粪便元蛋白组学实现了炎症性肠病患者病情缓解的功能特征描述

Maximilian Wolf, Julian Lange, Dirk Benndorf, Lina Welz, Susanna Nikolaus, Laura Katharina Sievers, Florian Tran, Kay Schallert, Patrick Hellwig, Stefan Schreiber, Matthias Gunzer, Philip Rosenstiel, Udo Reichl, Konrad Aden, Robert Heyer
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摘要

背景:肠道微生物组是炎症性肠病(IBD)发病和病程的重要因素。虽然在使用生物制剂治疗 IBD 的过程中观察到了肠道微生物组组成的变化,但阐明人类和微生物蛋白质及通路对治疗成功的依赖性的研究却很少。研究方法在使用三种不同的生物制剂治疗 14 周之前和之后,收集一组 IBD 患者的粪便样本。临床疾病活动评分用于确定临床反应和缓解。对缓解患者(12 人)和非缓解患者(12 人)治疗前的粪便元蛋白组进行比较,并评估两组患者在采样时间内的变化,以确定功能变化以及潜在的人类和微生物生物标记物。结果显示缓解期患者肠道屏障相关蛋白、中性粒细胞和免疫球蛋白的丰度显著下降。相反,在非缓解期患者中观察到这些蛋白质的增加。经过治疗后,缓解期患者样本中的微生物代谢途径发生了重大变化。例如,丁酸发酵产生的蛋白质含量有所增加。最后,还发现了预测和监测治疗成功的新的潜在生物标志物,如人类溶酶体相关膜糖蛋白 1(一种细胞毒性标志物)或微生物蒽酸合成酶成分 2(色氨酸代谢的一部分)。结论无论 IBD 是否缓解,与肠道炎症和肠道微生物组代谢相关的蛋白质都会发生不同的变化。这表明元蛋白质组学可以成为监测 IBD 治疗缓解情况的有用工具。
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Fecal metaproteomics enables functional characterization of remission in patients with inflammatory bowel disease
Background: The gut microbiome is an important contributor to the development and the course of inflammatory bowel disease (IBD). While changes in the gut microbiome composition were observed in response to IBD therapy using biologics, studies elucidating human and microbial proteins and pathways in dependence on therapy success are sparse. Methods: Fecal samples of a cohort of IBD patients were collected before and after 14 weeks of treatment with three different biologics. Clinical disease activity scores were used to determine the clinical response and remission. Fecal metaproteomes of remitting patients (n=12) and of non-remitting patients (n=12) were compared before treatment and changes within both groups were assessed over sampling time to identify functional changes and potential human and microbial biomarkers. Results: The abundance of proteins associated with the intestinal barrier, neutrophilic granulocytes, and immunoglobulins significantly decreased in remitting patients. In contrast, an increase of those proteins was observed in non-remitting patients. There were significant changes in pathways of microbial metabolism in samples from patients with remission after therapy. This included, for example, an increased abundance of proteins from butyrate fermentation. Finally, new potential biomarkers for the prediction and monitoring of therapy success could be identified, e.g. human lysosome-associated membrane glycoprotein 1, a cytotoxicity marker, or microbial anthranilate synthase component 2, a part of the tryptophan metabolism. Conclusions: Distinct changes of proteins related to gut inflammation and gut microbiome metabolism showed whether IBD remission was achieved or not. This suggests that metaproteomics could be a useful tool for monitoring remission in IBD therapies.
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