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Unravelling the metabolic impact of SBS-associated microbial dysbiosis: Insights from the piglet short bowel syndrome model

机译:揭示SBS相关微生物营养不良的代谢影响:来自仔猪短肠综合征模型的见解

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摘要

Liver disease is a major source of morbidity and mortality in children with short bowel syndrome (SBS). SBS-associated microbial dysbiosis has recently been implicated in the development of SBS-associated liver disease (SBS-ALD), however the pathological implications of this association have not been explored. In this study high-throughput sequencing of colonic content from the well-validated piglet SBS-ALD model was examined to determine alterations in microbial communities, and concurrent metabolic alterations identified in urine samples via targeted mass spectrometry approaches (GC-MS, LC-MS, FIA-MS) further uncovered impacts of microbial disturbance on metabolic outcomes in SBS-ALD. Multi-variate analyses were performed to elucidate contributing SBS-ALD microbe and metabolite panels and to identify microbe-metabolite interactions. A unique SBS-ALD microbe panel was clearest at the genus level, with discriminating bacteria predominantly from the Firmicutes and Bacteroidetes phyla. The SBS-ALD metabolome included important alterations in the microbial metabolism of amino acids and the mitochondrial metabolism of branched chain amino acids. Correlation analysis defined microbe-metabolite clustering patterns unique to SBS-ALD and identified a metabolite panel that correlates with dysbiosis of the gut microbiome in SBS.
机译:肝病是患有短肠综合征(SBS)儿童的发病率和死亡率的主要来源。最近,与SBS相关的微生物营养不良与SBS相关的肝病(SBS-ALD)的发展有关,但是尚未探讨这种相关的病理学意义。在这项研究中,对来自经过充分验证的仔猪SBS-ALD模型的结肠内容物进行高通量测序,以确定微生物群落的变化,并通过靶向质谱分析方法(GC-MS,LC-MS)在尿液样品中鉴定出并发的代谢变化,FIA-MS)进一步揭示了微生物干扰对SBS-ALD代谢结果的影响。进行多变量分析以阐明贡献的SBS-ALD微生物和代谢产物组,并鉴定微生物与代谢物的相互作用。独特的SBS-ALD微生物面板在属水平上最清晰,主要辨别来自Firmicutes和Bacteroidetes phyla的细菌。 SBS-ALD代谢组包括氨基酸的微生物代谢和支链氨基酸的线粒体代谢的重要变化。相关性分析定义了SBS-ALD特有的微生物-代谢物聚集模式,并确定了与SBS中肠道微生物组营养不良相关的代谢物组。

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