Pharmaceutics (Jun 2024)

Nanoliposomes Permeability in a Microfluidic Drug Delivery Platform across a 3D Hydrogel

  • Corentin Peyret,
  • Aleka Manousaki,
  • Sabine Bouguet-Bonnet,
  • Emmanuel Stratakis,
  • Laura Sanchez-Gonzalez,
  • Cyril J.F. Kahn,
  • Elmira Arab-Tehrany

DOI
https://doi.org/10.3390/pharmaceutics16060765
Journal volume & issue
Vol. 16, no. 6
p. 765

Abstract

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Nanoliposomes are nano-sized vesicles that can be used as drug delivery carriers with the ability to encapsulate both hydrophobic and hydrophilic compounds. Moreover, their lipid compositions facilitate their internalization by cells. However, the interaction between nanoliposomes and the membrane barrier of the human body is not well-known. If cellular tests and animal testing offer a solution, their lack of physiological relevance and ethical concerns make them unsuitable to properly mimic human body complexity. Microfluidics, which allows the environment of the human body to be imitated in a controlled way, can fulfil this role. However, existing models are missing the presence of something that would mimic a basal membrane, often consisting of a simple cell layer on a polymer membrane. In this study, we investigated the diffusion of nanoliposomes in a microfluidic system and found the optimal parameters to maximize their diffusion. Then, we incorporated a custom made GelMA with a controlled degree of substitution and studied the passage of fluorescently labeled nanoliposomes through this barrier. Our results show that highly substituted GelMA was more porous than lower substitution GelMA. Overall, our work lays the foundation for the incorporation of a hydrogel mimicking a basal membrane on a drug delivery microfluidic platform.

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