FECAL CALPROTECTIN AND INTESTINAL METABOLITES: WHAT IS THEIR IMPORTANCE IN THE ACTIVITY AND DIFFERENTIATION OF PATIENTS WITH INFLAMMATORY BOWEL DISEASES?

Arquivos brasileiros de cirurgia digestiva : ABCD = Brazilian archives of digestive surgery Pub Date : 2025-02-28 eCollection Date: 2025-01-01 DOI:10.1590/0102-6720202500001e1870

Lucas Correia Lins, Júnia Elisa Carvalho DE-Meira, Camila Wanderley Pereira, Alessandre Carmo Crispim, Marina Demas Rezende Gischewski, Manoel Álvaro de Freitas Lins-Neto, Fabiana Andréa Moura

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Abstract

Background: Inflammatory bowel disease (IBD), comprising Crohn's disease (CD) and ulcerative colitis (UC), lacks a known etiology. Although clinical symptoms, imaging, and colonoscopy are common diagnostic tools, fecal calprotectin (FC) serves as a widely used biomarker to track disease activity. Metabolomics, within the omics sciences, holds promise for identifying disease progression biomarkers. This approach involves studying metabolites in biological media to uncover pathological factors.

Aims: The purpose of this study was to explore fecal metabolomics in IBD patients, evaluate its potential in differentiating subtypes, and assess disease activity using FC.

Methods: Cross-sectional study including IBD patients, clinical data, and FC measurements (=200 μg/g as an indicator of active disease).

Results: Fecal metabolomics utilized chromatography mass spectrometry/solid phase microextraction with MetaboAnalyst 5.0 software for analysis. Of 52 patients (29 UC, 23 CD), 36 (69.2%) exhibited inflammatory activity. We identified 56 fecal metabolites, with hexadecanoic acid, squalene, and octadecanoic acid notably distinguishing CD from UC. For UC, octadecanoic and hexadecanoic acids correlated with disease activity, whereas octadecanoic acid was most relevant in CD.

Conclusions: These findings highlight the potential of metabolomics as a noninvasive complement for evaluating IBD, aiding diagnosis, and assessing disease activity.

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粪钙保护蛋白和肠道代谢产物：它们在炎症性肠病患者的活动和分化中的重要性是什么？

背景：炎症性肠病（IBD），包括克罗恩病（CD）和溃疡性结肠炎（UC），缺乏已知的病因。虽然临床症状、影像学和结肠镜检查是常见的诊断工具，但粪便钙保护蛋白（FC）作为一种广泛使用的生物标志物来跟踪疾病活动。代谢组学，在组学科学中，有望识别疾病进展的生物标志物。这种方法包括研究生物介质中的代谢物以揭示病理因素。目的：本研究的目的是探索IBD患者的粪便代谢组学，评估其在区分亚型方面的潜力，并使用FC评估疾病活动性。方法：采用横断面研究，包括IBD患者、临床资料和FC测量（=200 μg/g作为活动性疾病的指标）。结果：粪便代谢组学采用色谱-质谱/固相微萃取技术，使用MetaboAnalyst 5.0软件进行分析。52例患者（29例UC， 23例CD）中，36例（69.2%）表现出炎症活动。我们鉴定了56种粪便代谢物，其中十六烷酸、角鲨烯和十八烷酸显著区分了CD和UC。对于UC，十八烷酸和十六烷酸与疾病活动性相关，而十八烷酸与cd最相关。结论：这些发现突出了代谢组学作为评估IBD、辅助诊断和评估疾病活动性的非侵入性补充的潜力。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Arquivos brasileiros de cirurgia digestiva : ABCD = Brazilian archives of digestive surgery

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