Your search keyword '"Polymethacrylic Acids pharmacokinetics"' showing total 7 results

1. Dexibuprofen enteric film-coated tablets: design, characterization and pharmacokinetic analysis in human volunteers.

Author

Hanif AM, Rehman A, Bushra R, Aslam N, Alam S, Dawaba HM, Dawaba AM, and Sayed OM

Subjects

Humans, Male, Adult, Young Adult, Drug Liberation, Anti-Inflammatory Agents, Non-Steroidal pharmacokinetics, Anti-Inflammatory Agents, Non-Steroidal administration & dosage, Polymethacrylic Acids chemistry, Polymethacrylic Acids pharmacokinetics, Chemistry, Pharmaceutical methods, Healthy Volunteers, Drug Stability, Tablets, Enteric-Coated, Ibuprofen pharmacokinetics, Ibuprofen administration & dosage, Ibuprofen chemistry, Ibuprofen analogs & derivatives, Biological Availability

Abstract

Objective: This study aimed to develop a stable and scalable enteric film-coated tablet for the gastric irritant dexibuprofen., Methods: Utilizing direct compression with super-disintegration (crospovidone), the optimal core batches were coated with Opadry white seal coat and enterically coated with Eudragit ® L100 with pigment (Talc), demonstrating a 12% weight increase; release and integrity were assessed using specific pH buffers and SEM, with stability testing confirming a six-month shelf life at 40 °C and 75% RH., Results: The optimized formulation achieved 99.87% release in phosphate buffer within 60 min, maintained integrity for 120 min in acidic conditions, and exhibited superior bioavailability compared to Innovifen with relative bioavailability ≈of 121% and elevated C max (18.35 µg/ml compared to 11.1 µg/ml)., Conclusion: These results highlight the potential of this formulation to enhance patient safety and efficacy through delayed enteric technology and fast intestinal release.

Published

2024

2. The effect of some acrylic polymers on dissolution of celecoxib solid dispersion formulations.

Author

Maghsoodi M, Nokhodchi A, and Pourasghari Azar H

Subjects

Anti-Inflammatory Agents, Non-Steroidal pharmacokinetics, Calorimetry, Differential Scanning, Celecoxib pharmacokinetics, Drug Compounding methods, Drug Liberation, Humans, Hydrogen-Ion Concentration, Polymethacrylic Acids administration & dosage, Polymethacrylic Acids pharmacokinetics, Solubility, Spectroscopy, Fourier Transform Infrared, Anti-Inflammatory Agents, Non-Steroidal administration & dosage, Celecoxib administration & dosage

Abstract

Objective: The purpose of the present study was firstly to identify the effectiveness of Eudragit® polymers (Eudragit ® RL, RS, L100-55, L100, S100 and E100) in inhibition of celecoxib precipitation from buffer solutions (pH = 6.8). Furthermore, the influence of Eudragit ® polymers on non-sink dissolution behavior of celecoxib from solid dispersions was investigated., Methods: Solid dispersions were prepared by the rotary evaporation method. In vitro dissolution studies, FT-IR and differential scanning calorimetry were employed to characterize the formulations., Results: The results revealed that Eudragit ® E100, L100 and S100 inhibited precipitation of celecoxib efficiently. It is understood that crystallization during the dissolution of solid dispersions could happen through crystallization from solid matrix following contact with the dissolution medium or from the supersaturated solution produced following dissolution. The supersaturated drug concentrations attained from the dissolution of Eudragit ® -celecoxib solid dispersions were almost similar, suggesting that crystallization from solid matrix did not occur readily. However, only solid dispersions containing efficient crystallization inhibitor polymers were able to maintain the supersaturated solution up to the end of the dissolution run., Conclusion: Results revealed that the principal mechanism of attaining supersaturated solution of celecoxib from solid dispersions was related to crystallization inhibition from solution not from solid matrix.

Published

2021

3. Preparation and characterization of metformin hydrochloride loaded-Eudragit®RSPO and Eudragit®RSPO/PLGA nanoparticles.

Author

Cetin M, Atila A, Sahin S, and Vural I

Subjects

Delayed-Action Preparations administration & dosage, Delayed-Action Preparations chemical synthesis, Delayed-Action Preparations pharmacokinetics, Diabetes Mellitus, Type 2 drug therapy, Humans, Lactic Acid pharmacokinetics, Metformin pharmacokinetics, Polyglycolic Acid pharmacokinetics, Polylactic Acid-Polyglycolic Acid Copolymer, Polymethacrylic Acids pharmacokinetics, Reproducibility of Results, Chemistry, Pharmaceutical methods, Lactic Acid chemical synthesis, Metformin chemical synthesis, Nanoparticles chemistry, Polyglycolic Acid chemical synthesis, Polymethacrylic Acids chemical synthesis

