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Formulation of 3D Printed Tablet for Rapid Drug Release by Fused Deposition Modeling: Screening Polymers for Drug Release,Drug-Polymer Miscibility and Printability
Authors:Nayan G. Solanki  Md Tahsin  Ankita V. Shah  Abu T.M. Serajuddin
Affiliation:Department of Pharmaceutical Sciences, College of Pharmacy and Health Sciences, St. John''s University, 8000 Utopia Parkway, Queens, New York 11439
Abstract:The primary aim of this study was to identify pharmaceutically acceptable amorphous polymers for producing 3D printed tablets of a model drug, haloperidol, for rapid release by fused deposition modeling. Filaments for 3D printing were prepared by hot melt extrusion at 150°C with 10% and 20% w/w of haloperidol using Kollidon® VA64, Kollicoat® IR, Affinsiol?15 cP, and HPMCAS either individually or as binary blends (Kollidon® VA64 + Affinisol? 15 cP, 1:1; Kollidon® VA64 + HPMCAS, 1:1). Dissolution of crushed extrudates was studied at pH 2 and 6.8, and formulations demonstrating rapid dissolution rates were then analyzed for drug-polymer, polymer-polymer and drug-polymer-polymer miscibility by film casting. Polymer-polymer (1:1) and drug-polymer-polymer (1:5:5 and 2:5:5) mixtures were found to be miscible. Tablets with 100% and 60% infill were printed using MakerBot printer at 210°C, and dissolution tests of tablets were conducted at pH 2 and 6.8. Extruded filaments of Kollidon® VA64-Affinisol? 15 cP mixtures were flexible and had optimum mechanical strength for 3D printing. Tablets containing 10% drug with 60% and 100% infill showed complete drug release at pH 2 in 45 and 120 min, respectively. Relatively high dissolution rates were also observed at pH 6.8. The 1:1-mixture of Kollidon® VA64 and Affinisol?15 cP was thus identified as a suitable polymer system for 3D printing and rapid drug release.
Keywords:3D printing  fused deposition modeling  FDM  drug-polymer miscibility  rheology  amorphous solid dispersion  tablets  dissolution rate
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