治疗Naïve炎症性肠病的粘膜基因转录特征:欧洲ibd特征队列中疾病与症状对照和健康对照的比较分析

IF 2.5 Q2 GASTROENTEROLOGY & HEPATOLOGY

Clinical and Experimental Gastroenterology Pub Date : 2022-02-11 eCollection Date: 2022-01-01 DOI:10.2147/CEG.S343468

Simen Svendsen Vatn, Jonas Christoffer Lindstrøm, Aina E F Moen, Stephan Brackmann, Tone M Tannæs, Christine Olbjørn, Daniel Bergemalm, Åsa V Keita, Fernando Gomollon, Trond Espen Detlie, Torben Lüders, Rahul Kalla, Alex Adams, Jack Satsangi, Jørgen Jahnsen, Morten H Vatn, Jonas Halfvarson, Petr Ricanek, Hilde Nilsen

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引用次数: 3

摘要

背景:粘膜转录组学的研究为炎性肠病(IBD)的发病机制提供了新的见解。近年来，人们对基因表达特征的生物标志物预测潜力进行了探索。为了进一步研究IBD中的粘膜基因表达，我们招募了一组治疗naïve患者，并将他们与有症状和健康对照进行比较。方法:共纳入323例患者，其中克罗恩病(75例)、溃疡性结肠炎(87例)和IBD未分类(3例)，并设症状对照组(131例)和健康对照组(27例)。在回肠结肠镜检查中收集粘膜活检，并探讨炎症和非炎症粘膜的基因表达。使用Agilent G3 Human Gene expression 860K v3 One-Color芯片进行基因表达谱分析。我们记录了治疗升级到抗tnf药物或手术的信息，以及抗tnf反应，以探索粘膜转录组的预测机会。结果:排除IBD的症状对照者的基因表达谱与IBD患者相似，与健康对照者不同。在非炎症性克罗恩病和溃疡性结肠炎中，基因集富集分析揭示了参与基本细胞生物学过程的途径失调。在非炎症和炎症性克罗恩病和溃疡性结肠炎中，线粒体相关通路均出现失调(>2.6标准化富集评分)。结论:在探索IBD中基因表达特征时，非炎症样本可能优于炎症样本，并可能揭示疾病起始的潜在机制。对照组的基因表达特征与他们是否有症状有关，这可能对未来的研究设计具有重要意义。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Mucosal Gene Transcript Signatures in Treatment Naïve Inflammatory Bowel Disease: A Comparative Analysis of Disease to Symptomatic and Healthy Controls in the European IBD-Character Cohort.

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Mucosal Gene Transcript Signatures in Treatment Naïve Inflammatory Bowel Disease: A Comparative Analysis of Disease to Symptomatic and Healthy Controls in the European IBD-Character Cohort.

Background: Studies of the mucosal transcriptomic landscape have given new insight into the pathogenesis of inflammatory bowel disease (IBD). Recently, the predictive biomarker potential of gene expression signatures has been explored. To further investigate the mucosal gene expression in IBD, we recruited a cohort of treatment naïve patients and compared them to both symptomatic and healthy controls.

Methods: Altogether, 323 subjects were included: Crohn's disease (N = 75), ulcerative colitis (N = 87) and IBD unclassified (N = 3). Additionally, there were two control groups: symptomatic controls (N = 131) and healthy controls (N = 27). Mucosal biopsies were collected during ileocolonoscopy and gene expression in inflamed and non-inflamed mucosa was explored. Gene expression profiling was performed using Agilent G3 Human Gene Expression 860K v3 One-Color microarray. We recorded information about treatment escalation to anti-TNF agents or surgery, and anti-TNF response, to explore predictive opportunities of the mucosal transcriptome.

Results: Gene expression profiles in symptomatic controls in whom IBD had been excluded resembled that of IBD patients and diverged from that of healthy controls. In non-inflamed Crohn's disease and ulcerative colitis, gene set enrichment analysis revealed dysregulation of pathways involved in basic cellular biological processes. Mitochondria-associated pathways were dysregulated both in non-inflamed and inflamed Crohn's disease and ulcerative colitis (>2.6 normalized enrichment scores <-1.8). Gene expression signatures of Crohn's disease and ulcerative colitis did not predict time for treatment escalation (p = 0.175). No significant association was found between gene expression signatures and anti-TNF response.

Conclusion: Non-inflamed samples are probably superior to inflamed samples when exploring gene expression signatures in IBD and might reveal underlying mechanisms central for disease initiation. The gene expression signatures of the control groups were related to if they were symptomatic or not, which may have important implications for future study designs.

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来源期刊

Clinical and Experimental Gastroenterology GASTROENTEROLOGY & HEPATOLOGY-

CiteScore

5.10

自引率

0.00%

发文量

审稿时长

16 weeks