克罗恩病静止期症状为何挥之不去？研究产硫微生物和硫代谢途径的影响。

IF 4.5 3区医学 Q1 GASTROENTEROLOGY & HEPATOLOGY

Inflammatory Bowel Diseases Pub Date : 2024-11-14 DOI:10.1093/ibd/izae238

Jonathan Golob, Krishna Rao, Jeffrey A Berinstein, Prashant Singh, William D Chey, Chung Owyang, Nobuhiko Kamada, Peter D R Higgins, Vincent Young, Shrinivas Bishu, Allen A Lee

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引用次数: 0

摘要

导言：即使没有炎症，克罗恩病（CD）患者的持续症状也很普遍，并使生活质量下降。我们以前曾证实，在有持续性消化道症状（qCD + S）和无持续性消化道症状（qCD-S）的静止期克罗恩病患者中，硫化物生成微生物富集。因此，我们假设硫代谢途径将在粪便中富集，而在 qCD + S 中，不同数量的微生物将与重要的硫代谢途径有关：我们在 SPARC IBD 中进行了一项多中心观察性研究。方法：我们在 SPARC IBD 中进行了多中心观察性研究：39 名 qCD + S 患者、274 名 qCD-S 患者、21 名 aCD 患者和 40 名 IBS-D 患者接受了成对猎枪元基因组测序和非靶向代谢组分析。qCD + S患者的粪便代谢组与qCD-S和IBS-D患者有显著差异，但与aCD患者无显著差异。qCD + S患者富含含硫氨基酸途径，包括半胱氨酸和蛋氨酸，以及丝氨酸、甘氨酸和苏氨酸。相对于 qCD-S，谷胱甘肽和烟酸/烟酰胺途径也在 qCD + S 中富集，这表明线粒体功能障碍是 H2S 信号转导的下游目标。多组学整合表明，qCD + S 中富集的微生物与重要的硫代谢途径有关。包括 CTH、isfD、sarD 和 asrC 在内的细菌硫代谢基因在 qCD + S 中调控失调。最后，含硫微生物和不含硫微生物的硫代谢物在预测 qCD + S 的存在方面表现出良好的准确性：讨论：在 qCD + S 中，微生物衍生的硫通路和下游线粒体功能受到干扰，这表明 H2S 信号与这种病症的发病机制有关。未来的研究将确定靶向 H2S 通路是否能改善 qCD + S 患者的生活质量。

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Why Symptoms Linger in Quiescent Crohn's Disease: Investigating the Impact of Sulfidogenic Microbes and Sulfur Metabolic Pathways.

Introduction: Even in the absence of inflammation, persistent symptoms in patients with Crohn's disease (CD) are prevalent and worsen quality of life. We previously demonstrated enrichment in sulfidogenic microbes in quiescent Crohn's disease patients with (qCD + S) vs without persistent GI symptoms (qCD-S). Thus, we hypothesized that sulfur metabolic pathways would be enriched in stool while differentially abundant microbes would be associated with important sulfur metabolic pathways in qCD + S.

Methods: We performed a multicenter observational study nested within SPARC IBD. Quiescent inflammation was defined by fecal calprotectin level < 150 mcg/g. Persistent symptoms were defined by CD-PRO2. Active CD (aCD) and non-IBD diarrhea-predominant irritable bowel syndrome (IBS-D) were included as controls.

Results: Thirty-nine patients with qCD + S, 274 qCD-S, 21 aCD, and 40 IBS-D underwent paired shotgun metagenomic sequencing and untargeted metabolomic profiling. The fecal metabolome in qCD + S was significantly different relative to qCD-S and IBS-D but not aCD. Patients with qCD + S were enriched in sulfur-containing amino acid pathways, including cysteine and methionine, as well as serine, glycine, and threonine. Glutathione and nicotinate/nicotinamide pathways were also enriched in qCD + S relative to qCD-S, suggestive of mitochondrial dysfunction, a downstream target of H2S signaling. Multi-omic integration demonstrated that enriched microbes in qCD + S were associated with important sulfur metabolic pathways. Bacterial sulfur metabolic genes, including CTH, isfD, sarD, and asrC, were dysregulated in qCD + S. Finally, sulfur metabolites with and without sulfidogenic microbes showed good accuracy in predicting the presence of qCD + S.

Discussion: Microbial-derived sulfur pathways and downstream mitochondrial function are perturbed in qCD + S, which implicate H2S signaling in the pathogenesis of this condition. Future studies will determine whether targeting H2S pathways results in improved quality of life in qCD + S.

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来源期刊

Inflammatory Bowel Diseases 医学-胃肠肝病学

CiteScore

9.70

自引率

6.10%

发文量

462

审稿时长

1 months

期刊介绍： Inflammatory Bowel Diseases® supports the mission of the Crohn''s & Colitis Foundation by bringing the most impactful and cutting edge clinical topics and research findings related to inflammatory bowel diseases to clinicians and researchers working in IBD and related fields. The Journal is committed to publishing on innovative topics that influence the future of clinical care, treatment, and research.