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来自人类肠道的活性和分泌型IgA包被细菌组分揭示了一个代表性不足的微生物群核心。

Active and secreted IgA-coated bacterial fractions from the human gut reveal an under-represented microbiota core.

作者信息

D'Auria Giuseppe, Peris-Bondia Francesc, Džunková Mária, Mira Alex, Collado Maria Carmen, Latorre Amparo, Moya Andrés

机构信息

1] Joint Unit of Research in Genomics and Health, Centre for Public Health Research (CSISP) - Cavanilles Institute for Biodiversity and Evolutionary Biology (University of Valencia), Valencia, 46020; Spain [2] CIBER Epidemiología y Salud Pública (CIBERESP); Spain [3].

1] Joint Unit of Research in Genomics and Health, Centre for Public Health Research (CSISP) - Cavanilles Institute for Biodiversity and Evolutionary Biology (University of Valencia), Valencia, 46020; Spain [2] CIBER Epidemiología y Salud Pública (CIBERESP); Spain.

出版信息

Sci Rep. 2013 Dec 17;3:3515. doi: 10.1038/srep03515.

Abstract

Host-associated microbiota varies in distribution depending on the body area inhabited. Gut microbes are known to interact with the human immune system, maintaining gut homoeostasis. Thus, we studied whether secreted-IgA (S-IgA) coat specific microbial taxa without inducing strong immune responses. To do so, we fractionated gut microbiota by flow cytometry. We found that active and S-IgA-coated bacterial fractions were characterized by a higher diversity than those observed in raw faecal suspensions. A long-tail effect was observed in family distribution, revealing that rare bacteria represent up to 20% of total diversity. While Firmicutes was the most abundant phylum, the majority of its sequences were not assigned at the genus level. Finally, the single-cell-based approach enabled us to focus on active and S-IgA-coated bacteria. Thus, we revealed a microbiota core common to the healthy volunteers participating in the study. Interestingly, this core was composed mainly of low frequency taxa (e.g. Sphingomonadaceae).

摘要

与宿主相关的微生物群的分布因所栖息的身体部位而异。已知肠道微生物与人类免疫系统相互作用,维持肠道内环境稳定。因此,我们研究了分泌型免疫球蛋白A(S-IgA)是否能包裹特定的微生物类群而不引发强烈的免疫反应。为此,我们通过流式细胞术对肠道微生物群进行了分级分离。我们发现,活跃的和被S-IgA包裹的细菌级分的特征是其多样性高于原始粪便悬液中的细菌。在科的分布中观察到长尾效应,表明稀有细菌占总多样性的比例高达20%。虽然厚壁菌门是最丰富的菌门,但其大多数序列在属水平上未被归类。最后,基于单细胞的方法使我们能够专注于活跃的和被S-IgA包裹的细菌。因此,我们揭示了参与该研究的健康志愿者共有的微生物群核心。有趣的是,这个核心主要由低频类群(如鞘脂单胞菌科)组成。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3476/3865468/ba7fa037cdca/srep03515-f1.jpg

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