Raman-assessed cutaneous pharmacokinetics of doxepin topical products

Nota Zarmpi; Dimitrios Tsikritsis; Natalie A. Belsey; Elena Rantou; Priyanka Ghosh; Annette L. Bunge; Andrew Watson; Tim Woodman; Begona Delgado-Charro; Richard Guy

doi:10.1016/j.ijpharm.2026.126680

Raman-assessed cutaneous pharmacokinetics of doxepin topical products

Nota Zarmpi, Dimitrios Tsikritsis, Natalie A. Belsey, Elena Rantou, Priyanka Ghosh, Annette L. Bunge, Andrew Watson, Tim Woodman, Begona Delgado-Charro, Richard Guy

Research output: Contribution to journal › Article › peer-review

Abstract

Development of regulatory science tools to facilitate and accelerate accessibility to complex generic drug products continues to be the focus of significant research activity. The application of confocal Raman spectroscopy to the assessment of cutaneous drug pharmacokinetics is a particular example and has been exploited here to compare two approved topical creams (the reference-listed drug product and a generic) of doxepin hydrochloride with an intentionally non-equivalent, laboratory-made solution of the drug. Experiments involved administration of the formulations to pig skin ex vivo for 6 or 12 h (the uptake phase) followed by 2 and 4 h of clearance to generate Raman-assessed absorption-elimination profiles at nominal depths of 5 μm and 25 μm into the skin. This was achieved, despite overlap between spectral features of the drug with those from the skin, using a background signal removal strategy that also allowed the two functional excipients of the laboratory-made solution to be independently tracked. The areas under the Raman signal versus time absorption-elimination profiles showed (as expected) that the two creams were very similar but that the laboratory-made solution was distinctly different. First-order elimination rate constants describing the clearance phase post-application of doxepin from the superficial skin layers into the deeper tissue were also derived from the spectral data. While the experimental design was insufficiently powered to assess bioequivalence, the data background signal separation paradigm notably expands the potential value of the approach to a broader range of chemical species than had been originally envisaged

Original language	English
Article number	126680
Journal	International Journal of Pharmaceutics
Volume	693
Early online date	18 Feb 2026
DOIs	https://doi.org/10.1016/j.ijpharm.2026.126680
Publication status	E-pub ahead of print - 18 Feb 2026

Data Availability Statement

Data will be made available on request.

Acknowledgements

We dedicate this paper to Professor Joke Bouwstra in recognition of her incredibly rich and interdisciplinary research career and, specifically, her massive contributions to the fields of skin barrier function and topical/transdermal drug delivery.

Funding

We dedicate this paper to Professor Joke Bouwstra in recognition of her incredibly rich and interdisciplinary research career and, specifically, her massive contributions to the fields of skin barrier function and topical/transdermal drug delivery. This project is supported by the Food and Drug Administration (FDA) of the U.S. Department of Health and Human Services (HHS) as part of a financial assistance award (1-U01-FD 006533) totalling $1.25M with 100% funded by FDA/HHS. The contents are those of the author(s) and do not necessarily represent the official views of, nor an endorsement, by FDA/HHS, or the U.S. Government. Valuable insight from and stimulating discussions with Drs. Sam Raney and Markham Luke from the FDA's Office of Generic Drugs, and from Professor Jane White at the University of Bath, are gratefully acknowledged. NAB thanks the Community for Analytical Measurement Science for a 2020 CAMS Fellowship Award funded by the Analytical Chemistry Trust Fund.We dedicate this paper to Professor Joke Bouwstra in recognition of her incredibly rich and interdisciplinary research career and, specifically, her massive contributions to the fields of skin barrier function and topical/transdermal drug delivery. This project is supported by the Food and Drug Administration (FDA) of the U.S. Department of Health and Human Services (HHS) as part of a financial assistance award (1-U01-FD 006533) totalling id="ak005".25M with 100% funded by FDA/HHS. The contents are those of the author(s) and do not necessarily represent the official views of, nor an endorsement, by FDA/HHS, or the U.S. Government. Valuable insight from and stimulating discussions with Drs. Sam Raney and Markham Luke from the FDA's Office of Generic Drugs, and from Professor Jane White at the University of Bath, are gratefully acknowledged. NAB thanks the Community for Analytical Measurement Science for a 2020 CAMS Fellowship Award funded by the Analytical Chemistry Trust Fund.

