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Accession: PRJNA471054 ID: 471054

Transcriptome analysis of IFNγ producing and non-producing CD4 T cells during chronic intestinal inflammation. (house mouse)

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Purpose: The goal of this study is to compare transcriptome profiles of IFNγ producing (Thy1.1+) and IFNγ non-producing (Thy1.1-) CD4 T cells during chronic intestinal inflammation using RNA sequencing. Methods: Total mRNA was isolated from FACS sorted CD44+Thy1.1+ and CD44+Thy1.1-CD4 T cells and sequenced in duplicate using Illumina HiSeq 2500 (2x100 base pair, paired-end reads). The sequence reads were aligned using mouse GRCm38.75 reference genome. DESeq2 software was used for differential expression analysis. Results: Differential expression analysis with DESeq2 algorithm revealed that a total of 942 and 1091 genes were significantly increased in the IFNγ+ and IFNγ- effector CD4 T cells, respectively (adjusted p value <0.05). We also performed gene set enrichment analysis (GSEA) by pre-ranking RNA sequencing data according to an adjusted p-value and the sign of differential expression. GSEA regults suggested that IFNγ+ CD4 T cells had terminally differentiated phenotype, while IFNγ- CD4 T cells had transcriptional profile associated with self-renewal and stemness. Conclusions: Our study suggests that effector CD4 T cells exist in a spectrum of differentiation status during chronic intestinal inflammation, which impacts pathogenicity of CD4 T cells. Overall design: mRNA profiles of IFNγ producing and non-producing CD4 T cells during chronic intestinal inflammation.
AccessionPRJNA471054; GEO: GSE114346
Data TypeTranscriptome or Gene expression
ScopeMultiisolate
OrganismMus musculus[Taxonomy ID: 10090]
Eukaryota; Metazoa; Chordata; Craniata; Vertebrata; Euteleostomi; Mammalia; Eutheria; Euarchontoglires; Glires; Rodentia; Myomorpha; Muroidea; Muridae; Murinae; Mus; Mus; Mus musculus
PublicationsShin B et al., "Effector CD4 T cells with progenitor potential mediate chronic intestinal inflammation.", J Exp Med, 2018 Jul 2;215(7):1803-1812
SubmissionRegistration date: 11-May-2018
University of Alabama at Birmingham
RelevanceModel Organism
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Data volume, Supplementary Mbytes4
SRA Data Details
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Data volume, Gbases62
Data volume, Mbytes22191

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