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Startseite » 3D Printing » Multi-Purposable Filaments of HPMC for 3D Printing of Medications with Tailored Drug Release and Timed-Absorption

Multi-Purposable Filaments of HPMC for 3D Printing of Medications with Tailored Drug Release and Timed-Absorption

24. April 2018
Multi-Purposable Filaments of HPMC for 3D Printing of Medications with Tailored Drug Release and Timed-Absorption

24. April 2018

Three-dimensional printing (3DP), though developed for nonmedical applications and once regarded as futuristic only, has recently been deployed for the fabrication of pharmaceutical products.However, the existing feeding materials (inks and filaments) that are used for printing drug products have various shortcomings, including the lack of biocompatibility, inadequate extrudability andprintability, poor drug loading, and instability. Here, we have sought to develop a filament using a single pharmaceutical polymer, with no additives, which can be multi-purposed and manipulated bycomputational design for the preparation of tablets with desired release and absorption patterns. As such, we have used hydroxypropyl-methylcellulose (HPMC) and diltiazem, a model drug, to prepareboth drug-free and drug-impregnated filaments, and investigated their thermal and crystalline properties, studied the cytotoxicity of the filaments, designed and printed tablets with various infilldensities and patterns. By alternating the drug-free and drug-impregnated filaments, we fabricated various types of tablets, studied the drug release profiles, and assessed oral absorption in rats.Both diltiazem and HPMC were stable at extrusion and printing temperatures, and the drug loading was 10% (w/w). The infill density, as well as infill patterns, influenced the drug release profile,and thus, when the infill density was increased to 100%, the percentage of drug released dramatically declined. Tablets with alternating drug-free and drug-loaded layers showed delayed andintermittent drug release, depending on when the drug-loaded layers encountered the dissolution media. Importantly, the oral absorption patterns accurately reproduced the drug release profiles andshowed immediate, extended, delayed and episodic absorption of the drug from the rat gastrointestinal tract (GIT). Overall, we have demonstrated here that filaments for 3D printers can be preparedfrom a pharmaceutical polymer with no additives, and the novel computational design allows for fabricating tablets with the capability of producing distinct absorption patterns after oraladministration.

More
Graphical overview 3D pharmaceutical printing and filaments of hydroxypropyl-methylcellulose
Overview 3D printing for pharmaceutical products and multi-purposable filaments

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      • Captisol
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