Genome-wide DNA Methylome and Transcriptome Profiling Reveals Key Genes Involved in the Dysregulation of Adipose Stem Cells in Crohn’s Disease

转录组 DNA甲基化 生物 基因组 基因 遗传学 基因表达谱 疾病 干细胞 脂肪组织 计算生物学 基因表达 医学 病理 内分泌学
作者
Diandra Monfort-Ferré,A Boronat-Toscano,José-Francisco Sánchez-Herrero,Aleidis Caro,Margarita Menacho,Irene Vañó‐Segarra,Marc Martí,Beatriz Espina,Raquel Pluvinet,Lidia Cabrinety,Carme Abadia,Miriam Ejarque,Cati Nuñez-Roa,Elsa Maymó‐Masip,Lauro Sumoy,Joan Vendrell,Sonia Fernández‐Veledo,Carolina Serena
出处
期刊:Journal of Crohn's and Colitis [Oxford University Press]
被引量:3
标识
DOI:10.1093/ecco-jcc/jjae072
摘要

Abstract Background and Aims Crohn’s disease [CD] is characterised by the expansion of mesenteric adipose tissue [MAT], named creeping fat [CF], which seems to be directly related to disease activity. Adipose-stem cells [ASCs] isolated from the CF of patients with CD are extremely pro-inflammatory, which persists during disease remission. We hypothesised that the dysfunctional ASCs in CD accumulate epigenetic modifications triggered by the inflammatory environment, that could serve as molecular markers. Methods Genome-wide DNA methylome and transcriptome profiling were performed in ASCs isolated from MAT biopsies of patients with active and inactive disease and from non-Crohn’s disease patients [non-CD]. A validation cohort was used to test the main candidate genes via quantitative polymerase chain reaction in other fat depots and immune cells. Results We found differences in DNA methylation and gene expression between ASCs isolated from patients with CD and from non-CD subjects, but we found no differences related to disease activity. Pathway enrichment analysis revealed that oxidative stress and immune response were significantly enriched in active CD, and integration analysis identified MAB21L2, a cell fate-determining gene, as the most affected gene in CD. Validation analysis confirmed the elevated gene expression of MAB21L2 in MAT and in adipose tissue macrophages in active CD. We also found a strong association between expression of the calcium channel subunit gene CACNA1H and disease remission, as CACNA1H expression was higher in ASCs and MAT from patients with inactive CD, and correlates negatively with C-reactive protein in peripheral blood mononuclear cells. Conclusion We identified a potential gene signature of CD in ASCs obtained from MAT. Integration analysis highlighted two novel genes demonstrating a negative correlation between promoter DNA methylation and transcription: one linked to ASCs in CD [MAB21L2] and the other [CACNA1H] related to disease remission.
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