Dissolution Kinetic of Meloxicam From Hydrophilic Matrix-Type Films for Transdermal Therapy

Antonoaea, Paula

doi:10.31925/farmacia.2021.1.13

Cited by 2 publications

(3 citation statements)

References 19 publications

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“…Understanding the effect of dissolution media on release kinetics and the mathematical description of dissolution process is of main importance for the process of selection of appropriate dissolution conditions and for efficient product development [1,19].…”

Section: Dissolution Kineticsmentioning

confidence: 99%

Influence of Dissolution Conditions on the Dissolution Rate and Release Mechanism of Ketoprofen From Extended Release Hydrophilic Matrix Systems

CASIAN¹

2022

FARMACIA

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Development of a hydrophilic matrix based extended release system involves the appropriate selection of polymer type, excipients and active ingredient with suitable physicochemical properties in order to obtain the desired release profile. Considering the multivariate nature of factors affecting the dissolution rate from hydrophilic matrix tablets, this study evaluates the effect of dissolution media, device type and stirring rate on the dissolution rate and release mechanism of ketoprofen from hydroxyethylcellulose and hydroxypropylmethylcellulose K4M matrices. The results show that dissolution media type influenced the release rate mostly by limiting solubility, but also by influencing polymer hydration time and solubility. The effect of stirring rate was dependent on device type, dissolution media and product type. Results also show that the selection of device type is an important step in the development of an appropriate dissolution test considering the sticking properties of hydrophilic matrices. Using multivariate data analysis, by developing O2PLS models, the systematic variation between dissolution profiles, kinetic parameters and dissolution conditions was integrated, highlighting joint and unique sources of variations. O2PLS results show that drug release mechanism is mostly influenced by media type, followed by stirring rate and at last by product type. RezumatDezvoltarea unui sistem de eliberare cu cedare prelungită de tip matriță hidrofilă implică selectarea adecvată a tipului de polimer, a excipienților și a substanței medicamentoase, cu proprietăți fizico-chimice potrivite pentru a obține profilul de eliberare dorit. Având în vedere natura multivariată a factorilor care afectează cedarea din comprimate de tip matriță hidrofilă, acest studiu evaluează efectul mediului de dizolvare, tipul dispozitivului și vitezei de agitare asupra vitezei de dizolvare și mecanismului de eliberare a ketoprofenului din matrițe de hidroxietilceluloza și hidroxipropilmetilceluloză K4M. Rezultatele au evidențiat o influență a mediului de dizolvare, în principal prin limitarea solubilității, dar și prin influențarea timpului de hidratare a polimerului și a solubilității acestuia. Efectul vitezei de agitare a fost dependent de tipul dispozitivului, mediul de dizolvare și tipul de produs. De asemenea, s-a identificat importanța selectării tipului de dispozitiv în dezvoltarea unui test de dizolvare adecvat, având în vedere proprietățile de lipire ale matrițelor hidrofile. Folosind metode de analiză multivariată, prin dezvoltarea de modele O2PLS, a fost integrată variația sistematică între profilurile de dizolvare, parametrii cinetici și condițiile de dizolvare, identificând surse comune și unice de variații. Modelul O2PLS arată că mecanismul de eliberare a medicamentului este în mare parte influențat de tipul de mediu, urmat de viteza de agitare și în cele din urmă de tipul de produs.

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Section: Dissolution Kineticsmentioning

confidence: 99%

Influence of Dissolution Conditions on the Dissolution Rate and Release Mechanism of Ketoprofen From Extended Release Hydrophilic Matrix Systems

CASIAN¹

2022

FARMACIA

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“…Different types of diffusion cells are described each with different dimensions (the diffusion surface available has a diameter between 0.3 and 5.0 cm 2 ; a volume of the receptor solution between 2 and 20 mL), all having in common both an acceptor media and a donor media [1][2][3][4]. The Franz diffusimetric cell can be used in most of the studies that aim to establish the cutaneous permeability of some APIs [9][10][11]. The method that uses the vertical Franz cell enables the determination of the API released from a sample which in accordance with the 428 OECD/ OCDE specifications is deposited on a membrane (donor compartment).…”

