Phylotype-level 16S rRNA analysis reveals new bacterial indicators of health state in acute murine colitis

Autor(en)
David Berry, Clarissa Schwab, Gabriel John Milinovich, Karim Ben Mahfoudh, Thomas Decker, Marion Engel, Brigitte Hai, Eva Hainzl, Susanne Heider, Lukas Kenner, Isabella Rauch, Birgit Strobl, Michael Wagner, Christa Schleper, Tim Urich, Alexander Loy
Abstrakt

Human inflammatory bowel disease and experimental colitis models in mice are associated with shifts in intestinal microbiota composition, but it is unclear at what taxonomic/phylogenetic level such microbiota dynamics can be indicative for health or disease. Here, we report that dextran sodium sulfate (DSS)-induced colitis is accompanied by major shifts in the composition and function of the intestinal microbiota of STAT1(-/-) and wild-type mice, as determined by 454 pyrosequencing of bacterial 16S rRNA (gene) amplicons, metatranscriptomics and quantitative fluorescence in situ hybridization of selected phylotypes. The bacterial families Ruminococcaceae, Bacteroidaceae, Enterobacteriaceae, Deferribacteraceae and Verrucomicrobiaceae increased in relative abundance in DSS-treated mice. Comparative 16S rRNA sequence analysis at maximum possible phylogenetic resolution identified several indicator phylotypes for DSS treatment, including the putative mucin degraders Akkermansia and Mucispirillum. The analysis additionally revealed strongly contrasting abundance changes among phylotypes of the same family, particularly within the Lachnospiraceae. These extensive phylotype-level dynamics were hidden when reads were grouped at higher taxonomic levels. Metatranscriptomic analysis provided insights into functional shifts in the murine intestinal microbiota, with increased transcription of genes associated with regulation and cell signaling, carbohydrate metabolism and respiration and decreased transcription of flagellin genes during inflammation. These findings (i) establish the first in-depth inventory of the mouse gut microbiota and its metatranscriptome in the DSS colitis model, (ii) reveal that family-level microbial community analyses are insufficient to reveal important colitis-associated microbiota shifts and (iii) support a scenario of shifting intra-family structure and function in the phylotype-rich and phylogenetically diverse Lachnospiraceae in DSS-treated mice.

Organisation(en)
Department für Mikrobiologie, Immunbiologie und Genetik
Externe Organisation(en)
Helmholtz-Zentrum München - Deutsches Forschungszentrum für Gesundheit und Umwelt, Medizinische Universität Wien, Ludwig Boltzmann Institut für Krebsforschung, Veterinärmedizinische Universität Wien
Journal
The ISME Journal: multidisciplinary journal of microbial ecology
Band
6
Seiten
2091-2106
Anzahl der Seiten
16
ISSN
1751-7362
DOI
https://doi.org/10.1038/ismej.2012.39
Publikationsdatum
11-2012
Peer-reviewed
Ja
ÖFOS 2012
106022 Mikrobiologie
Sustainable Development Goals
SDG 3 – Gesundheit und Wohlergehen
Link zum Portal
https://ucrisportal.univie.ac.at/de/publications/1af12bcc-3e4c-4c1f-a6e2-99c761d94489