Abstract

The aim of the present study was to develop and characterize metformin HCl-loaded nanoparticle formulations. Nanoparticles were prepared by the nanoprecipitation method using both a single polymer (Eudragit(®)RSPO) and a polymer mixture (Eudragit/PLGA). The mean particle size ranged from 268.8 to 288 nm and the nanoparticle surface was positively charged (9.72 to 10.1 mV). The highest encapsulation efficiency was observed when Eudragit®RSPO was used. All formulations showed highly reproducible drug release profiles and the in vitro drug release in phosphate buffer (pH = 6.8) ranged from 92 to 100% in 12 h. These results suggest that Eudragit(®)RSPO or Eudragit/PLGA nanoparticles might represent a promising sustained-release oral formulation for metformin HCl, reducing the necessity of repeated administrations of high doses to maintain effective plasma concentrations, and thus, increasing patient compliance and reducing the incidence of side-effects.

Published

2013

4. Biodegradation behavior of gellan gum in simulated colonic media.

Author

Singh BN, Trombetta LD, and Kim KH

Subjects

Azathioprine pharmacokinetics, Biodegradation, Environmental drug effects, Chemistry, Pharmaceutical, Colon drug effects, Colon enzymology, Delayed-Action Preparations chemistry, Delayed-Action Preparations pharmacokinetics, Drug Carriers chemistry, Drug Carriers pharmacokinetics, Drug Evaluation, Preclinical methods, Gastric Juice, Inflammatory Bowel Diseases drug therapy, Intestinal Mucosa enzymology, Mannosidases chemistry, Mannosidases pharmacokinetics, Mannosidases ultrastructure, Microscopy, Electron, Scanning methods, Polymethacrylic Acids chemistry, Polymethacrylic Acids classification, Polymethacrylic Acids pharmacokinetics, Polysaccharides chemistry, Polysaccharides pharmacokinetics, Polysaccharides ultrastructure, Polysaccharides, Bacterial chemistry, Polysaccharides, Bacterial ultrastructure, Technology, Pharmaceutical, Time Factors, Viscosity drug effects, Colon metabolism, Polysaccharides, Bacterial metabolism

Abstract

The objective of this investigation was to test the biodegradability of gellan gum in the presence of galactomannanase in order to explore its suitability for the development of colon-specific controlled delivery systems. Gellan beads containing azathioprine (AZA) were prepared by ionotropic gelation in the presence of Ca2+ ions and were coated with an enteric polymer, Eudragit S-100. The effects of the simulated colonic fluid (SCF, pH 7.4 phosphate buffer) containing 15 mg/mL of galactomannanase on the in vitro release profiles of uncoated and enteric-coated beads were investigated, and the morphological changes in the structure of uncoated beads were assessed by scanning electron microscopy (SEM). In addition, 1% solution of deacetylated gellan gum was prepared and several aliquots of the resulting solution were evaluated rheologically to determine the concentration- and time-dependent effects of galactomannanase. Based on the percent drug released at 2 h, approximately 10% greater amount of drug was released in the SCF containing galactomannanase when compared with the enzyme-free dissolution medium. Results of rheological studies demonstrated that effects of galactomannanase on the viscosity of gellan gum solution are concentration-dependent rather than time-dependent. A significant decrease in the viscosity was noted in the presence of galactomannanase at a concentration of 15 mg/ mL, indicating that the polysaccharide degraded in an enzymatic reaction. SEM micrographs showed a distinct disruption of the polymeric network in the SCF. Overall, the results suggest that gellan gum undergoes significant degradation in the presence of galactomannanase which in turn facilitates the drug release from beads in the SCF in a controlled manner, thus approving the suitability of gellan gum as a carrier for controlled colonic delivery.

Published

2004

5. Optimization of methacrylic acid ester copolymers blends as controlled release coatings using response surface methodology.

Author

AlKhatib HS and Sakr A

Subjects

Delayed-Action Preparations chemistry, Delayed-Action Preparations pharmacokinetics, Surface Properties, Tablets, Enteric-Coated, Polymethacrylic Acids chemistry, Polymethacrylic Acids pharmacokinetics

Abstract

The aim of this study was to statistically optimize the use of blends of methacrylic acid ester copolymers with different permeability properties as controlled-release coating systems for tablets to produce predictable predesigned release profiles. A full factorial design was used to study and optimize the use of methacrylic acid ester copolymers Eudragit RS 30D and Eudragit RL 30D as coating materials for controlled release. Directly compressed theophylline tablets were coated with aqueous dispersions containing different proportions of the two copolymers using a side-vented coating pan (Accela Cota). The effect of polymer loading level at 5, 7.5, and 10% weight gain and curing time at 50 degrees C for 12 and 24 hours were also evaluated. Coated tablets were tested for their drug release in water using a United States Pharmacopeia (USP) dissolution apparatus #2. The results showed that increasing the content of the lower permeability copolymer Eudragit RS 30D, increasing the polymer load, and increasing curing time at 50 degrees C resulted in slower drug release. A statistical model that describes and predicts the drug release properties of the coated tablets as a function of the copolymers ratio in the coating dispersion, polymer load, and curing time at 50 degrees C was developed. The most significant factor affecting drug release was found to be the ratio of the two copolymers in the coating dispersion followed by the curing time at 50 degrees C and the polymer loading level. Good correlations were observed between the model fitted values andthe experimental values. An optimized formula prepared by superimposing two-dimensional contour plots was prepared; its release profile was found to be in agreement with the prediction obtained from the model.

