Comprehensive bile acid profiling in hereditary intrahepatic cholestasis: Genetic and clinical correlations

胆盐出口泵 胆汁淤积 胆汁酸 进行性家族性肝内胆汁淤积症 胆酸 内科学 熊去氧胆酸 胃肠病学 医学 生物 内分泌学 生物化学 基因 运输机 肝移植 移植
作者
Teng Liu,Ren‐Xue Wang,Jun Han,Chenzhi Hao,Yi‐Ling Qiu,Yanyan Yan,Liting Li,Neng‐Li Wang,Jing‐Yu Gong,Yi Lu,Meihong Zhang,Xin‐Bao Xie,Juncong Yang,Yi‐Jie You,Jiaqi Li,A. S. Knisely,Christoph H. Borchers,Victor Ling,Jian‐She Wang
出处
期刊:Liver International [Wiley]
卷期号:38 (9): 1676-1685 被引量:18
标识
DOI:10.1111/liv.13714
摘要

Genetic defects causing dysfunction in bile salt export pump (BSEP/ABCB11) lead to liver diseases. ABCB11 mutations alter the bile acid metabolome. We asked whether profiling plasma bile acids could reveal compensatory mechanisms and track genetic and clinical status.We compared plasma bile acids in 17 ABCB11-mutated patients, 35 healthy controls and 12 genetically undiagnosed cholestasis patients by ultra-high-performance liquid chromatography/multiple-reaction monitoring-mass spectrometry (UPLC/MRM-MS). We developed an index to rank bile acid hydrophobicity, and thus toxicity, based on LC retention times. We recruited 42 genetically diagnosed hereditary cholestasis patients, of whom 12 were presumed to have impaired BSEP function but carried mutations in genes other than ABCB11, and 8 healthy controls, for further verification.The overall hydrophobicity indices of total bile acids in both the ABCB11-mutated group (11.89 ± 1.07 min) and the undiagnosed cholestasis group (11.46 ± 1.07 min) were lower than those of healthy controls (13.69 ± 0.77 min) (both p < 0.005). This was owing to increased bile acid modifications. Secondary bile acids were detected in patients without BSEP expression, suggesting biliary bile acid secretion through alternative routes. A diagnostic panel comprising lithocholic acid (LCA), tauro-LCA, glyco-LCA and hyocholic acid was identified that could differentiate the ABCB11-mutated cohort from healthy controls and undiagnosed cholestasis patients (AUC=0.946, p < 0.0001) and, in non-ABCB11-mutated cholestasis patients, could distinguish BSEP dysfunction from normal BSEP function (9/12 vs 0/38, p < 0.0000001).Profiling of plasma bile acids has provided insights into cholestasis alleviation and may be useful for the clinical management of cholestatic diseases.

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