Literature DB >> 12781628

Characterisation of some cytotoxic endpoints using rat liver and HepG2 spheroids as in vitro models and their application in hepatotoxicity studies. I. Glucose metabolism and enzyme release as cytotoxic markers.

Jinsheng Xu1, Mingwen Ma, Wendy M Purcell.   

Abstract

Cytotoxicity endpoints, spontaneous glucose secretion/consumption and LDH and gamma-GT release, were characterised in rat liver and HepG2 spheroids as in vitro models for toxicology studies. Preprepared rat liver spheroids and HepG2 spheroids cultured in a six-well plate format were exposed to varying concentrations of galactosamine, propranolol, diclofenac, and paracetamol. All four model toxins significantly affected glucose secretion, which agreed well with LDH and/or gamma-GT release in rat liver spheroids. These toxins also significantly increased LDH and/or gamma-GT release in HepG2 spheroids. Whereas glucose consumption in HepG2 spheroids did not show conclusive results, LDH activities in both types of spheroids were similar and their levels were relatively high. Accordingly, the level of LDH leakage in both types of spheroids was much higher than gamma-GT after exposure to the toxins. In contrast, gamma-GT activity in HepG2 spheroids was sixfold higher than that in rat liver spheroids. This study revealed that galactosamine interfered with the gamma-GT assay and paracetamol interfered with the LDH assay. It demonstrated, for the first time, that glucose secretion by liver spheroids can be used as a functional indicator of cytotoxicity. Test compounds may interfere with enzymatic assays as indicated by LDH and gamma-GT release in this study. Combining functional parameters together with two or more indicators of enzyme releases can provide a reliable cytotoxicity evaluation. Liver and HepG2 spheroids as in vitro models showed good predictions in chemical-induced hepatic cytotoxicity.

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Year:  2003        PMID: 12781628     DOI: 10.1016/s0041-008x(03)00089-9

Source DB:  PubMed          Journal:  Toxicol Appl Pharmacol        ISSN: 0041-008X            Impact factor:   4.219


  11 in total

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Authors:  Xiaolei Ma; Fuchuan Zhou; Yuanyuan Chen; Yuanyuan Zhang; Lihua Hou; Xiaohong Cao; Chunling Wang
Journal:  Glycoconj J       Date:  2014-06-08       Impact factor: 2.916

4.  shRNA silencing of AS3MT expression minimizes arsenic methylation capacity of HepG2 cells.

Authors:  Zuzana Drobna; Weibing Xing; David J Thomas; Miroslav Stýblo
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5.  Modulation of hepatocarcinoma cell morphology and activity by parylene-C coating on PDMS.

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6.  Two-dimensional microarray of HepG2 spheroids using collagen/polyethylene glycol micropatterned chip.

Authors:  T Tamura; Y Sakai; K Nakazawa
Journal:  J Mater Sci Mater Med       Date:  2007-10-30       Impact factor: 3.896

7.  Determination of drug toxicity using 3D spheroids constructed from an immortal human hepatocyte cell line.

Authors:  Stephen J Fey; Krzysztof Wrzesinski
Journal:  Toxicol Sci       Date:  2012-03-27       Impact factor: 4.849

8.  Hepatoprotective and antioxidant activity of standardized herbal extracts.

Authors:  Bhaskarmurthy Deepak Hiraganahalli; Velusami Chandrasekaran Chinampudur; Shekhar Dethe; Deepak Mundkinajeddu; Manoj Kumar Pandre; Jaya Balachandran; Amit Agarwal
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9.  Lactobacillus fermentum Postbiotic-induced Autophagy as Potential Approach for Treatment of Acetaminophen Hepatotoxicity.

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Journal:  Front Microbiol       Date:  2017-04-06       Impact factor: 5.640

10.  Spheroid Size Does not Impact Metabolism of the β-blocker Propranolol in 3D Intestinal Fish Model.

Authors:  Laura M Langan; Stewart F Owen; Maciej Trznadel; Nicholas J F Dodd; Simon K Jackson; Wendy M Purcell; Awadhesh N Jha
Journal:  Front Pharmacol       Date:  2018-08-22       Impact factor: 5.810

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