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首页> 外文期刊>Analytica chimica acta >Global profiling and identification of bile acids by multi-dimensional data mining to reveal a way of eliminating abnormal bile acids
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Global profiling and identification of bile acids by multi-dimensional data mining to reveal a way of eliminating abnormal bile acids

机译:多维数据挖掘全球分析和抗胆汁鉴定,揭示消除异常胆汁酸的方法

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Bile acids (BAs), as crucial endogenous metabolites, are closely related to cholestasis, metabolic disorders, and cancer. To better understand their function and disease pathogenesis, global profiling of BAs is necessary. Here, multidimensional data mining was developed for the discovery and identification of potentially unknown BAs in cholestasis rats. Based on an in-house theoretical BA database and using a newly established liquid chromatography-tandem high-resolution mass spectrometry (LC-HRMS/MS) method, four-dimensional (4D) data including the retention times (RT), abundances, HRMS, and HRMS/MS spectra were acquired and elucidated. And 491 BAs were totally profiled. Then, the relationships between RT with different conjugation types, different positions and configurations of hydroxyl/ketone groups as well as fragmentation rules of hydroxyl, ortho-hydroxyl, ketone, and conjugated groups of BAs were summarized to assist BA identification for the first time. Finally, 292 BAs were assigned with molecular formulas, 201 of which were putatively identified by integrating the 4D data, applying structure-driven relative retention time rules, and a comparison with synthetic BAs. The estimated concentrations of 201 BAs, including 93 reported and 108 newly identified BAs, were quantified by using surrogate standards with similar structure. Among 201 BAs, 38 BAs were detected in both humans and rats for the first time. Our strategy has expanded the scope of BAs and provides away to identify a class of metabolites. Compared to normal rats, the significantly increased sulfated and glucuronide conjugated BAs in urine and feces from experimentally cholestatic rats may reveal a way to diagnose intrahepatic cholestasis. (C) 2020 Elsevier B.V. All rights reserved.
机译:作为至关重要的内源代谢物,胆汁酸(BAS)与胆汁淤积,代谢紊乱和癌症密切相关。为了更好地了解其功能和疾病发病机制,必须为BAS的全球分析是必要的。在这里,开发了多维数据挖掘,用于发现和鉴定胆汁淤积大鼠的潜在未知的族。基于内部理论BA数据库,并使用新建立的液相色谱 - 串联高分辨率质谱(LC-HRMS / MS)方法,四维(4D)数据,包括保留时间(RT),丰度,HRMS ,获得并阐明HRMS / MS光谱。和491个BAS完全成熟。然后,概括了具有不同缀合类型,不同的缀合类型,不同位置和羟基/酮基团的碎裂规律的羟基,羟基,酮和缀合物的裂纹组合,首次辅助BA鉴定。最后,通过集成4D数据,应用结构驱动的相对保留时间规则以及与合成BAS的比较,分配292个BAC。通过使用具有相似结构的替代标准,量化201族的估计浓度和108个新鉴定的BAS。在201个BAS中,第一次在人类和大鼠中检测到38个BAC。我们的战略扩大了BAS的范围,并提供了识别一类代谢物。与正常大鼠相比,来自实验胆汁脂肪动物大鼠的尿液和粪便中显着增加的硫酸盐和葡糖醛酸缀合的肺部可能揭示一种诊断肝内胆汁淤积的方法。 (c)2020 Elsevier B.V.保留所有权利。

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