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ERX978675: Illumina HiSeq 2500 paired end sequencing; Integrated microbiome and host profiling in a mouse model of colitis suggests host immune activity drives changes in the gut micro-environment that influence both microbial community structure and gene expression
1 ILLUMINA (Illumina HiSeq 2500) run: 35.8M spots, 7.2G bases, 4.4Gb downloads

Design: Integrated microbiome and host profiling in a mouse model of colitis suggests host immune activity drives changes in the gut micro-environment that influence both microbial community structure and gene expression
Submitted by: Kennedy Institute of Rheumatology, University of Oxford (Kennedy Institute of Rheumatology, University of O)
Study: Integrated microbiome and host profiling in a mouse model of colitis suggests host immune activity drives changes in the gut micro-environment that influence both microbial community structure and gene expression
show Abstracthide Abstract
The gut microbiome is significantly altered in inflammatory bowel diseases, but the basis of these changes is not well understood. We have combined metagenomic and metatranscriptomic profiling of the gut microbiome to assess changes to both bacterial community structure and transcriptional activity in a mouse model of colitis. Gene families involved in microbial resistance to oxidative stress, including Dps/ferritin, Fe-dependent peroxidase and glutathione S-transferase, were transcriptionally up-regulated in colitis, implicating a role for increased oxygen tension in gut microbiota modulation. Transcriptional profiling of the host gut tissue and host RNA in the gut lumen revealed a marked increase in the transcription of genes with an activated macrophage and granulocyte signature, suggesting the involvement of these cell types in influencing microbial gene expression. Down-regulation of host glycosylation genes further supports a role for inflammation-driven changes to the gut niche that may impact the microbiome. We propose that members of the bacterial community react to inflammation-associated increased oxygen tension by inducing genes involved in oxidative stress resistance. Furthermore, correlated transcriptional responses between host glycosylation and bacterial glycan utilisation support a role for altered usage of host-derived carbohydrates in colitis.
Sample: rna_stool-aIL10R-R3
SAMEA3403095 • ERS739145 • All experiments • All runs
Organism: Mus musculus
Library:
Name: rna_stool-aIL10R-R3
Instrument: Illumina HiSeq 2500
Strategy: RNA-Seq
Source: METATRANSCRIPTOMIC
Selection: RANDOM
Layout: PAIRED
Construction protocol: intraperitoneal injection of anti-IL10 receptor antibody at days 0 and 7 For simultaneous DNA and RNA extraction, pellets were dissolved in 500 ul extraction buffer (200 mM NaCl, 20 mM EDTA, 4 M guanidine thiocyanate, 1 % (v/v) β-mercaptoethanol) and 210 ul 20 % (w/v) SDS and lysed with a bead beater twice for 2 minutes employing Lysing Matrix E tubes (MP Biomedicals). Samples were centrifuged at 8000 g for 5 minutes and the supernatant was diluted with 3 volumes of lysing buffer (ZR-Duet DNA/RNA Miniprep Kit, Zymo Research). DNA and RNA were further extracted employing the ZR-Duet DNA/RNA Miniprep Kit according to the manufacturer’s instructions. Total RNA was depleted of ribosomal RNA using Epibio’s universal bacteria ribo-zero kit, single version. Libraries were constructed using the NEBNext Ultra directional RNA Library Prep Kit (E7420L).
Spot descriptor:
forward101  reverse

Experiment attributes:
Experimental Factor: disease: none
Experimental Factor: treatment: Intraperitoneal injection of 10mg anti-IL10R antib (show full text...)(hide...)
Intraperitoneal injection of 10mg anti-IL10R antibody on days 0 and 7
LIBRARY_STRAND: not applicable
Runs: 1 run, 35.8M spots, 7.2G bases, 4.4Gb
Run# of Spots# of BasesSizePublished
ERR89929635,796,2867.2G4.4Gb2015-05-23

ID:
1504249

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