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A study of hydrophobic domain formation of polymeric drug precipitation inhibitors in aqueous solution

  • Egis Zeneli
  • , Justus Johann Lange
  • , René Holm
  • , Martin Kuentz*
  • *Kontaktforfatter
  • University of Applied Sciences and Arts Northwestern Switzerland
  • University of Basel
  • University College Cork

Publikation: Bidrag til tidsskriftTidsskriftartikelForskningpeer review

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Abstract

Despite the widespread use of polymers as precipitation inhibitors in supersaturating drug formulations, the current understanding of their mechanisms of action is still incomplete. Specifically, the role of hydrophobic drug interactions with polymers by considering possible supramolecular conformations in aqueous dispersion is an interesting topic. Accordingly, this study investigated the tendency of polymers to create hydrophobic domains, where lipophilic compounds may nest to support drug solubilisation and supersaturation. Fluorescence spectroscopy with the environment-sensitive probe pyrene was compared with atomistic molecular dynamics simulations of the model drug fenofibrate (FENO). Subsequently, kinetic drug supersaturation and thermodynamic solubility experiments were conducted. As a result, the different polymers showed hydrophobic domain formation to a varying degree and the molecular simulations supported interpretation of fluorescence spectroscopy data. Molecular insights were gained into the conformational structure of how the polymers interacted with FENO in solution phase, which apart from nucleation and crystal growth effects, determined drug concentrations in solution. Notable was that even at the lowest polymer concentration of 0.01 %, w/v, there were polymer-specific solubilisation effects of FENO observed and the resulting reduction in apparent drug supersaturation provided relevant knowledge both from a mechanistic and practical perspective.

OriginalsprogEngelsk
Artikelnummer106791
TidsskriftEuropean Journal of Pharmaceutical Sciences
Vol/bind198
Antal sider10
ISSN0928-0987
DOI
StatusUdgivet - 1. jul. 2024

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