Literature DB >> 24685772

How useful are clinical liver function tests in in vitro human hepatotoxicity assays?

Jürgen Borlak1, Anil Chougule2, Prafull Kumar Singh3.   

Abstract

In preclinical hepatotoxicity testing cell based assays are frequently employed. However, prediction of clinical drug induced liver injury (DILI) remains a major challenge. Here we examined the usefulness of frequently employed markers of hepatocellular injury in cultures of primary human hepatocytes (PHH) in response to treatment with either paracetamol, rifampicin, petadolex and/or amiodarone. The changes in the metabolic competency (urea and albumin) and cellular injury (AST, ALT, ALP, LDH, γGT and succinate dehydrogenase) were determined at therapeutic and above drug concentrations as to evaluate the utility of these markers in in vitro systems. Initially, treatment of PHH with any of the drugs caused a statistically significant reduction in enzyme activities to suggest a switch from basic amino acid metabolism towards induced detoxification. However, treatment for prolonged periods of time caused cytolysis, as evidenced by the significant rise in extracellular LDH and the concomitant increase in ALT and AST activity. Notably, amongst the various endpoints studied, urea was best to demonstrate dose dependent metabolic stress, while other markers of hepatocellular injury were highly variable. Taken collectively, urea measurement proofed to be robust in predicting hepatocellular stress; therefore it should be included in preclinical testing strategies for an improved prediction of DILI.
Copyright © 2014 Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  Aminotransferases; Ammonia detoxification; Drug induced liver injury; Hepatotoxicity testing; Human hepatocyte cultures; Urea

Mesh:

Substances:

Year:  2014        PMID: 24685772     DOI: 10.1016/j.tiv.2014.03.006

Source DB:  PubMed          Journal:  Toxicol In Vitro        ISSN: 0887-2333            Impact factor:   3.500


  10 in total

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2.  A microfluidic 3D hepatocyte chip for hepatotoxicity testing of nanoparticles.

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3.  Dose-, treatment- and time-dependent toxicity of superparamagnetic iron oxide nanoparticles on primary rat hepatocytes.

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Authors:  Ylva Terelius; Robert A Figler; Svetlana Marukian; Maria S Collado; Mark J Lawson; Aaron J Mackey; David Manka; Charles W Qualls; Brett R Blackman; Brian R Wamhoff; Ajit Dash
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Review 5.  The Importance of Standardization on Analyzing Circulating RNA.

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6.  Genomics of lipid-laden human hepatocyte cultures enables drug target screening for the treatment of non-alcoholic fatty liver disease.

Authors:  Stephanie Breher-Esch; Nishika Sahini; Anna Trincone; Christin Wallstab; Jürgen Borlak
Journal:  BMC Med Genomics       Date:  2018-12-14       Impact factor: 3.063

7.  Influence of Genistein on Hepatic Lipid Metabolism in an In Vitro Model of Hepatic Steatosis.

Authors:  Lena Seidemann; Anne Krüger; Victoria Kegel-Hübner; Daniel Seehofer; Georg Damm
Journal:  Molecules       Date:  2021-02-22       Impact factor: 4.411

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Authors:  Eun-Hee Lee; Jung-Hwa Oh; Saravanakumar Selvaraj; Se-Myo Park; Mi-Sun Choi; Reinhard Spanel; Seokjoo Yoon; Jürgen Borlak
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10.  Amelioration of the Protein Expression of Cox2, NFκB, and STAT-3 by Some Antioxidants in the Liver of Sodium Fluoride-Intoxicated Rats.

Authors:  Ahlam Alhusaini; Laila Faddaa; Hanaa M Ali; Iman Hassan; Nagla F El Orabi; Yieldiz Bassiouni
Journal:  Dose Response       Date:  2018-09-19       Impact factor: 2.658

  10 in total

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