Utility of spherical human liver microtissues for prediction of clinical drug-induced liver injury

Proctor, William R.; Foster, Alison J.; Vogt, Jennifer; Summers, Claire; Middleton, Brian; Pilling, Mark; Shienson, Daniel; Kijańska, Monika; Ströbel, Simon; Kelm, Jens M.; Morgan, Paul; Messner, Simon; Williams, Dominic P.

doi:10.1007/s00204-017-2002-1

Cited by 227 publications

(250 citation statements)

References 52 publications

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“…Richert et al postulated that exposure periods longer than 72 hours in human hepatocytes do not increase the DILI‐prediction rate compared with shorter exposure times. Contrary to this Proctor et al recently reported higher predictivity of liver toxicants by 3D hLiMT (14‐day treatment) vs plated D2 primary human hepatocytes (48h‐treatment). In contrast to our cytotoxicity results, Otieno et al described that TAK875 1 is not cytotoxic in hepatocytes and HepG2 cells (data were not shown) following incubation of 100 µM for 72 hours.…”

Section: Resultsmentioning

confidence: 72%

Mechanistic investigations of the liver toxicity of the free fatty acid receptor 1 agonist fasiglifam (TAK875) and its primary metabolites

Ackerson

Amberg

Atzrodt

et al. 2019

J Biochem & Molecular Tox

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For fasiglifam (TAK875) and its metabolites the substance‐specific mechanisms of liver toxicity were studied. Metabolism studies were run to identify a putatively reactive acyl glucuronide metabolite. In vitro cytotoxicity and caspase 3/7 activation were assessed in primary human and dog hepatocytes in 2D and 3D cell culture. Involvement of glutathione (GSH) detoxication system in mediating cytotoxicity was determined by assessing potentiation of cytotoxicity in a GSH depleted in vitro system. In addition, potential mitochondrial liabilities of the compounds were assessed in a whole‐cell mitochondrial functional assay. Fasiglifam showed moderate cytotoxicity in human primary hepatocytes in the classical 2D cytotoxicity assays and also in the complex 3D human liver microtissue (hLiMT) after short‐term treatment (24 hours or 48 hours) with TC50 values of 56 to 68 µM (adenosine triphosphate endpoint). The long‐term treatment for 14 days in the hLiMT resulted in a slight TC50 shift over time of 2.7/3.6 fold lower vs 24‐hour treatment indicating possibly a higher risk for cytotoxicity during long‐term treatment. Cellular GSH depletion and impairment of mitochondrial function by TAK875 and its metabolites evaluated by Seahorse assay could not be found being involved in DILI reported for TAK875. The acyl glucuronide metabolites of TAK875 have been finally identified to be the dominant reason for liver toxicity.

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Section: Resultsmentioning

confidence: 72%

Mechanistic investigations of the liver toxicity of the free fatty acid receptor 1 agonist fasiglifam (TAK875) and its primary metabolites

Ackerson

Amberg

Atzrodt

et al. 2019

J Biochem & Molecular Tox

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“…Two systematic benchmarking studies for hepatotoxicity tests have been published in PHH spheroids to date. Proctor et al used a commercial proprietary model to test the toxicity of 110 drugs (69 DILI‐positive and 41 DILI‐negative) during 14 days of repeated exposures using the InSphero model and reported overall sensitivity and specificity of 59% and 80%, respectively. In contrast, we used chemically defined media and ULA 3D PHH spheroids to expose a panel of 123 drugs (70 DILI‐positive and 53 DILI‐negative), correctly predicting the hepatotoxicity of 48 out of 70 compounds (sensitivity = 69%) without a single false‐positive result (specificity = 100%; Figure A) .…”

Section: Applications Of Advanced Primary Human Hepatocyte Culture Momentioning

confidence: 99%

3D Primary Hepatocyte Culture Systems for Analyses of Liver Diseases, Drug Metabolism, and Toxicity: Emerging Culture Paradigms and Applications

Lauschke

Shafagh

Hendriks

et al. 2019

Biotechnology Journal

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Recent research has shown that the maintenance of relevant liver functions ex vivo requires models in which the cells exhibit an in vivo‐like phenotype, often achieved by reconstitution of appropriate cellular interactions. Multiple different models have been presented that differ in the cells utilized, media, and culture conditions. Furthermore, several technologically different approaches have been presented including bioreactors, chips, and plate‐based systems in fluidic or static media constituting of chemically diverse materials. Using such models, the ability to predict drug metabolism, drug toxicity, and liver functionality have increased tremendously as compared to conventional in vitro models in which cells are cultured as 2D monolayers. Here, the authors highlight important considerations for microphysiological systems for primary hepatocyte culture, review current culture paradigms, and discuss their opportunities for studies of drug metabolism, hepatotoxicity, liver biology, and disease.

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“…Therefore, the risk of human DILI has been massively underestimated by the in vitro system. Similar problems exist for the category 1 compounds dantrolene, methotrexate, stavudine and trovafloxacin (Proctor et al 2017;Table S-3, S3h LiMT data). It is interesting to note that cytotoxicity allows a good prediction of human blood concentrations associated with an increased risk of DILI for some compounds, while it leads to a massive underestimation of other severe DILI compounds.…”

mentioning

confidence: 58%

“…However, a comprehensive study including a sufficiently large number of compounds for validation of these endpoints is not yet available. The merit of the present study (Proctor et al 2017) is that it delivers a comprehensive cytotoxicity database, which clearly demonstrates that cytotoxicity alone is not sufficient to predict human DILI. In conclusion, the hunt for an accurate in vitro system quantitatively predicting human hepatotoxicity has only just begun.…”

mentioning

confidence: 95%

Highlight report: prediction of drug induced liver injury (DILI) with human hepatocytes in vitro

Albrecht

2017

Arch Toxicol

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Utility of spherical human liver microtissues for prediction of clinical drug-induced liver injury

Cited by 227 publications

References 52 publications

Mechanistic investigations of the liver toxicity of the free fatty acid receptor 1 agonist fasiglifam (TAK875) and its primary metabolites

Mechanistic investigations of the liver toxicity of the free fatty acid receptor 1 agonist fasiglifam (TAK875) and its primary metabolites

3D Primary Hepatocyte Culture Systems for Analyses of Liver Diseases, Drug Metabolism, and Toxicity: Emerging Culture Paradigms and Applications

Highlight report: prediction of drug induced liver injury (DILI) with human hepatocytes in vitro

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