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A Liver-Centric Multiscale Modeling Framework for Xenobiotics

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Listed:
  • James P Sluka
  • Xiao Fu
  • Maciej Swat
  • Julio M Belmonte
  • Alin Cosmanescu
  • Sherry G Clendenon
  • John F Wambaugh
  • James A Glazier

Abstract

We describe a multi-scale, liver-centric in silico modeling framework for acetaminophen pharmacology and metabolism. We focus on a computational model to characterize whole body uptake and clearance, liver transport and phase I and phase II metabolism. We do this by incorporating sub-models that span three scales; Physiologically Based Pharmacokinetic (PBPK) modeling of acetaminophen uptake and distribution at the whole body level, cell and blood flow modeling at the tissue/organ level and metabolism at the sub-cellular level. We have used standard modeling modalities at each of the three scales. In particular, we have used the Systems Biology Markup Language (SBML) to create both the whole-body and sub-cellular scales. Our modeling approach allows us to run the individual sub-models separately and allows us to easily exchange models at a particular scale without the need to extensively rework the sub-models at other scales. In addition, the use of SBML greatly facilitates the inclusion of biological annotations directly in the model code. The model was calibrated using human in vivo data for acetaminophen and its sulfate and glucuronate metabolites. We then carried out extensive parameter sensitivity studies including the pairwise interaction of parameters. We also simulated population variation of exposure and sensitivity to acetaminophen. Our modeling framework can be extended to the prediction of liver toxicity following acetaminophen overdose, or used as a general purpose pharmacokinetic model for xenobiotics.

Suggested Citation

  • James P Sluka & Xiao Fu & Maciej Swat & Julio M Belmonte & Alin Cosmanescu & Sherry G Clendenon & John F Wambaugh & James A Glazier, 2016. "A Liver-Centric Multiscale Modeling Framework for Xenobiotics," PLOS ONE, Public Library of Science, vol. 11(9), pages 1-40, September.
  • Handle: RePEc:plo:pone00:0162428
    DOI: 10.1371/journal.pone.0162428
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    References listed on IDEAS

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    1. Lars Ole Schwen & Arne Schenk & Clemens Kreutz & Jens Timmer & María Matilde Bartolomé Rodríguez & Lars Kuepfer & Tobias Preusser, 2015. "Representative Sinusoids for Hepatic Four-Scale Pharmacokinetics Simulations," PLOS ONE, Public Library of Science, vol. 10(7), pages 1-39, July.
    2. John Wambaugh & Imran Shah, 2010. "Simulating Microdosimetry in a Virtual Hepatic Lobule," PLOS Computational Biology, Public Library of Science, vol. 6(4), pages 1-16, April.
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    Cited by:

    1. Xiao Fu & James P Sluka & Sherry G Clendenon & Kenneth W Dunn & Zemin Wang & James E Klaunig & James A Glazier, 2018. "Modeling of xenobiotic transport and metabolism in virtual hepatic lobule models," PLOS ONE, Public Library of Science, vol. 13(9), pages 1-34, September.

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