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Associations between infant fungal and bacterial dysbiosis and childhood atopic wheeze in a nonindustrialized setting

机译:婴儿真菌和细菌脱泻病与儿童特征喘气的关联

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BackgroundAsthma is the most prevalent chronic disease of childhood. Recently, we identified a critical window early in the life of both mice and Canadian infants during which gut microbial changes (dysbiosis) affect asthma development. Given geographic differences in human gut microbiota worldwide, we studied the effects of gut microbial dysbiosis on atopic wheeze in a population living in a distinct developing world environment.ObjectiveWe sought to determine whether microbial alterations in early infancy are associated with the development of atopic wheeze in a nonindustrialized setting.MethodsWe conducted a case-control study nested within a birth cohort from rural Ecuador in which we identified 27 children with atopic wheeze and 70 healthy control subjects at 5爕ears of age. We analyzed bacterial and eukaryotic gut microbiota in stool samples collected at 3爉onths of age using 16S and 18S sequencing. Bacterial metagenomes were predicted from 16S rRNA data by using Phylogenetic Investigation of Communities by Reconstruction of Unobserved States and categorized by function with Kyoto Encyclopedia of Genes and Genomes ontology. Concentrations of fecal short-chain fatty acids were determined by using gas chromatography.ResultsAs previously observed in Canadian infants, microbial dysbiosis at 3爉onths of age was associated with later development of atopic wheeze. However, the dysbiosis in Ecuadorian babies involved different bacterial taxa, was more pronounced, and also involved several fungal taxa. Predicted metagenomic analysis emphasized significant dysbiosis-associated differences in genes involved in carbohydrate and taurine metabolism. Levels of the fecal short-chain fatty acids acetate and caproate were reduced and increased, respectively, in the 3-month stool samples of children who went on to have atopic wheeze.ConclusionsOur findings support the importance of fungal and bacterial microbiota during the first 100燿ays of life on the development of atopic wheeze and provide additional support for considering modulation of the gut microbiome as a primary asthma prevention strategy.
机译:Backgroundsthma是童年最普遍的慢性疾病。最近,我们在小鼠和加拿大婴儿的生命中鉴定了一个关键的窗口,在此期间肠道微生物变化(脱泻)会影响哮喘发育。鉴于全世界人体肠道微生物肿瘤的地理差异,我们研究了肠道微生物消除对生活中不同发展的世界环境中的人口的特应喘息症的影响。目的旨在确定早期婴儿期的微生物改动是否与Atopic喘息的发展有关一项非工业化的设定。甲基丁我们在农村厄瓜多尔嵌套在厄瓜多尔的出生队列内嵌套的病例对照研究,其中我们确定了27名特应见喘息的儿童和70名健康对照受试者的5岁耳朵。我们在使用16s和18s测序的3℃的粪便样品中分析了细菌和真核肠道微生物。通过利用未观察状态的重建,通过使用京都基因和基因组本体论的京都百科全书分类,从16S rRNA数据预测了16S rRNA数据。通过使用气相色谱法测定粪便短链脂肪酸的浓度。先前在加拿大婴儿观察到的方法,3‰年龄的微生物脱泻病患者与后期喘息的后期发育有关。然而,厄瓜多尔婴儿的失益涉及不同的细菌分类群,更加明显,也涉及几个真菌分类群。预测的毕业群分析强调了涉及碳水化合物和牛磺酸代谢的基因的显着脱敏相关差异。醋酸盐和丙烯酸盐的水平分别减少和增加,在继续具有特应患有Atopic喘息的儿童的3个月粪便样本中。结论调查结果支持在前100个中的真菌和细菌微生物的重要性耀致力于开发特应喘息症的生活,并提供额外的支持,以考虑肠道微生物组的调节作为初级哮喘预防策略。

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