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httk: R Package for High-Throughput Toxicokinetics

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  • Pearce, Robert G.
  • Setzer, R. Woodrow
  • Strope, Cory L.
  • Sipes, Nisha S.
  • Wambaugh, John F.

Abstract

Thousands of chemicals have been profiled by high-throughput screening programs such as ToxCast and Tox21; these chemicals are tested in part because most of them have limited or no data on hazard, exposure, or toxicokinetics. Toxicokinetic models aid in predicting tissue concentrations resulting from chemical exposure, and a "reverse dosimetry" approach can be used to predict exposure doses sufficient to cause tissue concentrations that have been identified as bioactive by high-throughput screening. We have created four toxicokinetic models within the R software package httk. These models are designed to be parameterized using high-throughput in vitro data (plasma protein binding and hepatic clearance), as well as structure-derived physicochemical properties and species-specific physiological data. The package contains tools for Monte Carlo sampling and reverse dosimetry along with functions for the analysis of concentration vs. time simulations. The package can currently use human in vitro data to make predictions for 553 chemicals in humans, rats, mice, dogs, and rabbits, including 94 pharmaceuticals and 415 ToxCast chemicals. For 67 of these chemicals, the package includes rat-specific in vitro data. This package is structured to be augmented with additional chemical data as they become available. Package httk enables the inclusion of toxicokinetics in the statistical analysis of chemicals undergoing high-throughput screening.

Suggested Citation

  • Pearce, Robert G. & Setzer, R. Woodrow & Strope, Cory L. & Sipes, Nisha S. & Wambaugh, John F., 2017. "httk: R Package for High-Throughput Toxicokinetics," Journal of Statistical Software, Foundation for Open Access Statistics, vol. 79(i04).
  • Handle: RePEc:jss:jstsof:v:079:i04
    DOI: http://hdl.handle.net/10.18637/jss.v079.i04
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    Cited by:

    1. Jiaqi Ding & Wenxin Liu & Hong Zhang & Lingyan Zhu & Lin Zhu & Jianfeng Feng, 2021. "Liver-Based Probabilistic Risk Assessment of Exposure to Organophosphate Esters via Dust Ingestion Using a Physiologically Based Toxicokinetic (PBTK) Model," IJERPH, MDPI, vol. 18(23), pages 1-18, November.
    2. Deepika Deepika & Vikas Kumar, 2023. "The Role of “Physiologically Based Pharmacokinetic Model (PBPK)” New Approach Methodology (NAM) in Pharmaceuticals and Environmental Chemical Risk Assessment," IJERPH, MDPI, vol. 20(4), pages 1-19, February.

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