Physiologically Based Pharmacokinetic Modeling in Risk Assessment: Case Study With Pyrethroids

Author:

Mallick Pankajini1,Song Gina1,Efremenko Alina Y1,Pendse Salil N1,Creek Moire R2,Osimitz Thomas G3,Hines Ronald N4ORCID,Hinderliter Paul5,Clewell Harvey J6,Lake Brian G7,Yoon Miyoung1,Moreau Marjory1

Affiliation:

1. ScitoVation, LLC, Durham, North Carolina 27713

2. Moire Creek Toxicology Consulting Services, Lincoln, California 95648

3. Science Strategies, LLC, Charlottesville, Virginia 22902

4. US EPA, Office of Research and Development, Center for Public Health and Environmental Assessment, Research Triangle Park, North Carolina 27709

5. Syngenta, Greensboro, North Carolina 27409

6. Ramboll, Research Triangle Park, North Carolina 27709

7. Faculty of Health and Medical Sciences, University of Surrey, Surrey GU2 7XH, UK

Abstract

Abstract The assessment of potentially sensitive populations is an important application of risk assessment. To address the concern for age-related sensitivity to pyrethroid insecticides, life-stage physiologically based pharmacokinetic (PBPK) modeling supported by in vitro to in vivo extrapolation was conducted to predict age-dependent changes in target tissue exposure to 8 pyrethroids. The purpose of this age-dependent dosimetry was to calculate a Data-derived Extrapolation Factor (DDEF) to address age-related pharmacokinetic differences for pyrethroids in humans. We developed a generic human PBPK model for pyrethroids based on our previously published rat model that was developed with in vivo rat data. The results demonstrated that the age-related differences in internal exposure to pyrethroids in the brain are largely determined by the differences in metabolic capacity and in physiology for pyrethroids between children and adults. The most important conclusion from our research is that, given an identical external exposure, the internal (target tissue) concentration is equal or lower in children than in adults in response to the same level of exposure to a pyrethroid. Our results show that, based on the use of the life-stage PBPK models with 8 pyrethroids, DDEF values are essentially close to 1, resulting in a DDEF for age-related pharmacokinetic differences of 1. For risk assessment purposes, this indicates that no additional adjustment factor is necessary to account for age-related pharmacokinetic differences for these pyrethroids.

Funder

Council for the Advancement of Pyrethroid Human Risk Assessment

CAPHRA

Publisher

Oxford University Press (OUP)

Subject

Toxicology

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