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Fasted intestinal solubility limits and distributions applied to the biopharmaceutics and developability classification systems
- Source :
- European Journal of Pharmaceutics and Biopharmaceutics
- Publication Year :
- 2022
- Publisher :
- Elsevier BV, 2022.
-
Abstract
- Graphical abstract<br />After oral administration, a drug’s solubility in intestinal fluid is an important parameter influencing bioavailability and if the value is known it can be applied to estimate multiple biopharmaceutical parameters including the solubility limited absorbable dose. Current in vitro measurements may utilise fasted human intestinal fluid (HIF) or simulated intestinal fluid (SIF) to provide an intestinal solubility value. This single point value is limited since its position in relation to the fasted intestinal solubility envelope is unknown. In this study we have applied a nine point fasted equilibrium solubility determination in SIF, based on a multi-dimensional analysis of fasted human intestinal fluid composition, to seven drugs that were previously utilised to investigate the developability classification system (ibuprofen, mefenamic acid, furosemide, dipyridamole, griseofulvin, paracetamol and acyclovir). The resulting fasted equilibrium solubility envelope encompasses literature solubility values in both HIF and SIF indicating that it measures the same solubility space as current approaches with solubility behaviour consistent with previous SIF design of experiment studies. In addition, it identifies that three drugs (griseofulvin, paracetamol and acyclovir) have a very narrow solubility range, a feature that single point solubility approaches would miss. The measured mid-point solubility value is statistically equivalent to the value determined with the original fasted simulated intestinal fluid recipe, further indicating similarity and that existing literature results could be utilised as a direct comparison. Since the multi-dimensional approach covered greater than ninety percent of the variability in fasted intestinal fluid composition, the measured maximum and minimum equilibrium solubility values should represent the extremes of fasted intestinal solubility and provide a range. The seven drugs all display different solubility ranges and behaviours, a result also consistent with previous studies. The dose/solubility ratio for each measurement point can be plotted using the developability classification system to highlight individual drug behaviours. The lowest solubility represents a worst-case scenario which may be useful in risk-based quality by design biopharmaceutical calculations than the mid-point value. The method also permits a dose/solubility ratio frequency distribution determination for the solubility envelope which permits further risk-based refinement, especially where the drug crosses a classification boundary. This novel approach therefore provides greater in vitro detail with respect to possible biopharmaceutical performance in vivo and an improved ability to apply risk-based analysis to biopharmaceutical performance. Further studies will be required to expand the number of drugs measured and link the in vitro measurements to in vivo results.
- Subjects :
- RM
PREDICTION
Administration, Oral
Biological Availability
Acyclovir
Pharmaceutical Science
Ibuprofen
Article
Mefenamic acid
Griseofulvin
Biopharmaceutics
MEDIA
FLUIDS
DESIGN
DISSOLUTION
Furosemide
Fasted simulated intestinal fluid
Humans
ORAL-DRUG ABSORPTION
Pharmacology & Pharmacy
ComputingMethodologies_COMPUTERGRAPHICS
Science & Technology
EQUILIBRIUM SOLUBILITY
Intestinal Secretions
Dipyridamole
General Medicine
Hydrogen-Ion Concentration
Biopharmaceutics classification system
VARIABILITY
Developability classification system
Paracetamol
Intestinal Absorption
Pharmaceutical Preparations
Solubility
Life Sciences & Biomedicine
Biotechnology
Subjects
Details
- ISSN :
- 09396411
- Volume :
- 170
- Database :
- OpenAIRE
- Journal :
- European Journal of Pharmaceutics and Biopharmaceutics
- Accession number :
- edsair.doi.dedup.....7a5b0f1a056217891a3ba888136454b5
- Full Text :
- https://doi.org/10.1016/j.ejpb.2021.12.006