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首页> 外文期刊>Infection and immunity >Bordetella pertussis Naturally Occurring Isolates with Altered Lipooligosaccharide Structure Fail To Fully Mature Human Dendritic Cells
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Bordetella pertussis Naturally Occurring Isolates with Altered Lipooligosaccharide Structure Fail To Fully Mature Human Dendritic Cells

机译:百日咳博德特氏菌天然存在的带有改变的脂寡糖结构的分离株无法完全成熟的人树突状细胞

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Bordetella pertussis is a Gram-negative bacterium and the causative agent of whooping cough. Despite high vaccination coverage, outbreaks are being increasingly reported worldwide. Possible explanations include adaptation of this pathogen, which may interfere with recognition by the innate immune system. Here, we describe innate immune recognition and responses to different B. pertussis clinical isolates. By using HEK-Blue cells transfected with different pattern recognition receptors, we found that 3 out of 19 clinical isolates failed to activate Toll-like receptor 4 (TLR4). These findings were confirmed by using the monocytic MM6 cell line. Although incubation with high concentrations of these 3 strains resulted in significant activation of the MM6 cells, it was found to occur mainly through interaction with TLR2 and not through TLR4. When using live bacteria, these 3 strains also failed to activate TLR4 on HEK-Blue cells, and activation of MM6 cells or human monocyte-derived dendritic cells was significantly lower than activation induced by the other 16 strains. Mass spectrum analysis of the lipid A moieties from these 3 strains indicated an altered structure of this molecule. Gene sequence analysis revealed mutations in genes involved in lipid A synthesis. Findings from this study indicate that B. pertussis isolates that do not activate TLR4 occur naturally and that this phenotype may give this bacterium an advantage in tempering the innate immune response and establishing infection. Knowledge on the strategies used by this pathogen in evading the host immune response is essential for the improvement of current vaccines or for the development of new ones.
机译:百日咳博德特氏菌是革兰氏阴性细菌,是百日咳的病原。尽管接种疫苗的覆盖率很高,但世界范围内爆发的疫情越来越多。可能的解释包括对该病原体的适应,这可能会干扰先天免疫​​系统的识别。在这里,我们描述先天免疫识别和不同百日咳博德特氏菌临床分离株的反应。通过使用转染了不同模式识别受体的HEK-Blue细胞,我们发现19种临床分离株中有3种未能激活Toll样受体4(TLR4)。通过使用单核细胞MM6细胞系证实了这些发现。尽管与这3个菌株的高浓度温育导致MM6细胞的显着激活,但发现它主要通过与TLR2相互作用而不是通过TLR4发生。使用活细菌时,这3个菌株也未能激活HEK-Blue细胞上的TLR4,并且MM6细胞或人单核细胞衍生的树突状细胞的激活显着低于其他16个菌株诱导的激活。来自这3个菌株的脂质A部分的质谱分析表明该分子的结构改变。基因序列分析揭示了参与脂质A合成的基因突变。这项研究的发现表明,不激活TLR4的百日咳博德特氏菌分离物是天然存在的,这种表型可以使这种细菌在调节先天免疫应答和建立感染方面具有优势。对该病原体在逃避宿主免疫应答中所使用策略的知识,对于改进当前疫苗或开发新疫苗至关重要。

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