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Mass Spectrometry-Based Proteomics Reveal Alcohol Dehydrogenase 1B as a Blood Biomarker Candidate to Monitor Acetaminophen-Induced Liver Injury
Authors:Floriane Pailleux  Pauline Maes  Michel Jaquinod  Justine Barthelon  Marion Darnaud  Claire Lacoste  Yves Vandenbrouck  Benoît Gilquin  Mathilde Louwagie  Anne-Marie Hesse  Alexandra Kraut  Jrme Garin  Vincent Leroy  Jean-Pierre Zarski  Christophe Bruley  Yohann Cout  Didier Samuel  Philippe Ichai  Jamila Faivre  Virginie Brun
Abstract:Acute liver injury (ALI) is a severe disorder resulting from excessive hepatocyte cell death, and frequently caused by acetaminophen intoxication. Clinical management of ALI progression is hampered by the dearth of blood biomarkers available. In this study, a bioinformatics workflow was developed to screen omics databases and identify potential biomarkers for hepatocyte cell death. Then, discovery proteomics was harnessed to select from among these candidates those that were specifically detected in the blood of acetaminophen-induced ALI patients. Among these candidates, the isoenzyme alcohol dehydrogenase 1B (ADH1B) was massively leaked into the blood. To evaluate ADH1B, we developed a targeted proteomics assay and quantified ADH1B in serum samples collected at different times from 17 patients admitted for acetaminophen-induced ALI. Serum ADH1B concentrations increased markedly during the acute phase of the disease, and dropped to undetectable levels during recovery. In contrast to alanine aminotransferase activity, the rapid drop in circulating ADH1B concentrations was followed by an improvement in the international normalized ratio (INR) within 10–48 h, and was associated with favorable outcomes. In conclusion, the combination of omics data exploration and proteomics revealed ADH1B as a new blood biomarker candidate that could be useful for the monitoring of acetaminophen-induced ALI.
Keywords:bioinformatics  proteomics  mass spectrometry  liver  blood  biomarker  acetaminophen
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