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Community-Wide Response of the Gut Microbiota to Enteropathogenic Citrobacter rodentium Infection Revealed by Deep Sequencing ▿

机译:通过深度测序揭示肠道菌群对肠道致病性柠檬酸杆菌的感染的整个社区反应Response

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摘要

We investigated the spatial and temporal response of the murine gut microbiome to infection with Citrobacter rodentium, an attaching-and-effacing bacterium that provokes innate and adaptive immune responses, resulting in transient bacterial colitis. Previous studies have suggested that C. rodentium-induced inflammation is associated with an increased abundance of Enterobacteriaceae. We report here a deeper analysis of this model using DNA bar coding and 454 pyrosequencing to characterize 101,894 partial 16S rRNA gene sequences from 85 microbial samples from tissue-adhered and luminal bacteria of the cecum, proximal colon, and distal colon, which allowed us to identify previously unappreciated spatial and kinetic changes in multiple bacterial lineages. The deep sequencing data revealed that C. rodentium was most abundantly associated with the cecal mucosa at day 9 postinfection and then diminished in abundance, providing the first reported use of deep sequencing to track a pathogen in vivo through the course of infection. Notable changes were associated with both the mucosally adhered and luminal microbiota at both day 9 and day 14 postinfection. Alterations in abundance were seen for Proteobacteria, Deferribacteres, Clostridia, and others; however, changes in Enterobacteriaceae could be accounted for by the presence of C. rodentium itself, which is a member of this family. The Lactobacillus group decreased in abundance during infection, which may be important for pathogenesis because members of this lineage modulate the composition of the gut microbiota and are used as probiotics. Thus, deep sequencing provides previously inaccessible information on how Citrobacter infection and clearance reshapes the gut microbial community in space and time.
机译:我们调查了鼠肠道微生物组对啮齿动物柠檬酸杆菌感染的时空反应,柠檬酸杆菌是一种附着和消灭细菌,会引起先天性和适应性免疫反应,从而导致短暂性细菌性结肠炎。先前的研究表明,啮齿动物衣原体诱导的炎症与肠杆菌科细菌的丰度增加有关。我们在这里报告使用DNA条码和454焦磷酸测序对该模型进行更深入的分析,以表征来自盲肠,近端结肠和远端结肠的组织粘附和腔内细菌的85个微生物样品中101,894个部分16S rRNA基因序列的特征,这使我们能够确定多个细菌谱系中以前未曾意识到的空间和动力学变化。深度测序数据显示,在感染后第9天,啮齿类念珠菌与盲肠粘膜最紧密相关,然后大量减少,这是首次报道了在感染过程中使用深度测序在体内追踪病原体的情况。感染后第9天和第14天,黏膜粘附和腔内菌群均出现显着变化。变形杆菌,去铁杆菌,梭状芽胞杆菌等的丰度发生了变化。但是,肠杆菌科的变化可能是由于啮齿类梭状芽胞杆菌本身的存在而引起的,而啮齿类杆菌是该家族的成员。乳杆菌群在感染期间的丰度下降,这可能对发病机理很重要,因为该谱系的成员调节肠道菌群的组成并被用作益生菌。因此,深度测序提供了以前无法获得的有关柠檬酸杆菌感染和清除如何在空间和时间上重塑肠道微生物群落的信息。

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