Properties of spherical pellets produced by a hot-melt extrusion and spheronization process

Young, Christopher Ryan

28 August 2008

Not available / text

Melt spinning

Pelletizing

Drugs--Controlled release

NMR and MRI studies of controlled release drug delivery systems

Zhang, Qilei

January 2012

No description available.

660

In vitro and in vivo testing of a gastric retention device : development and evaluation of a new colonic delivery system

Ahmed, Iman Saad

04 September 2002

This thesis describes evaluation of a gastric retention device (GRD) developed at Oregon State University. The device was originally fabricated from Xanthan gum and Locust bean gum. A modified gastric retention device containing other additives was developed and investigated in this work. The modified device was evaluated in vitro for swelling and dissolution properties using riboflavin as a model drug. Different shapes and sizes of GRDs were tested in dogs to study the gastric retention potential of these devices. The effect of the device on food emptying from the stomach in dogs was also investigated. Endoscopic studies in dogs also showed that the device swells rapidly and considerably in gastric fluid. The bioavailability of riboflavin from three different size GRDs was determined in six fasted human volunteers and compared to an immediate release formulation. The biostudy indicated that the bioavailability of riboflavin from a large size GRD was more than triple that measured after administration of the immediate release formulation. Deconvolution was used to determine gastric residence time of the different size GRDs. A new colonic delivery system made of acetaminophen loaded beads produced by extrusion and spheronization and coated with different ratios of pectin and ethylcellulose coating solutions in a spray coating apparatus was also developed in this work. Such beads release their drug content in the colon due to susceptibility of pectin in the outer coat to enzymatic action of colonic bacteria. The new delivery system was evaluated in vitro by conducting release studies in different dissolution media to mimic transit times, pH and enzyme conditions in the gastrointestinal tract. The gastrointestinal transit behavior of drug beads was also assessed by conducting gamma-scintigraphic studies in dogs. The bioavailability and pharmacokinetic parameters of acetaminophen from several colonic delivery system formulations were determined in human volunteers and compared to the immediate release commercial product Tylenol®. A selected pectin-ethylcellulose coat formulation in the ratio 1:3 was further evaluated in six volunteers under both fed and fasting conditions and was found to be effective and to provide sustained drug release in the colon over a period of 12 hours. / Graduation date: 2003

Oral medication

Drugs -- Controlled release

Drug delivery systems

1) Development and in vivo testing of a gastric retention device (GRD) in dogs : 2) product formulations and in vitro-in vivo evaluation of a) immediate release formulation of itraconazole, b) controlled-release formulation of ketoprofen in adults

Kapsi, Shivakumar G.

24 November 1998

This thesis describes 1) development of a gastric retention device (GRD) to increase gastric retention time of certain drugs, 2) product formulations of an immediate release itraconazole and controlled-release ketoprofen. GRD was fabricated from crosslinked carbohydrate polymers. Rate and extent of hydration of the film in water and in simulated gastric fluid, compressibility of film, shape of the film, and in vivo gastric transit time in the stomach of dog were used as tools to evaluate gastric retention properties. Hydration studies were carried out at 37��C. Evaluation of the device containing radio-opaque agents, in dogs for gastric retention was carried out with the help of X-rays. The device was found to stay in the stomach of dogs for at least 10 hours. GRD containing amoxicillin trihydrate caplets were evaluated in a human. The area under the excretion rate curve was found to increase by 30% when compared to without the device. A successful development of a formulation of water insoluble itraconazole, without the use of organic solvents, was achieved with modifications from eutectic mixture techniques. Solubilization of the drug was achieved in polyethylene glycol of higher molecular weight. A series of formulations made by varying the amounts ingredients therein, were evaluated for dissolution profile in comparison with the reference, Sporanox��. Effect of molecular weights of PEG and types of PEG were evaluated for desired drug dissolution. Preliminary study from 6 subjects under the conditions of fasting and fed indicated that bioavailability from the new formulation was increased slightly when compared to the reference. This may be correlated to difference in the rate of in vitro dissolution, where the new formulation has initial faster dissolution. A controlled-release formulation of ketoprofen was also developed using a diffusion-controlled polymer, which was coated onto the drug beads. Release of drugs from such beads is controlled by the thickness of the coat. Thickness of the coat was evaluated by SEM and was correlated to the desired in vitro drug release in comparison to the reference Oruvail��. A three-way cross over study involving the new formulation and two marketed products in 12 subjects under fasting conditions indicated that there was a significant difference between the new product and marketed products, so as to be considered non-bioequivalent. Use of In Vitro-In Vivo Correlations and Convolution- Deconvolution relations predicted desired in vitro drug dissolution in a subsequent modification of the formulation. / Graduation date: 1999

Drugs -- Controlled release

Drug delivery systems

Oral medication

Development and evaluation of an oral controlled release and a transdermal delivery system, for melatonin in human subjects

Lee, Beom-jin

08 December 1992

Graduation date: 1993

Transdermal medication

Drugs -- Controlled release

Physicochemical and mechanical characterization of hot-melt extruded dosage forms

Crowley, Michael McDonald

28 August 2008

Not available / text

Drug delivery systems

Polymeric drugs

Drugs--Controlled release

Properties of polymeric drug delivery systems prepared by hot-melt extrusion

Zhu, Yucun

28 August 2008

Not available / text

Polymeric drugs

Drug delivery systems

Drugs--Controlled release

Lightly crosslinked poly(ethylene glycol)-tethered, pH-responsive biomaterials

Thomas, Joshua Brock

28 August 2008

Not available / text

Drugs--Controlled release

Polymeric drug delivery systems

Polymeric drugs

Investigation of cellulose ether polymers in controlled drug delivery

Mahaguna, Vorapann

28 March 2011

Not available / text

Drug delivery systems

Drugs--Controlled release

Cellulose ethers

Application of Silk Fibroin In Controlled-Release of Theophylline/

Özgarip, Yarkın. Bayraktar, Oğuz

January 2004

Thesis (Master)--İzmir Institute of Technology, İzmir, 2004. / Includes bibliographical references (leaves. 55-58).