Published

2003

6. Studies in preparation and evaluation of pH-independent sustained-release matrix tablets of verapamil HCl using directly compressible Eudragits.

Author

Gohel MC, Patel TP, and Bariya SH

Subjects

Biological Availability, Chemistry, Pharmaceutical, Delayed-Action Preparations chemistry, Delayed-Action Preparations pharmacokinetics, Polymethacrylic Acids chemistry, Polymethacrylic Acids pharmacokinetics, Pressure, Tablets, Verapamil pharmacokinetics, Drug Compounding methods, Drug Evaluation, Preclinical methods, Hydrogen-Ion Concentration

Abstract

The objective of the present study was to investigate the impact of formulation factors on the properties of a 12h modified-release formulation of verapamil HCl. A 2(3) full factorial design was employed to investigate the influence of amount of Eudragit RS PO/RL PO (X1, a matrixing agent), HPMC K4M (X2, an auxiliary matrixing agent cum binder) and PEG 4000 (X3, channelling agent cum plasticizer). The tablets were prepared by direct compression and they were evaluated for in vitro dissolution studies in 0.1 N HCl. The time required for 90% of the drug release (t90) and similarity factor (f2) were used as responses for the selection of most appropriate batches. Swelling and fluid penetration studies were carried out in 0.1 N HCl. Time required for 90% of the drug release (t90) was calculated by using an appropriate kinetic model for each batch. An ideal drug release profile (i.e., 25% in the first hour and a constant drug release thereafter) was considered as a reference release profile for calculation of f2. Multiple regression analysis was adopted to evolve refined models for t90. The required release pattern was shown by batches containing a low level of Eudragit RS PO/RL PO (30% w/w), low level of HPMC K4M (10% w/w), and high level of PEG 4000 (15% w/w). Response surface plots are shown for t90. These formulations showed slower drug release in alkaline medium (pH 7.2). Succinic acid and KH2PO4 were incorporated in the matrix in order to obtain pH-independent drug release. Swelling of tablets and fluid penetration in the matrix were found to be influenced by the selected independent variables. This study demonstrates that the desired drug release pattern can be obtained by adopting a systematic formulation approach.

Published

2003

7. Influence of thermal processing on the properties of chlorpheniramine maleate tablets containing an acrylic polymer.

Author

Zhu Y, Shah NH, Malick AW, Infeld MH, and McGinity JW

Subjects

Chlorpheniramine pharmacokinetics, Citrates chemical synthesis, Citrates pharmacokinetics, Polymers pharmacokinetics, Polymethacrylic Acids chemical synthesis, Polymethacrylic Acids pharmacokinetics, Tablets, Enteric-Coated, Chlorpheniramine chemical synthesis, Hot Temperature, Polymers chemical synthesis

Abstract

The purpose of this investigation was to determine the effects of thermal processing and post-processing thermal treatment on the release properties of chlorpheniramine maleate (CPM) from matrix tablets containing Eudragit RS PO and triethyl citrate (TEC). CPM tablets containing Eudragit RS PO with and without TEC were prepared by direct compression (DC), high shear hot-melt granulation (HMG), and hot-melt extrusion (HME). X-ray diffraction patterns showed that the CPM was distributed in Eudragit RS PO at the molecular level following HME. The thermogravimetry analysis (TGA) profiles of CPM, Eudragit RS PO, and TEC demonstrated that these materials were thermally stable during both the high shear HMG and HME processes. The tablets were subjected to post-processing thermal treatment by storing the tablets at 60 degrees C in open containers for 24 hr. Tablets prepared by DC showed the highest drug release rate constant of 36.2% hr-1/2. When 4% TEC was incorporated into the formulation, the drug release rate constant for the directly compressed tablets decreased to 32.4% hr-1/2. After high shear HMG and HME of the powder blend containing 4% TEC, the drug release rate constant decreased to 30.8 and 13.8% hr-1/2 for the respective processes. The drug release rate constants for all tablets decreased following post-processing thermal treatment. The reduction in release rate was due to an increase in the intermolecular binding and entanglement between drug molecules and polymer molecules that occurred during thermal processing. Post-processing thermal treatment of the hot-melt extrudates had a minimal effect on the drug release rate since the HME process enhanced the drug and polymer entanglement to a greater extent.

Published

2002