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Bacterial Secretions of Nonpathogenic Escherichia?coli Elicit Inflammatory Pathways: a Closer Investigation of Interkingdom Signaling

机译:非致病性细菌分泌物大肠杆菌(Escherichia?coli)炎性途径:信号传导信号的更深入研究

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ABSTRACT There have been many studies on the relationship between nonpathogenic bacteria and human epithelial cells; however, the bidirectional effects of the secretomes (secreted substances in which there is no direct bacterium-cell contact) have yet to be fully investigated. In this study, we use a transwell model to explore the transcriptomic effects of bacterial secretions from two different nonpathogenic Escherichia coli strains on the human colonic cell line HCT-8 using next-generation transcriptome sequencing (RNA-Seq). E.?coli BL21 and W3110, while genetically very similar (99.1% homology), exhibit key phenotypic differences, including differences in their production of macromolecular structures (e.g., flagella and lipopolysaccharide) and in their secretion of metabolic byproducts (e.g., acetate) and signaling molecules (e.g., quorum-sensing autoinducer 2 [AI-2]). After analysis of differential epithelial responses to the respective secretomes, this study shows for the first time that a nonpathogenic bacterial secretome activates the NF-κB-mediated cytokine-cytokine receptor pathways while also upregulating negative-feedback components, including the NOD-like signaling pathway. Because of AI-2’s relevance as a bacterium-bacterium signaling molecule and the differences in its secretion rates between these strains, we investigated its role in HCT-8 cells. We found that the expression of the inflammatory cytokine interleukin 8 (IL-8) responded to AI-2 with a pattern of rapid upregulation before subsequent downregulation after 24?h. Collectively, these data demonstrate that secreted products from nonpathogenic bacteria stimulate the transcription of immune-related biological pathways, followed by the upregulation of negative-feedback elements that may serve to temper the inflammatory response. IMPORTANCE The symbiotic relationship between the microbiome and the host is important in the maintenance of human health. There is a growing need to further understand the nature of these relationships to aid in the development of homeostatic probiotics and also in the design of novel antimicrobial therapeutics. To our knowledge, this is the first global-transcriptome study of bacteria cocultured with human epithelial cells in a model to determine the transcriptional effects of epithelial cells in which epithelial and bacterial cells are allowed to “communicate” with each other only through diffusible small molecules and proteins. By beginning to demarcate the direct and indirect effects of bacteria on the gastrointestinal (GI) tract, two-way interkingdom communication can potentially be mediated between host and microbe.
机译:摘要关于非致病性细菌与人类上皮细胞之间关系的研究很多。然而,尚未完全研究分泌蛋白组(没有细菌与细胞直接接触的分泌物质)的双向作用。在这项研究中,我们使用transwell模型,使用下一代转录组测序(RNA-Seq),探索两种不同的非致病性大肠杆菌菌株对人结肠细胞系HCT-8的细菌分泌的转录组学影响。大肠杆菌BL21和W3110,虽然在遗传上非常相似(99.1%同源性),但表现出关键的表型差异,包括它们在大分子结构(例如鞭毛和脂多糖)的产生以及代谢副产物(例如乙酸盐)的分泌方面的差异。和信号分子(例如群体感应自动诱导物2 [AI-2])。在分析了对各个分泌蛋白的差异上皮反应后,该研究首次显示了非致病性细菌分泌蛋白激活了NF-κB介导的细胞因子-细胞因子受体途径,同时还上调了负反馈成分,包括类似NOD的信号传导途径。 。由于AI-2作为细菌-细菌信号分子的相关性以及这些菌株之间其分泌速率的差异,我们研究了其在HCT-8细胞中的作用。我们发现炎性细胞因子白细胞介素8(IL-8)的表达以快速上调的方式响应AI-2,然后在24小时后随后下调。总体而言,这些数据表明,非致病菌的分泌产物刺激了免疫相关生物途径的转录,随后上调了可能抑制炎症反应的负反馈元素。重要信息微生物组与宿主之间的共生关系对于维持人类健康很重要。越来越需要进一步了解这些关系的性质,以帮助开发体内稳态的益生菌,并设计新颖的抗菌药物。据我们所知,这是首次在模型中对与人类上皮细胞共培养的细菌进行全球转录组研究,以确定上皮细胞的转录效应,其中上皮细胞和细菌细胞仅通过可扩散的小分子彼此“交流”和蛋白质。通过开始区分细菌对胃肠道的直接和间接作用,宿主和微生物之间可能会介导双向相互交流。

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