Mechanistic Modeling of In Vitro Skin Permeation and Extrapolation to In Vivo for Topically Applied Metronidazole Drug Products Using a Physiologically Based Pharmacokinetic Model

Sumit Arora; James Clarke; Eleftheria Tsakalozou; Priyanka Ghosh; Khondoker Alam; Jeffery E Grice; Michael S Roberts; Masoud Jamei; Sebastian Polak

doi:10.1021/acs.molpharmaceut.2c00229

Mechanistic Modeling of In Vitro Skin Permeation and Extrapolation to In Vivo for Topically Applied Metronidazole Drug Products Using a Physiologically Based Pharmacokinetic Model

Mol Pharm. 2022 Sep 5;19(9):3139-3152. doi: 10.1021/acs.molpharmaceut.2c00229. Epub 2022 Aug 15.

Authors

Affiliations

¹ Certara UK Ltd, Simcyp Division, Sheffield S1 2BJ, U.K.
² Office of Research and Standards, Office of Generic Drugs, Center for Drug Evaluation and Research, U.S. Food and Drug Administration (FDA), Silver Spring, Maryland 20993, United States.
³ Therapeutics Research Centre, Diamantina Institute, University of Queensland, Brisbane 4102, Australia.
⁴ Clinical and Health Sciences, University of South Australia, Adelaide 5005, Australia.
⁵ Faculty of Pharmacy, Jagiellonian University Medical College, Medyczna 9, Kraków 30-688, Poland.

PMID: 35969125
DOI: 10.1021/acs.molpharmaceut.2c00229

Abstract

Physiologically based pharmacokinetic (PBPK) modeling has increasingly been employed in dermal drug development and regulatory assessment, providing a framework to integrate relevant information including drug and drug product attributes, skin physiology parameters, and population variability. The current study aimed to develop a stepwise modeling workflow with knowledge gained from modeling in vitro skin permeation testing (IVPT) to describe in vivo exposure of metronidazole locally in the stratum corneum following topical application of complex semisolid drug products. The initial PBPK model of metronidazole in vitro skin permeation was developed using infinite and finite dose aqueous metronidazole solution. Parameters such as stratum corneum lipid-water partition coefficient (K_sclip/water) and stratum corneum lipid diffusion coefficient (D_sclip) of metronidazole were optimized using IVPT data from simple aqueous solutions (infinite) and MetroGel (10 mg/cm² dose application), respectively. The optimized model, when parameterized with physical and structural characteristics of the drug products, was able to accurately predict the mean cumulative amount permeated (cm²/h) and flux (μg/cm²/h) profiles of metronidazole following application of different doses of MetroGel and MetroCream. Thus, the model was able to capture the impact of differences in drug product microstructure and metamorphosis of the dosage form on in vitro metronidazole permeation. The PBPK model informed by IVPT study data was able to predict the metronidazole amount in the stratum corneum as reported in clinical studies. In summary, the proposed model provides an enhanced understanding of the potential impact of drug product attributes in influencing in vitro skin permeation of metronidazole. Key kinetic parameters derived from modeling the metronidazole IVPT data improved the predictions of the developed PBPK model of in vivo local metronidazole concentrations in the stratum corneum. Overall, this work improves our confidence in the proposed workflow that accounts for drug product attributes and utilizes IVPT data toward improving predictions from advanced modeling and simulation tools.

Keywords: IVPT; PBPK model; complex semisolid formulations; dermal absorption; in vitro in vivo extrapolation; mechanistic modeling.

Publication types

Research Support, U.S. Gov't, P.H.S.
Research Support, Non-U.S. Gov't

MeSH terms

Administration, Cutaneous
Lipids
Metronidazole*
Skin*
Water

Substances

Lipids
Water
Metronidazole

Grants and funding

U01 FD006522/FD/FDA HHS/United States