Characterisation of skin penetration pathways using stimulated Raman scattering microscopy

[Display omitted] Understanding the mechanisms governing the penetration of substances into the skin is crucial for the development of safe and effective topical drug delivery systems and skincare products. This study examined the partitioning of model permeants into human skin, by assessing six sub...

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Veröffentlicht in:European journal of pharmaceutics and biopharmaceutics 2024-11, Vol.204, p.114518, Article 114518
Hauptverfasser: Goel, Anukrati, Pendlington, Ruth, Glavin, Stephen, Chen, Tao, Belsey, Natalie A.
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Sprache:eng
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Zusammenfassung:[Display omitted] Understanding the mechanisms governing the penetration of substances into the skin is crucial for the development of safe and effective topical drug delivery systems and skincare products. This study examined the partitioning of model permeants into human skin, by assessing six substances with diverse logP values. We employed stimulated Raman scattering (SRS) microscopy, an ambient, label-free optical imaging technique known for its ability to provide chemical distribution with subcellular resolution. Our investigation assessed partitioning into the two primary pathways through which substances traverse the skin: the intercellular lipid matrix and the intracellular route via corneocyte cells. We observed that the partitioning behaviour was strongly influenced by the lipophilicity of the molecule, with lipophilic compounds showing greater affinity for intercellular matrix with increased lipophilicity. Conversely, hydrophilic molecules demonstrated a preference for corneocyte cells, with their affinity increasing with increased hydrophilicity. The findings contribute to our understanding of the mechanisms underlying topical delivery and offer important implications and new methods beneficial for the development of safe and effective topical products. In addition, the methods presented could be valuable to reveal changes in drug partitioning or to assess targeting approaches in diseased skin models.
ISSN:0939-6411
1873-3441
1873-3441
DOI:10.1016/j.ejpb.2024.114518