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通过组织代谢组学分析,氨基酸和脂质代谢的差异可以区分克罗恩病和特发性/隐窝腺源性肛门直肠瘘,这可能为潜在的发病机制提供线索。

Differences in amino acid and lipid metabolism distinguish Crohn's from idiopathic/cryptoglandular perianal fistulas by tissue metabonomic profiling and may offer clues to underlying pathogenesis.

机构信息

Robin Phillips Fistula Research Unit, St Mark's Hospital and Academic Institute, Harrow, Middlesex.

Department of Surgery and Cancer.

出版信息

Eur J Gastroenterol Hepatol. 2021 Dec 1;33(12):1469-1479. doi: 10.1097/MEG.0000000000001976.

Abstract

INTRODUCTION

Few studies have investigated perianal fistula etiopathogenesis, and although the cryptoglandular theory is widely accepted in idiopathic cases, in Crohn's disease, it is thought to involve the interplay between microbiological, immunological and genetic factors. A pilot study was conducted to assess for metabolic variations in Crohn's perianal fistula tissue that might differ from that of idiopathic (cryptoglandular) perianal fistula tissue as a comparator. The goal was to identify any potential biomarkers of disease, which may improve the understanding of pathogenesis.

AIMS AND METHODS

Fistula tract biopsies were obtained from 30 patients with idiopathic perianal fistula and 20 patients with Crohn's anal fistula. Two different assays were used in an ultra-high-performance liquid chromatography system coupled with a mass spectrometric detector to achieve broad metabolome coverage. Univariate and multivariate statistical data analyses were used to identify differentiating metabolic features corresponding to the perianal fistula phenotype (i.e. Crohn's disease vs. idiopathic).

RESULTS

Significant orthogonal partial least squares discriminant analysis predictive models (validated with cross-validated-analysis of variance P value <0.05) differentiated metabolites from tissue samples from Crohn's vs. idiopathic anal fistula patients using both metabolic profiling platforms. A total of 41 metabolites were identified, suggesting alterations in pathways, including amino acid, carnitine and lipid metabolism.

CONCLUSION

Metabonomics may reveal biomarkers of Crohn's perianal fistula. Further work in larger numbers is required to validate the findings of these studies as well as cross-correlation with microbiome work to better understand the impact of host-gut/environment interactions in the pathophysiology of Crohn's and idiopathic perianal fistulas and identify novel therapeutic targets.

摘要

简介

很少有研究调查肛周瘘管的病因发病机制,尽管隐窝腺理论在特发性病例中被广泛接受,但在克罗恩病中,它被认为涉及微生物、免疫和遗传因素的相互作用。进行了一项试点研究,以评估克罗恩病肛周瘘管组织中的代谢变化,这些变化可能与作为对照的特发性(隐窝腺)肛周瘘管组织不同。目的是确定任何潜在的疾病生物标志物,这可能有助于更好地了解发病机制。

目的和方法

从 30 例特发性肛周瘘管和 20 例克罗恩病肛周瘘管患者中获得瘘管组织活检。使用两种不同的分析方法,在超高效液相色谱系统与质谱检测器耦合的系统中,实现广泛的代谢组覆盖。使用单变量和多变量统计数据分析来确定与肛周瘘管表型(即克罗恩病与特发性)相对应的区分代谢特征。

结果

使用两种代谢组学平台,显著的正交偏最小二乘判别分析预测模型(经交叉验证方差分析 P 值<0.05 验证)区分了来自克罗恩病与特发性肛周瘘管患者组织样本的代谢物。共鉴定出 41 种代谢物,提示氨基酸、肉碱和脂质代谢等途径发生改变。

结论

代谢组学可能揭示克罗恩病肛周瘘管的生物标志物。需要进一步在更大数量的患者中进行验证,以及与微生物组学工作的交叉相关性研究,以更好地理解宿主-肠道/环境相互作用对克罗恩病和特发性肛周瘘管的病理生理学的影响,并确定新的治疗靶点。

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