Investigation of acetaminophen toxicity in HepG2/C3a microscale cultures using a system biology model of glutathione depletion

Leclerc, Éric; Hamon, Jérémy; Claude, I.; Jellali, Rachid; Naudot, Marie; Bois, Frédéric

doi:10.1007/s10565-015-9302-0

Cited by 21 publications

(18 citation statements)

References 40 publications

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“…Although many models have been developed for toxicity pathways, currently there are only a few models specifically designed for liver cells. As discussed, Leclerc et al adapted a general oxidative stress model to describe liver cell dynamics [22]. The question arises whether all dynamical models designed for a particular organ or cell line can be applied to a different organ, in our case the liver.…”

Section: Discussionmentioning

confidence: 99%

“…This indeed is consistent with the hypothesis that adjusting the parameter values is often sufficient to reuse a model for a different tissue or cell line. The oxidative stress model by Leclerc et al [22] focuses on the effect of a single drug and its mechanism of action. To be able to evaluate if drugs are potentially harmful to the liver, we need a model that is sufficiently general to be employed for many different drugs.…”

Section: Discussionmentioning

confidence: 99%

“…The oxidative stress and the heat-shock response (HSR) pathways have already been applied to the liver [22,23], but to our knowledge, this is not yet the case for other stress pathways. As we will discuss below in more detail, general models or models for different cell types or organs can be repurposed for liver cells.…”

Section: Stress and Death Pathwaysmentioning

confidence: 99%

“…Later, the same group [22] adapted this PK-SB model for liver cells, by recalibrating the model using transcriptomic data, including ROS data at different time points and literature-based GSH data. They used the compound Acetyl-paraaminophenol (APAP) to induce cytotoxicity in a liver-on-a-chip and compared the results with the PK-SB model.…”

Section: Modelingmentioning

confidence: 99%

“…Finally, PK and PK-PD modeling are employed to translate this threshold to a corresponding tolerable drug intake in humans. This process was illustrated by Leclerc et al [22] who integrated their dynamical model of the oxidative stress pathway with a PK model predicting how much of the drug actually reaches the cell. Experimental measurements were performed with an organ-on-a-chip setup, and the PK model described the amount of the drug flowing into the extracellular compartments, taking into account adsorption and desorption rates.…”

Section: Expert Opinionmentioning

confidence: 99%

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Unraveling cellular pathways contributing to drug-induced liver injury by dynamical modeling

Kuijper

Yang

Water

et al. 2016

Expert Opinion on Drug Metabolism & Toxicology

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Introduction: Drug-induced liver injury (DILI) is a significant threat to human health and a major problem in drug development. It is hard to predict due to its idiosyncratic nature and which does not show up in animal trials. Hepatic adaptive stress response pathway activation is generally observed in drug-induced liver injury. Dynamical pathway modeling has the potential to foresee adverse effects of drugs before they go in trial. Ordinary differential equation modeling can offer mechanistic insight, and allows us to study the dynamical behavior of stress pathways involved in DILI. Areas covered: This review provides an overview on the progress of the dynamical modeling of stress and death pathways pertinent to DILI, i.e. pathways relevant for oxidative stress, inflammatory stress, DNA damage, unfolded proteins, heat shock and apoptosis. We also discuss the required steps for applying such modeling to the liver. Expert opinion: Despite the strong progress made since the turn of the century, models of stress pathways have only rarely been specifically applied to describe pathway dynamics for DILI. We argue that with minor changes, in some cases only to parameter values, many of these models can be repurposed for application in DILI research. Combining both dynamical models with in vitro testing might offer novel screening methods for the harmful side-effects of drugs. ARTICLE HISTORY

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Stress and Death Pathwaysmentioning

confidence: 99%

Section: Modelingmentioning

confidence: 99%

Section: Expert Opinionmentioning

confidence: 99%

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Unraveling cellular pathways contributing to drug-induced liver injury by dynamical modeling

Kuijper

Yang

Water

et al. 2016

Expert Opinion on Drug Metabolism & Toxicology

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Metabolomics‐on‐a‐chip approach to study hepatotoxicity of DDT, permethrin and their mixtures

Jellali

Gilard

Pandolfi

et al. 2018

J of Applied Toxicology

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Despite the diversity of studies on pesticide toxicities, there is a serious lack of information concerning the toxic effect of pesticides mixtures. Dichlorodiphenyl-trichloroethane (DDT) and permethrin (PMT) are among the most prevalent pesticides in the environment and have been the subject of several toxicological studies. However, there are no data on the toxicity of their mixtures. In this study, we used an approach combining cell culture in microfluidic biochips with gas chromatography-mass spectrometry metabolomics profiling to investigate the biomarkers of toxicity of DDT, PMT and their mixtures. All parameters observed indicated that no significant effect was observed in hepatocytes cultures exposed to low doses (15 μm) of DDT and PMT. Conversely, combined low doses induce moderate oxidative stress and cell death. The toxic signature of high doses of pesticides (150 μm) was illustrated by severe oxidative stress and cell mortality. Metabolomics profiling revealed that hepatocytes exposure to DDT150, PMT150 and DDT150 and PMT150 cause important modulation in intermediates of glutathione pathway and tricarboxylic acid cycle, amino acids and metabolites associated to hepatic necrosis and inflammation (α-ketoglutarate, arginine and 2-hydroxybutyrate). These changes were more striking in the combined group. Finally, DDT150 led to a significant increase of benzoate, decanoate, octanoate, palmitate, stearate and tetradecanoate, which illustrates the estrogen modulation. This study demonstrates the potential of metabolomics-on-a-chip approach to improve knowledge on the mode of action of pesticides.

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Roles of Mitochondrial DNA in Energy Metabolism

Bhatia

Wang

2017

Mitochondrial DNA and Diseases

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Mitochondria are independent double-membrane organelles responsible for energy production, specifically by completing oxidative phosphorylation. Mitochondria are essential to regulate energy metabolism, signaling pathways, and cell death. Mitochondrial DNA (mtDNA) can be altered by metabolic disorders, oxidative stress, or inflammation in the progression and development of various diseases. In this chapter, we overview the role of mtDNA in energy metabolism and the diseases that are associated with mtDNA abnormality, with a special focus on the major factors which regulate the mechanism of mtDNA in metabolism.

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Investigation of acetaminophen toxicity in HepG2/C3a microscale cultures using a system biology model of glutathione depletion

Cited by 21 publications

References 40 publications

Unraveling cellular pathways contributing to drug-induced liver injury by dynamical modeling

Unraveling cellular pathways contributing to drug-induced liver injury by dynamical modeling

Metabolomics‐on‐a‐chip approach to study hepatotoxicity of DDT, permethrin and their mixtures

Roles of Mitochondrial DNA in Energy Metabolism

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