Determination of Inherent Dissolution Performance of Drug Substances
The dissolution behavior of novel active pharmaceutical ingredients (API) is a crucial parameter in drug formulation since it frequently affects the drug release. Generally, a distinction is made between surface-reaction- and diffusion-controlled drug release. Therefore, dissolution studies such as...
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doaj-f6738991f45d4c4888f5295fa4237ff92021-01-23T00:06:35ZengMDPI AGPharmaceutics1999-49232021-01-011314614610.3390/pharmaceutics13020146Determination of Inherent Dissolution Performance of Drug SubstancesDominik Sleziona0Amelie Mattusch1Gerhard Schaldach2David R. Ely3Gabriele Sadowski4Markus Thommes5TU Dortmund, Laboratory of Solids Process Engineering, Faculty of Biochemical and Chemical Engineering, Emil-Figge-Str. 68, 44227 Dortmund, GermanyTU Dortmund, Laboratory of Solids Process Engineering, Faculty of Biochemical and Chemical Engineering, Emil-Figge-Str. 68, 44227 Dortmund, GermanyTU Dortmund, Laboratory of Solids Process Engineering, Faculty of Biochemical and Chemical Engineering, Emil-Figge-Str. 68, 44227 Dortmund, GermanyIvy Tech Community College Lafayette, School of Advanced Manufacturing, Engineering and Applied Science, 3101 S Creasy Ln, Lafayette, IN 47905, USATU Dortmund, Laboratory of Thermodynamics, Faculty of Biochemical and Chemical Engineering, Technical University Dortmund, Emil-Figge-Str. 70, 44227 Dortmund, GermanyTU Dortmund, Laboratory of Solids Process Engineering, Faculty of Biochemical and Chemical Engineering, Emil-Figge-Str. 68, 44227 Dortmund, GermanyThe dissolution behavior of novel active pharmaceutical ingredients (API) is a crucial parameter in drug formulation since it frequently affects the drug release. Generally, a distinction is made between surface-reaction- and diffusion-controlled drug release. Therefore, dissolution studies such as the intrinsic dissolution test defined in the pharmacopeia have been performed for many years. In order to overcome the disadvantages of the common intrinsic dissolution test, a new experimental setup was developed within this study. Specifically, a flow channel was designed and tested for measuring the mass transfer from a flat, solid surface dissolving into a fluid flowing over the surface with well-defined flow conditions. A mathematical model was developed that distinguishes between surface-reaction- and diffusion-limited drug release based on experimental data. Three different drugs—benzocaine, theophylline and griseofulvin—were used to investigate the mass flux during dissolution due to surface reaction, diffusion and convection kinetics. This new technique shows potential to be a valuable tool for the identification of formulation strategies.https://www.mdpi.com/1999-4923/13/2/146drug releaseflow channelintrinsic dissolutionsurface reactiontwo-film theory |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Dominik Sleziona Amelie Mattusch Gerhard Schaldach David R. Ely Gabriele Sadowski Markus Thommes |
spellingShingle |
Dominik Sleziona Amelie Mattusch Gerhard Schaldach David R. Ely Gabriele Sadowski Markus Thommes Determination of Inherent Dissolution Performance of Drug Substances Pharmaceutics drug release flow channel intrinsic dissolution surface reaction two-film theory |
author_facet |
Dominik Sleziona Amelie Mattusch Gerhard Schaldach David R. Ely Gabriele Sadowski Markus Thommes |
author_sort |
Dominik Sleziona |
title |
Determination of Inherent Dissolution Performance of Drug Substances |
title_short |
Determination of Inherent Dissolution Performance of Drug Substances |
title_full |
Determination of Inherent Dissolution Performance of Drug Substances |
title_fullStr |
Determination of Inherent Dissolution Performance of Drug Substances |
title_full_unstemmed |
Determination of Inherent Dissolution Performance of Drug Substances |
title_sort |
determination of inherent dissolution performance of drug substances |
publisher |
MDPI AG |
series |
Pharmaceutics |
issn |
1999-4923 |
publishDate |
2021-01-01 |
description |
The dissolution behavior of novel active pharmaceutical ingredients (API) is a crucial parameter in drug formulation since it frequently affects the drug release. Generally, a distinction is made between surface-reaction- and diffusion-controlled drug release. Therefore, dissolution studies such as the intrinsic dissolution test defined in the pharmacopeia have been performed for many years. In order to overcome the disadvantages of the common intrinsic dissolution test, a new experimental setup was developed within this study. Specifically, a flow channel was designed and tested for measuring the mass transfer from a flat, solid surface dissolving into a fluid flowing over the surface with well-defined flow conditions. A mathematical model was developed that distinguishes between surface-reaction- and diffusion-limited drug release based on experimental data. Three different drugs—benzocaine, theophylline and griseofulvin—were used to investigate the mass flux during dissolution due to surface reaction, diffusion and convection kinetics. This new technique shows potential to be a valuable tool for the identification of formulation strategies. |
topic |
drug release flow channel intrinsic dissolution surface reaction two-film theory |
url |
https://www.mdpi.com/1999-4923/13/2/146 |
work_keys_str_mv |
AT dominiksleziona determinationofinherentdissolutionperformanceofdrugsubstances AT ameliemattusch determinationofinherentdissolutionperformanceofdrugsubstances AT gerhardschaldach determinationofinherentdissolutionperformanceofdrugsubstances AT davidrely determinationofinherentdissolutionperformanceofdrugsubstances AT gabrielesadowski determinationofinherentdissolutionperformanceofdrugsubstances AT markusthommes determinationofinherentdissolutionperformanceofdrugsubstances |
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