Differential responses of human dendritic cells to metabolites from the oral/airway microbiome

K. Whiteson, S. Agrawal, A. Agrawal
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引用次数: 12

Abstract

Small molecule metabolites that are produced or altered by host‐associated microbial communities are emerging as significant immune response modifiers. However, there is a key gap in our knowledge of how oral microbial metabolites affect the immune response. Here, we examined the effects of metabolites from five bacterial strains found commonly in the oral/airway microbial communities of humans. The five strains, each isolated from cystic fibrosis patient sputum, were Pseudomonas aeruginosa FLR01 non‐mucoid (P1) and FLR02 mucoid (P2) forms, Streptococcus pneumoniae (Sp), S. salivarius (Ss) and Rothia mucilaginosa (Rm). The effect of bacterial metabolites on dendritic cell (DC) activation, T cell priming and cytokine secretion was determined by exposing DCs to bacterial supernatants and individual metabolites of interest. Supernatants from P1 and P2 induced high levels of tumour necrosis factor (TNF)‐α, interleukin (IL)−12 and IL‐6 from DCs and primed T cells to secrete interferon (IFN)‐γ, IL‐22 compared to supernatants from Sp, Ss and Rm. Investigations into the composition of supernatants using gas chromatography–mass spectroscopy (GC‐MS) revealed signature metabolites for each of the strains. Supernatants from P1 and P2 contained high levels of putrescine and glucose, while Sp and Ss contained high levels of 2,3‐butanediol. The individual metabolites replicated the results of whole supernatants, although the magnitudes of their effects were reduced significantly. Altogether, our data demonstrate for the first time that the signature metabolites produced by different bacteria have different effects on DC functions. The identification of signature metabolites and their effects on the host immune system can provide mechanistic insights into diseases and may also be developed as biomarkers.
人类树突状细胞对口腔/气道微生物组代谢物的差异反应
宿主相关微生物群落产生或改变的小分子代谢物正成为重要的免疫反应调节剂。然而,我们对口服微生物代谢物如何影响免疫反应的了解还存在一个关键的空白。在这里,我们研究了人类口腔/气道微生物群落中常见的五种细菌菌株的代谢物的影响。从囊性纤维化患者的痰中分离得到5株菌株,分别为铜绿假单胞菌FLR01非黏液样菌(P1)和FLR02黏液样菌(P2),肺炎链球菌(Sp),唾液链球菌(Ss)和粘液罗氏菌(Rm)。细菌代谢物对树突状细胞(DC)活化、T细胞启动和细胞因子分泌的影响通过将DC暴露于细菌上清液和感兴趣的个体代谢物来确定。与Sp、Ss和Rm的上清液相比,P1和P2的上清液诱导dc中高水平的肿瘤坏死因子(TNF)‐α、白细胞介素(IL)−12和IL‐6,并诱导T细胞分泌干扰素(IFN)‐γ、IL‐22。利用气相色谱-质谱(GC - MS)对上清液的组成进行了研究,揭示了每种菌株的特征代谢物。P1和P2的上清液含有高水平的腐胺和葡萄糖,而Sp和Ss含有高水平的2,3 -丁二醇。单个代谢物复制了整个上清的结果,尽管它们的影响程度显着降低。总之,我们的数据首次证明了不同细菌产生的特征代谢物对DC功能有不同的影响。特征代谢物的鉴定及其对宿主免疫系统的影响可以提供疾病的机制见解,也可以开发为生物标志物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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