全基因组 DNA 甲基组和转录组分析揭示了克罗恩病中脂肪干细胞失调的关键基因。

Diandra Monfort-Ferré, Albert 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 Maymo-Masip, Lauro Sumoy, Joan Vendrell, Sonia Fernández-Veledo, Carolina Serena
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引用次数: 0

摘要

背景和目的:克罗恩病(CD)的特征是肠系膜脂肪组织(MAT)的扩张,被称为 "爬行脂肪"(CF),这似乎与疾病活动直接相关。从 CD 患者的肠系膜脂肪组织中分离出的脂肪干细胞(ASCs)具有极强的促炎性,这种情况在疾病缓解期间依然存在。我们推测,CD 患者功能失调的 ASCs 积累了由炎症环境引发的表观遗传修饰,这些修饰可作为分子标记:方法:我们对从活动性和非活动性克罗恩病患者以及非克罗恩病患者(非 CD)的 MAT 脂肪组织活检组织中分离出的 ASCs 进行了全基因组 DNA 甲基组和转录组分析。在其他脂肪库和免疫细胞中通过 qPCR 对主要候选基因进行了验证:结果:我们发现从 CD 患者和非 CD 患者体内分离出的 ASCs 在 DNA 甲基化和基因表达方面存在差异,但与疾病活动性无关。通路富集分析表明,氧化应激和免疫反应在活动性 CD 中明显富集,整合分析发现细胞命运决定基因 MAB21L2 是 CD 中受影响最大的基因。验证分析证实,在活动性 CD 中,MAT 和脂肪组织巨噬细胞中的 MAB21L2 基因表达升高。我们还发现了钙通道亚基基因 CACNA1H 的表达与疾病缓解之间的密切联系,因为在非活动性 CD 患者的 ASCs 和 MAT 中,CACNA1H 的表达较高,并且与外周血单核细胞中的 C 反应蛋白呈负相关:我们在从 MAT 中获得的 ASCs 中发现了 CD 的潜在基因特征。整合分析突出显示了启动子 DNA 甲基化与转录呈负相关的两个新基因:一个与 CD 中的 ASCs 有关(MAB21L2),另一个与疾病缓解有关(CACNA1H)。
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Genome-wide DNA Methylome and Transcriptome Profiling Reveals Key Genes Involved in the Dysregulation of Adipose Stem Cells in Crohn's Disease.

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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