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Representative Sinusoids for Hepatic Four-Scale Pharmacokinetics Simulations

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Listed:
  • Lars Ole Schwen
  • Arne Schenk
  • Clemens Kreutz
  • Jens Timmer
  • María Matilde Bartolomé Rodríguez
  • Lars Kuepfer
  • Tobias Preusser

Abstract

The mammalian liver plays a key role for metabolism and detoxification of xenobiotics in the body. The corresponding biochemical processes are typically subject to spatial variations at different length scales. Zonal enzyme expression along sinusoids leads to zonated metabolization already in the healthy state. Pathological states of the liver may involve liver cells affected in a zonated manner or heterogeneously across the whole organ. This spatial heterogeneity, however, cannot be described by most computational models which usually consider the liver as a homogeneous, well-stirred organ.The goal of this article is to present a methodology to extend whole-body pharmacokinetics models by a detailed liver model, combining different modeling approaches from the literature. This approach results in an integrated four-scale model, from single cells via sinusoids and the organ to the whole organism, capable of mechanistically representing metabolization inhomogeneity in livers at different spatial scales. Moreover, the model shows circulatory mixing effects due to a delayed recirculation through the surrounding organism.To show that this approach is generally applicable for different physiological processes, we show three applications as proofs of concept, covering a range of species, compounds, and diseased states: clearance of midazolam in steatotic human livers, clearance of caffeine in mouse livers regenerating from necrosis, and a parameter study on the impact of different cell entities on insulin uptake in mouse livers.The examples illustrate how variations only discernible at the local scale influence substance distribution in the plasma at the whole-body level. In particular, our results show that simultaneously considering variations at all relevant spatial scales may be necessary to understand their impact on observations at the organism scale.

Suggested Citation

  • 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.
  • Handle: RePEc:plo:pone00:0133653
    DOI: 10.1371/journal.pone.0133653
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    References listed on IDEAS

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    1. Yae Jin Yoon & Soeun Chang & Oh Youn Kim & Bo-Kyeong Kang & Jaesung Park & Jae-Hong Lim & Jung Yun Huang & Yoon-Keun Kim & Jae Ho Byun & Yong Song Gho, 2013. "Three-Dimensional Imaging of Hepatic Sinusoids in Mice Using Synchrotron Radiation Micro-Computed Tomography," PLOS ONE, Public Library of Science, vol. 8(7), pages 1-1, July.
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    Cited by:

    1. 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.
    2. Quentin Cangelosi & Shawn A Means & Harvey Ho, 2017. "A multi-scale spatial model of hepatitis-B viral dynamics," PLOS ONE, Public Library of Science, vol. 12(12), pages 1-28, December.
    3. 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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