AI Article Synopsis

  • Drug induced liver injury (DILI) is a critical issue in new drug development, and gadoxetate's hepatic uptake rate shows promise as a biomarker for assessing DILI risk.
  • A comparative study evaluated various pharmacokinetic models to determine the simplest and most effective one for understanding liver function in both humans and rats, informing potential drug dosage selections.
  • The findings offer clear guidelines for selecting mathematical models to assess liver function biomarkers and propose a framework for translating research insights between species.

Article Abstract

Background: Drug induced liver injury (DILI) is a major concern when developing new drugs. A promising biomarker for DILI is the hepatic uptake rate of the contrast agent gadoxetate. This rate can be estimated using a novel approach combining magnetic resonance imaging and mathematical modeling. However, previous work has used different mathematical models to describe liver function in humans or rats, and no comparative study has assessed which model is most optimal to use, or focused on possible translatability between the two species.

Aims: Our aim was therefore to do a comparison and assessment of models for DILI biomarker assessment, and to develop a conceptual basis for a translational framework between the species.

Methods And Results: We first established which of the available pharmacokinetic models to use by identifying the most simple and identifiable model that can describe data from both human and rats. We then developed an extension of this model for how to estimate the effects of a hepatotoxic drug in rats. Finally, we illustrated how such a framework could be useful for drug dosage selection, and how it potentially can be applied in personalized treatments designed to avoid DILI.

Conclusion: Our analysis provides clear guidelines of which mathematical model to use for model-based assessment of biomarkers for liver function, and it also suggests a hypothetical path to a translational framework for DILI.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9821424PMC
http://journals.plos.org/plosone/article?id=10.1371/journal.pone.0279168PLOS

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