings clarified the underlying mechanism of the M. tuberculosis and host HRH1 interaction and may provide useful information for the development of novel antituberculosis treatments. Once engulfed in macrophage phagosomes, M. tuberculosis adopts various strategies to take advantage of the host environment for its intracellular survival. Histamine is an organic nitrogen-containing compound that mediates a plethora of cellular processes via different receptors, but the crosstalk mechanism between M. tuberculosis and HRH1 in macrophages is not clear. Our results revealed that M. tuberculosis infection enhanced HRH1 expression, which in turn restrained macrophage bactericidal activity by modulating the GRK2-p38MAPK signaling pathway, inhibiting NOX2-mediated cROS production and phagosome maturation. Clarification of the underlying mechanism by which M. tuberculosis utilizes host HRH1 to favor its intracellular survival may provide useful information for the development of novel antituberculosis treatments.
结核病(TB)是由单一病原体结核分枝杆菌引起的,是全球十大致命疾病之一。这种情况因耐多药结核病(MDR-TB)和广泛耐药结核病(XDR-TB)病例的增加而加剧。组胺是一种有机含氮化合物,通过不同的受体介导多种细胞过程。迄今为止,已鉴定出的四种组胺受体之一的组胺受体 H1(HRH1)的表达先前被报道在结核分枝杆菌感染时增强,尽管其潜在机制尚不清楚。在本研究中,我们应用共聚焦显微镜、流式细胞术和 Western blot 显示,分枝杆菌感染后巨噬细胞中 HRH1 的表达增强。此外,通过结合基因敲低、免疫沉淀、细胞内细菌负荷分析、荧光标记和成像技术,我们发现结核分枝杆菌靶向宿主 HRH1 以抑制 NOX2 介导的 cROS 产生,并通过 GRK2-p38MAPK 信号通路抑制吞噬体成熟和酸化。我们的研究结果阐明了结核分枝杆菌与宿主 HRH1 相互作用的潜在机制,并可能为新型抗结核治疗的开发提供有用信息。一旦被巨噬细胞吞噬体吞噬,结核分枝杆菌就会采用各种策略利用宿主环境进行细胞内生存。组胺是一种有机含氮化合物,通过不同的受体介导多种细胞过程,但结核分枝杆菌与巨噬细胞中 HRH1 的串扰机制尚不清楚。我们的结果表明,结核分枝杆菌感染增强了 HRH1 的表达,进而通过调节 GRK2-p38MAPK 信号通路、抑制 NOX2 介导的 cROS 产生和吞噬体成熟来抑制巨噬细胞杀菌活性。阐明结核分枝杆菌利用宿主 HRH1 促进其细胞内生存的潜在机制可能为新型抗结核治疗的开发提供有用信息。
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