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结合黏膜微生物组和宿主多组学数据显示出在小儿溃疡性结肠炎中的预后潜力。

Combining mucosal microbiome and host multi-omics data shows prognostic potential in paediatric ulcerative colitis.

作者信息

Kulecka Maria, O'Sullivan Jill, Fitzgerald Rachel, Velikonja Ana, Huseyin Chloe E, Laserna-Mendieta Emilio J, Ruiz-Limón Patricia, Eckenberger Julia, Vidal-Marín Miriam, Truppel Bastian-Alexander, Singh Raminder, Naik Sandhia, Croft Nicholas M, Temko Andriy, Zomer Aldert, MacSharry John, Melgar Silvia, Deb Protima, Sanderson Ian R, Claesson Marcus J

机构信息

APC Microbiome Ireland, University College Cork, Cork, Ireland.

School of Microbiology, University College Cork, Cork, Ireland.

出版信息

Nat Commun. 2025 Aug 4;16(1):7157. doi: 10.1038/s41467-025-62533-z.

Abstract

Current first-line treatments of paediatric ulcerative colitis (UC) maintain a 6-month remission in only half of the patients. Relapse prediction at diagnosis could enable earlier introduction of immunosuppressants. We collected intestinal biopsies from 56 treatment-naïve children, combining mucosal quantitative microbial profiling with host epigenomics, transcriptomics, genotyping, and in vitro and in vivo experiments on selected bacteria. Baseline bacterial diversity is lower in relapsing children, who have fewer butyrate producers but more oral-associated bacteria, whereof Veillonella parvula induces inflammation in epithelial cell lines and IL10 mice. Microbiota has the strongest association with future relapse, followed by host epigenome and transcriptome. Interferon gamma signalling is also linked to relapse-associated bacteria. Relapse-prediction using separate omics data is outperformed by a robust machine learning approach combining microbiomes and epigenomes. In summary, host-microbe data have prognostic potential in paediatric UC. Our translational findings also suggest that pro-inflammatory oral-associated colonizers can exploit the reduced colonic bacterial diversity of relapsing children.

摘要

目前小儿溃疡性结肠炎(UC)的一线治疗仅能使半数患者维持6个月的缓解期。诊断时进行复发预测有助于更早使用免疫抑制剂。我们收集了56名未接受过治疗的儿童的肠道活检样本,将黏膜定量微生物分析与宿主表观基因组学、转录组学、基因分型以及对选定细菌进行的体外和体内实验相结合。复发儿童的基线细菌多样性较低,丁酸产生菌较少,但口腔相关细菌较多,其中小韦荣球菌可在上皮细胞系和IL10小鼠中诱导炎症。微生物群与未来复发的关联最强,其次是宿主表观基因组和转录组。干扰素γ信号传导也与复发相关细菌有关。将微生物组和表观基因组相结合的强大机器学习方法在复发预测方面优于单独使用组学数据。总之,宿主-微生物数据在小儿UC中具有预后潜力。我们的转化研究结果还表明,促炎性口腔相关定植菌可利用复发儿童结肠细菌多样性降低的情况。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/640a/12322004/cd78aa7653f1/41467_2025_62533_Fig1_HTML.jpg

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