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On the usefulness of four in vitro methods in assessing the intraluminal performance of poorly soluble, ionisable compounds in the fasted state
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Publikationsdatum
2022
Autor:innen
O'Dwyer, Patrick J.
Box, Karl J
Vertzoni, Maria
Reppas, Christos
Imanidis, Georgios
Zeitschriftentitel
ISSN der Zeitschrift
Bandtitel
Verlag
Elsevier
Zusammenfassung
A small-scale two-stage biphasic system, a small-scale two-stage dissolution-permeation system, the Erweka
mini-paddle apparatus, and the BioGIT system were evaluated for their usefulness in assessing the intraluminal
performance of two low solubility drugs in the fasted state, one with weakly acidic properties (tested in a salt
form, diclofenac potassium) and one with weakly alkaline properties [ritonavir, tested as an amorphous solid
dispersion (ASD) formulation].
In all in vitro methods, an immediate-release tablet and a powder formulation of diclofenac potassium were
both rapidly dissolved in Level II biorelevant media simulating the conditions in the upper small intestine.
Physiologically based biopharmaceutics (PBB) modelling for the tablet formulation resulted in a successful
simulation of the average plasma profile in adults, whereas for the powder formulation modelling indicated that
gastric emptying and transport through the intestinal epithelium limit the absorption rates.
Detailed information on the behaviour of the ritonavir ASD formulation under both simulated gastric and
upper small intestinal conditions were crucial for understanding the luminal performance. PBB modelling
showed that the dissolution and precipitation parameters, estimated from the Erweka mini-paddle apparatus
data and the small-scale two-stage biphasic system data, respectively, were necessary to adequately simulate the
average plasma profile after administration of the ritonavir ASD formulation. Simulation of the gastrointestinal
transfer process from the stomach to the small intestine was necessary to evaluate the effects of hypochlorhydric
conditions on the luminal performance of the ritonavir ASD formulation.
Based on this study, the selection of the appropriate in vitro method for evaluating the intraluminal perfor-
mance of ionisable lipophilic drugs depends on the characteristics of the drug substance. The results suggest that
for (salts of) acidic drugs (e.g., diclofenac potassium) it is only an issue of availability and ease of operation of the
apparatus. For weakly alkaline substances (e.g., ritonavir), the results indicate that the dynamic dissolution
process needs to be simulated, with the type of requested information (e.g., dissolution parameters, precipitation
parameters, luminal concentrations) being key for selecting the most appropriate method. Regardless of the
ionisation characteristics, early in the drug development process the use of small-scale systems may be inevitable,
due to the limited quantities of drug substance available.
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DOI der Originalpublikation
Zitation
O’DWYER, Patrick J., Karl J BOX, Maria VERTZONI, Christos REPPAS und Georgios IMANIDIS, 2022. On the usefulness of four in vitro methods in assessing the intraluminal performance of poorly soluble, ionisable compounds in the fasted state. European Journal of Pharmaceutical Sciences. 2022. Bd. 168. DOI 10.1016/j.ejps.2021.106034. Verfügbar unter: https://doi.org/10.1016/j.ejps.2021.106034