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Expression of Proinflammatory and Regulatory Cytokines via NF-κB and MAPK-Dependent and IFN Regulatory Factor-3-Independent Mechanisms in Human Primary Monocytes Infected by Mycobacterium tuberculosis

机译:结核分枝杆菌感染人原代单核细胞中通过NF-κB和MAPK依赖性和IFN调节因子3独立机制的促炎和调节细胞因子的表达。

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摘要

Knowledge of the molecular events regulating the innate response to Mycobacterium tuberculosis (Mtb) is critical for understanding immunological pathogenesis and protection from tuberculosis. To this aim, the regulation and the expression of regulatory and proinflammatory cytokines were investigated in human primary monocytes upon Mtb infection. We found that Mtb-infected monocytes preferentially express a proinflammatory cytokine profile, including IL-6, TNF-α, and IL-1β. Conversely, among the regulatory cytokines, Mtb elicited IL-10 and IL-23 release while no expression of IL-12p70, IL-27, and IFN-β was observed. The analysis of the signalling pathways leading to this selective cytokine expression showed that in monocytes Mtb activates MAPK and NF-κB but is unable to stimulate IRF-3 phosphorylation, a transcription factor required for IL-12p35 and IFN-β gene expression. Thus, by inducing a specific cytokine profile, Mtb can influence the immunoregulatory properties of monocytes, which represent important target of novel vaccinal strategies against Mtb infection.
机译:对调节对结核分枝杆菌(Mtb)的先天反应的分子事件的了解对于理解免疫发病机理和对结核的保护至关重要。为了这个目的,研究了Mtb感染后人原代单核细胞中调节性和促炎性细胞因子的调节和表达。我们发现感染Mtb的单核细胞优先表达促炎性细胞因子谱,包括IL-6,TNF-α和IL-1β。相反,在调节性细胞因子中,Mtb引起IL-10和IL-23释放,而未观察到IL-12p70,IL-27和IFN-β的表达。对导致这种选择性细胞因子表达的信号通路的分析表明,在单核细胞中,Mtb激活MAPK和NF-κB,但不能刺激IRF-3磷酸化(IL-12p35和IFN-β基因表达所需的转录因子)。因此,通过诱导特定的细胞因子谱,Mtb可以影响单核细胞的免疫调节特性,这是针对Mtb感染的新型疫苗策略的重要目标。

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