Section: Introductionmentioning

confidence: 99%

“…The method that uses the vertical Franz cell enables the determination of the API released from a sample which in accordance with the 428 OECD/ OCDE specifications is deposited on a membrane (donor compartment). After the diffusion through the membrane's pores, the API is crossing the membrane in the acceptor compartment from where it can be quantified by applying a suitable dosage method for the selected API [9][10][11][12][13]. Among the most important parameters that are taken into consideration whilst using the Franz cell is the provision of a corresponding seal of the membrane and the analysed formulation, a good homogeneity of the receptor solution (found under the membrane), easy sampling at different time intervals and corresponding control of the temperature during the determinations.…”

Section: Introductionmentioning

confidence: 99%

Design and Characterisation of New Dermal Polymeric Films for Treatment of Inflammatory Pain

ANTONOAEA

2023

FARMACIA

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This study aimed to develop two polymeric films containing indomethacin (IND) coded as F1 and F2. As a formulation variable, the propylene glycol (PG) concentration was used (F1-10%PG and F2-30%PG). DSC analysis was used to evaluate the compatibility between the film-forming agent and the IND. These two formulations were obtained through the solvent evaporation technique and evaluated for: uniformity of weight, elongation, folding endurance, behaviour in different humidity conditions, and the in vitro releasing test using a Franz cell. The DSC obtained results showed good compatibility between the film-forming agent and the IND. The analysis of the elongation behaviour considering an increased force and repeated folds obtained showed close results for both formulations. Also, in both cases, an increased tendency of drying through volatilization compared to the capacity of fixing water from the atmosphere was noticed, highlighting the importance of maintaining an exterior protection membrane when the film is applied to the skin. Through the in vitro dissolution test, after 30 h the cumulative amount of IND released was: F1 -83 ± 4.44 µg/cm 2 ; F2 -127 ± 4.41 µg/cm 2 , which demonstrated that an increased concentration of PG favours an increased release of concentration of drug. The proper kinetic model that characterized the IND release was established using the Akaike index, also the F1-10%PG is fitted through the Korsmeyer-Peppas kinetics, whilst F2-30%PG is fitted through the First-order kinetic. In conclusion, pain transdermal therapy may represent an alternative to other forms of treatment, being eligible for patients with deglutition issues. RezumatAcest studiu își propune dezvoltarea a două formulări de filme polimerice cu conținut de indometacină (IND): F1, F2, în care, ca variabilă de formulare s-a utilizat concentrația de propilenglicol (PG): F1-10%PG, respectiv F2-30%PG. Pentru evaluarea compatibilității între polimerul formator de film și IND s-a aplicat analiza DSC a acestora. Cele 2 formulări s-au preparat prin tehnica evaporării solventului și s-au evaluat în ceea ce privește: greutatea, rezistența la întindere, rezistența la pliere, comportamentul în diferite condiții de umiditate și cedarea in vitro prin metoda cu celula Franz. Rezultatele obținute ne-au arătat o bună compatibilitate între polimerul formator de film și IND. La analiza comportamentului la alungire sub acțiunea unei forțe crescătoare, respectiv la plieri repetate s-au obținut rezultate apropiate pentru F1 și F2. De asemenea, ambele formulări au prezentat o tendință mai mare de a se usca prin volatilizare față de capacitatea de a fixa vaporii de apă din atmosferă, ceea ce scoate în evidență importanța menținerii unei membrane de protecție exterioare atunci când sunt aplicate pe piele. Prin studiul in vitro, după 30 h cantitatea cumulativă de IND cedat a fost: F1 -83 ± 4,44 µg/cm 2 ; F2 -127 ± 4,41 µg/cm 2 , rezultatele obținute demonstrând că o concentrație mai mare de PG favorizează cedarea unei cantități mai mari de substanță activ...

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Dissolution Kinetic of Meloxicam From Hydrophilic Matrix-Type Films for Transdermal Therapy

Cited by 2 publications

References 19 publications

Influence of Dissolution Conditions on the Dissolution Rate and Release Mechanism of Ketoprofen From Extended Release Hydrophilic Matrix Systems

Influence of Dissolution Conditions on the Dissolution Rate and Release Mechanism of Ketoprofen From Extended Release Hydrophilic Matrix Systems

Design and Characterisation of New Dermal Polymeric Films for Treatment of Inflammatory Pain

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