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Influenza A virus-mediated priming enhances cytokine secretion by human dendritic cells infected with Streptococcus pneumoniae

机译:甲型流感病毒介导的引发增强了被肺炎链球菌感染的人树突状细胞分泌的细胞因子

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Secondary infections with Streptococcus pneumoniae (SP) are frequently observed following influenza A virus (IAV) infection and have a substantial impact on global health. Despite this, the basis for the disease progression is incompletely understood. To investigate the effect of co-infection on human monocyte-derived dendritic cells (MDDCs) we analysed the expression of clinically important pro-inflammatory and immune-modulatory cytokines. IAV infection or treatment with supernatants from IAV-infected cell cultures resulted in priming of the DCs which subsequently influenced the production of IL-12p70, as well as IL-6, following SP infection. Co-infection of the same cell was not required but this effect was dependent on the time, dose and duration of the infections, as well as pathogen viability, bacterial uptake and endosome acidification. Bacterially infected cells were characterized as the main producers of IL-12p70. Finally, we showed that type I interferons were primarily responsible for the priming of IL-12p70 that was observed by infection with IAV. These results provide a probable mechanism for the elevated levels of particular cytokines observed in IAV and SP co-infected cell cultures with implications for the pathogenic outcome observed during in vivo infection.
机译:甲型流感病毒(IAV)感染后常会发生继发性肺炎链球菌(SP)感染,并对全球健康产生重大影响。尽管如此,仍未完全了解疾病进展的基础。为了研究共感染对人单核细胞来源的树突状细胞(MDDC)的影响,我们分析了临床上重要的促炎和免疫调节细胞因子的表达。 IAV感染或用IAV感染的细胞培养物的上清液处理导致DC引发,随后在SP感染后影响DC的IL-12p70和IL-6的产生。不需要同时感染同一细胞,但是这种效果取决于感染的时间,剂量和持续时间,以及病原体的生存力,细菌的吸收和内体酸化。被细菌感染的细胞被表征为IL-12p70的主要产生者。最后,我们表明I型干扰素主要是通过IAV感染观察到的IL-12p70引发。这些结果为IAV和SP共感染细胞培养物中观察到的特定细胞因子水平升高提供了可能的机制,并暗示了在体内感染期间观察到的致病结果。

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