Funders	Funder number
Analytical Chemistry Trust Fund
Office of Generic Drugs
Community for Analytical Measurement Science
U.S. Food and Drug Administration
U.S. Department of Health and Human Services
HHS	1-U01-FD 006533

Keywords

Cutaneous pharmacokinetics
Raman spectroscopy
Regulatory science
Topical drug bioavailability
Topical drug product bioequivalence

ASJC Scopus subject areas

Pharmaceutical Science

Access to Document

10.1016/j.ijpharm.2026.126680Licence: CC BY

Cite this

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title = "Raman-assessed cutaneous pharmacokinetics of doxepin topical products",

abstract = "Development of regulatory science tools to facilitate and accelerate accessibility to complex generic drug products continues to be the focus of significant research activity. The application of confocal Raman spectroscopy to the assessment of cutaneous drug pharmacokinetics is a particular example and has been exploited here to compare two approved topical creams (the reference-listed drug product and a generic) of doxepin hydrochloride with an intentionally non-equivalent, laboratory-made solution of the drug. Experiments involved administration of the formulations to pig skin ex vivo for 6 or 12 h (the uptake phase) followed by 2 and 4 h of clearance to generate Raman-assessed absorption-elimination profiles at nominal depths of 5 μm and 25 μm into the skin. This was achieved, despite overlap between spectral features of the drug with those from the skin, using a background signal removal strategy that also allowed the two functional excipients of the laboratory-made solution to be independently tracked. The areas under the Raman signal versus time absorption-elimination profiles showed (as expected) that the two creams were very similar but that the laboratory-made solution was distinctly different. First-order elimination rate constants describing the clearance phase post-application of doxepin from the superficial skin layers into the deeper tissue were also derived from the spectral data. While the experimental design was insufficiently powered to assess bioequivalence, the data background signal separation paradigm notably expands the potential value of the approach to a broader range of chemical species than had been originally envisaged",

keywords = "Cutaneous pharmacokinetics, Raman spectroscopy, Regulatory science, Topical drug bioavailability, Topical drug product bioequivalence",

author = "Nota Zarmpi and Dimitrios Tsikritsis and Belsey, \{Natalie A.\} and Elena Rantou and Priyanka Ghosh and Bunge, \{Annette L.\} and Andrew Watson and Tim Woodman and Begona Delgado-Charro and Richard Guy",

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AU - Zarmpi, Nota

AU - Tsikritsis, Dimitrios

AU - Belsey, Natalie A.

AU - Rantou, Elena

AU - Ghosh, Priyanka

AU - Bunge, Annette L.

AU - Watson, Andrew

AU - Woodman, Tim

AU - Delgado-Charro, Begona

AU - Guy, Richard

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AB - Development of regulatory science tools to facilitate and accelerate accessibility to complex generic drug products continues to be the focus of significant research activity. The application of confocal Raman spectroscopy to the assessment of cutaneous drug pharmacokinetics is a particular example and has been exploited here to compare two approved topical creams (the reference-listed drug product and a generic) of doxepin hydrochloride with an intentionally non-equivalent, laboratory-made solution of the drug. Experiments involved administration of the formulations to pig skin ex vivo for 6 or 12 h (the uptake phase) followed by 2 and 4 h of clearance to generate Raman-assessed absorption-elimination profiles at nominal depths of 5 μm and 25 μm into the skin. This was achieved, despite overlap between spectral features of the drug with those from the skin, using a background signal removal strategy that also allowed the two functional excipients of the laboratory-made solution to be independently tracked. The areas under the Raman signal versus time absorption-elimination profiles showed (as expected) that the two creams were very similar but that the laboratory-made solution was distinctly different. First-order elimination rate constants describing the clearance phase post-application of doxepin from the superficial skin layers into the deeper tissue were also derived from the spectral data. While the experimental design was insufficiently powered to assess bioequivalence, the data background signal separation paradigm notably expands the potential value of the approach to a broader range of chemical species than had been originally envisaged

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Raman-assessed cutaneous pharmacokinetics of doxepin topical products

Abstract

Data Availability Statement

Acknowledgements

Funding

Keywords

ASJC Scopus subject areas

Access to Document

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