Caroline W Grant, Brian D Juran, Ahmad H Ali, Erik M Schlicht, Jackie K Bianchi, Xin Hu, Yongliang Liang, Zachery Jarrell, Ken H Liu, Young-Mi Go, Dean P Jones, Douglas I Walker, Gary W Miller, Trine Folseraas, Tom H Karlsen, Nicholas F LaRusso, Gregory J Gores, Arjun P Athreya, Konstantinos N Lazaridis
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This novel study utilized state-of-the-art high-resolution mass spectrometry (HRMS) with bile samples to provide the first characterization of environmental chemicals and metabolomics (collectively, the exposome) in PSC patients located in the United States of America (USA) (<i>n</i> = 24) and Norway (<i>n</i> = 30). First, environmental chemical- and metabolome-wide association studies were conducted to assess geographic-based similarities and differences in the bile of PSC patients. Nine environmental chemicals (false discovery rate, FDR < 0.20) and 3143 metabolic features (FDR < 0.05) differed by site. Next, pathway analysis was performed to identify metabolomic pathways that were similarly and differentially enriched by the site. Fifteen pathways were differentially enriched (<i>P</i> < .05) in the categories of amino acid, glycan, carbohydrate, energy, and vitamin/cofactor metabolism. Finally, chemicals and pathways were integrated to derive exposure-effect correlation networks by site. These networks demonstrate the shared and differential chemical-metabolome associations by site and highlight important pathways that are likely relevant to PSC. The USA patients demonstrated higher environmental chemical bile content and increased associations between chemicals and metabolic pathways than those in Norway. Polychlorinated biphenyl (PCB)-118 and PCB-101 were identified as chemicals of interest for additional investigation in PSC given broad associations with metabolomic pathways in both the USA and Norway patients. 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引用次数: 0
摘要
原发性硬化性胆管炎(PSC)是一种复杂的胆管疾病。其病因尚不完全清楚,但环境化学物质可能会增加风险。PSC患者胆汁代谢组改变,可能受到环境化学物质的影响。这项新研究利用最先进的高分辨率质谱法(HRMS)和胆汁样本,首次对美国(n = 24)和挪威(n = 30) PSC患者的环境化学物质和代谢组学(统称为暴露体)进行了表征。首先,进行了环境化学和代谢组全关联研究,以评估PSC患者胆汁的地理相似性和差异性。九种环境化学物质(错误发现率,FDR P
Environmental chemicals and endogenous metabolites in bile of USA and Norway patients with primary sclerosing cholangitis.
Primary sclerosing cholangitis (PSC) is a complex bile duct disorder. Its etiology is incompletely understood, but environmental chemicals likely contribute to risk. Patients with PSC have an altered bile metabolome, which may be influenced by environmental chemicals. This novel study utilized state-of-the-art high-resolution mass spectrometry (HRMS) with bile samples to provide the first characterization of environmental chemicals and metabolomics (collectively, the exposome) in PSC patients located in the United States of America (USA) (n = 24) and Norway (n = 30). First, environmental chemical- and metabolome-wide association studies were conducted to assess geographic-based similarities and differences in the bile of PSC patients. Nine environmental chemicals (false discovery rate, FDR < 0.20) and 3143 metabolic features (FDR < 0.05) differed by site. Next, pathway analysis was performed to identify metabolomic pathways that were similarly and differentially enriched by the site. Fifteen pathways were differentially enriched (P < .05) in the categories of amino acid, glycan, carbohydrate, energy, and vitamin/cofactor metabolism. Finally, chemicals and pathways were integrated to derive exposure-effect correlation networks by site. These networks demonstrate the shared and differential chemical-metabolome associations by site and highlight important pathways that are likely relevant to PSC. The USA patients demonstrated higher environmental chemical bile content and increased associations between chemicals and metabolic pathways than those in Norway. Polychlorinated biphenyl (PCB)-118 and PCB-101 were identified as chemicals of interest for additional investigation in PSC given broad associations with metabolomic pathways in both the USA and Norway patients. Associated pathways include glycan degradation pathways, which play a key role in microbiome regulation and thus may be implicated in PSC pathophysiology.
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