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BackgroundAlthough a majority of patients with PSC have colitis [PSC-IBD; primary sclerosing cholangitis-inflammatory bowel disease], this is phenotypically different from ulcerative colitis [UC]. We sought to define further the pathophysiological differences between PSC-IBD and UC, by applying a comparative and integrative approach to colonic gene expression, gut microbiota and immune infiltration data.MethodsColonic biopsies were collected from patients with PSC-IBD [n = 10], UC [n = 10], and healthy controls [HC; n = 10]. Shotgun RNA-sequencing for differentially expressed colonic mucosal genes [DEGs], 16S rRNA analysis for microbial profiling, and immunophenotyping were performed followed by multi-omic integration.ResultsThe colonic transcriptome differed significantly between groups [p = 0.01]. Colonic transcriptomes from HC were different from both UC [1343 DEGs] and PSC-IBD [4312 DEGs]. Of these genes, only 939 had shared differential gene expression in both UC and PSC-IBD compared with HC. Imputed pathways were predominantly associated with upregulation of immune response and microbial defense in both disease cohorts compared with HC. There were 1692 DEGs between PSC-IBD and UC. Bile acid signalling pathways were upregulated in PSC-IBD compared with UC [p = 0.02]. Microbiota profiles were different between the three groups [p = 0.01]; with inferred function in PSC-IBD also being consistent with dysregulation of bile acid metabolism. Th17 cells and IL17-producing CD4 cells were increased in both PSC-IBD and UC when compared with HC [p ConclusionsColonic transcriptomic and microbiota analysis in PSC-IBD point toward dysregulation of colonic bile acid homeostasis compared with UC. This highlights important mechanisms and suggests the possibility of novel approaches in treating PSC-IBD.

Original publication

DOI

10.1093/ecco-jcc/jjaa021

Type

Journal article

Journal

Journal of Crohn's & colitis

Publication Date

07/2020

Volume

14

Pages

935 - 947

Addresses

Institute of Cancer and Genomic Sciences, University of Birmingham, Birmingham, UK.

Keywords

Intestinal Mucosa, Colon, Humans, Cholangitis, Sclerosing, Colitis, Ulcerative, Bile Acids and Salts, RNA, Ribosomal, 16S, Interleukin-17, Case-Control Studies, Sequence Analysis, RNA, Immunophenotyping, Computational Biology, Signal Transduction, Immunity, Up-Regulation, Homeostasis, Adult, Middle Aged, Female, Male, Th17 Cells, Transcriptome, Gastrointestinal Microbiome