Szczegóły publikacji

Opis bibliograficzny

3D printed drug delivery systems in action–magnetic resonance imaging and relaxometry for monitoring mass transport phenomena / Ewelina Baran, Artur Birczyński, Bartłomiej Milanowski, Jolanta Klaja, Piotr NOWAK, Przemysław Dorożyński, Piotr Kulinowski // ACS Applied Materials & Interfaces ; ISSN 1944-8244. — 2024 — vol. 16 iss. 31, s. 40714–40725. — Bibliogr. s. 40724–40725, Abstr. — Publikacja dostępna online od: 2024-07-26

Autorzy (7)

  • Baran Ewelina
  • Birczyński Artur
  • Milanowski Bartłomiej
  • Klaja Jolanta
  • AGHNowak Piotr
  • Dorożyński Przemysław
  • Kulinowski Piotr

Słowa kluczowe

digital light processing3D printingstereolithographymass transportDLPmagnetic resonance imagingcontrolled release drug delivery systemsvat photopolymerizationVPPadditive manufacturingMRI

Dane bibliometryczne

ID BaDAP154911
Data dodania do BaDAP2024-09-13
Tekst źródłowyURL
DOI10.1021/acsami.4c08501
Rok publikacji2024
Typ publikacjiartykuł w czasopiśmie
Otwarty dostęptak
Czasopismo/seriaACS Applied Materials & Interfaces

Abstract

The hypothesis of the study was that (1) 3D printed drug delivery systems (DDS) could be characterized in situ during drug release using NMR/MRI techniques in terms of mass transport phenomena description (interfacial phenomena), particularly for systems dealing with two mobile phases (e.g., water and low molecular weight liquid polymer); (2) consequently, it could be possible to deduce how these interfacial mass transport phenomena influence functional properties of 3D printed DDS. Matrix drug delivery systems, prepared using masked stereolithography (MSLA), containing poly(ethylene glycol) diacrylate (PEGDA) and low molecular weight polyethylene glycol (PEG) with ropinirole hydrochloride (RH) were studied as example formulations. The PEGDA to PEG (mobile phase) concentration ratio influenced drug release. It was reflected in spatiotemporal changes in parametric T2 relaxation time (T2) and amplitude (A) images obtained using magnetic resonance imaging (MRI) and T1-T2 relaxation time correlations obtained using low-field time-domain nuclear magnetic resonance (LF TD NMR) relaxometry during incubation in water. For most of the tested formulations, two signal components related to PEG and water were assessed in the hydrated matrices by MRI relaxometry (parametric T2/A images). The PEG component faded out due to outward PEG diffusion and was gradually replaced by the water component. Both components spatially and temporally changed their parameters, reflecting evolving water–polymer interactions. The study shows that dynamic phenomena related to bidirectional mass transport can be quantified in situ using NMR and MRI techniques to gain insight into drug release mechanisms from 3D printed DDS systems.

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