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Journal article

The effect of the molecular weight of polyvinylpyrrolidone and the model drug on laser-induced in situ amorphization

Edited by Jampilek, Josef

From

University of Copenhagen1

Karolinska Institutet2

Uppsala University3

Department of Photonics Engineering, Technical University of Denmark4

Diode Lasers and LED Systems, Department of Photonics Engineering, Technical University of Denmark5

Laser radiation has been shown to be a promising approach for in situ amorphization, i.e., drug amorphization inside the final dosage form. Upon exposure to laser radiation, elevated temperatures in the compacts are obtained. At temperatures above the glass transition temperature (Tg) of the polymer, the drug dissolves into the mobile polymer.

Hence, the dissolution kinetics are dependent on the viscosity of the polymer, indirectly determined by the molecular weight (Mw) of the polymer, the solubility of the drug in the polymer, the particle size of the drug and the molecular size of the drug. Using compacts containing 30 wt% of the drug celecoxib (CCX), 69.25 wt% of three different Mw of polyvinylpyrrolidone (PVP: PVP12, PVP17 or PVP25), 0.25 wt% plasmonic nanoaggregates (PNs) and 0.5 wt% lubricant, the effect of the polymer Mw on the dissolution kinetics upon exposure to laser radiation was investigated.

Furthermore, the effect of the model drug on the dissolution kinetics was investigated using compacts containing 30 wt% of three different drugs (CCX, indomethacin (IND) and naproxen (NAP)), 69.25 wt% PVP12, 0.25 wt% PN and 0.5 wt% lubricant. In perfect correlation to the Noyes–Whitney equation, this study showed that the use of PVP with the lowest viscosity, i.e., the lowest Mw (here PVP12), led to the fastest rate of amorphization compared to PVP17 and PVP25.

Furthermore, NAP showed the fastest rate of amorphization, followed by IND and CCX in PVP12 due to its high solubility and small molecular size.

Language: English
Publisher: MDPI
Year: 2021
Pages: 4035
ISSN: 14203049 and 14315157
Types: Journal article
DOI: 10.3390/molecules26134035
ORCIDs: 0000-0002-1021-6898 , 0000-0002-8710-6347 , Hansen, Anders Kragh , 0000-0002-8922-3774 , 0000-0002-5992-9688 , 0000-0001-6514-8960 and 0000-0001-5040-620X

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