• Title of article

    Development of a physiologically-based toxicokinetic model of acrylamide and glycidamide in rats and humans

  • Author/Authors

    Sweeney، نويسنده , , Lisa M. and Kirman، نويسنده , , Christopher R. and Gargas، نويسنده , , Michael L. and Carson، نويسنده , , M. Leigh and Tardiff، نويسنده , , Robert G.، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2010
  • Pages
    18
  • From page
    668
  • To page
    685
  • Abstract
    Physiologically-based toxicokinetic (“pharmacokinetic”) (PBPK or PBTK) modeling can be used as a tool to compare internal doses of acrylamide (AA) and its metabolite glycidamide (GA) in humans and rats. An earlier PBTK model for AA and GA in rats was refined and extended to humans based on new data. With adjustments to the previous parameters, excellent fits to a majority of the data for male Fisher 344 rats were obtained. Kinetic parameters for the human model were estimated based on fit to available human data for urinary metabolites of AA, and levels of hemoglobin adducts of AA and GA measured in studies in which human volunteers ingested known doses of AA. The simulations conducted with the rat and human models predicted that rats and humans ingesting comparable levels of AA (in mg/kg day) would have similar levels of GA in blood and tissues. This finding stands in contrast to the default approach that assumes a 3.2-fold increase in human risk due to pharmacokinetic differences between rats and humans. This model was used in a companion paper to estimate safe levels of ingested AA.
  • Keywords
    Acrylamide , Glycidamide , Human PBPK model , Food safety , Neurotoxicity , CANCER
  • Journal title
    Food and Chemical Toxicology
  • Serial Year
    2010
  • Journal title
    Food and Chemical Toxicology
  • Record number

    2121659