RESUMO
The phenomena taking place at the patch-skin interface, in particular the adhesion of a pressure sensitive adhesive (PSA) film loaded with drug and the partition of the drug between the patch and the skin were correlated. The kinetics of adhesion as well as those of drug passage were studied in detail. Adhesion data were collected from peel test either on skin or on a polymer model. Passage of the drug was studied in a simple system composed of PSA film stuck on skin. In some experiments the film was left on the skin throughout the experiment; in others, it was periodically removed and stuck on again to keep the adhesion force constant during the whole of the experiment. We observed a rapid increase of the drug content in the skin until a plateau was reached. One adhesion for the whole experiment or several adhesions gave a similar curve. The main difference was the rate of increase of skin drug content and the value of the plateau. Different hypotheses concerning the relationship between the adhesion of this PSA and changes in the flux of drug have been put forward. However, it is difficult to extrapolate from this model to the in vivo situation because of variation both between individuals and with time.
Assuntos
Farmacocinética , Absorção Cutânea/fisiologia , Adesividade , Administração Cutânea , Humanos , Politetrafluoretileno , Promegestona/administração & dosagem , Promegestona/análogos & derivados , Promegestona/farmacocinética , Elastômeros de SiliconeRESUMO
The adhesion of a new Transdermal Therapeutic System (TTS) made of silicone and loaded with a progestomimetic drug was characterised. The goal of this study was to use well-known methods or to adapt them to collect representative data. Individually, methods such as surface tension, peel test and rheology are already widely used. Results show that the choice of a substrate for peel tests can be made in the light of surface tension data and that polymers like poly(tetrafluoroethylene) (PTFE) are good alternatives to skin. Peeling characterisations are made a function of thickness of films, drug content in active, conditions of preparation and conditions of use such as pressure. Dynamic rheology is more difficult to link to other methods as it mainly reflects internal phenomena and properties that arise in the bulk, as opposed on its surface. Master curves enable results to be used more easily, but the theories to interpret the data are still not powerful enough to replace peel testing.
