Extended release dosage form
a technology of extended release and dosage form, which is applied in the direction of heterocyclic compound active ingredients, drug compositions, biocide, etc., can solve the problems of reducing structural integrity, dosage forms that did not protect a drug from oxidation, and not maintain the stability of a drug formulation
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example 1
[0080]The solubility of various hydrophilic materials to osmotic pressure was evaluated. First, aqueous solutions of the hydrophilic material hydroxypropyl-cellulose, commercially-available from Hercules, Wilmington, Del., under the trade name Klucel® were prepared using grades of different molecular weights. The solutions were prepared with molecular weights of 80,000 grams per mole, 300,000 and 1 million grams per mole using Klucel EF, GF and HF, respectively. An intermediate molecular weight of 190,000 grams per mole was also generated by blending equal weight portions of the EF and GF grades. The resulting solutions were then cast on glass plates and dried at room temperature. The resulting films were removed from the plates and a discs of 2.4 cm2 area were punched from the films. Thicknesses of the discs were measured with a table micrometer. Four discs of each molecular weight type were then individually bagged in nylon mesh bags having 12 openings per inch and attached to a p...
example 2
[0081]A novel, therapeutic composition comprising hydromorphone and acetaminophen, wherein the hydromorphone is a member selected from the group consisting of hydromorphone pharmaceutically acceptable base and hydromorphone pharmaceutically acceptable salt is prepared as follows. First, 175 g of hydromorphone hydrochloride, 500 g of acetaminophen, 647.5 g of poly(ethylene oxide) possessing a 100,000 molecular weight, and 43.75 g of poly(vinylpyrrolidone) having an average molecular weight of 40,000 are added to a mixing bowl and the ingredients dry mixed for 10 minutes. Then, 331 g of denatured, anhydrous alcohol is added slowly to the blended ingredients with continuous blending for 10 minutes. Next, the freshly prepared granulation is passed through a 20 mesh screen, allowed to dry at 25° C. for about 20 hours, and then passed through a 16 mesh screen. Next, the granulation is transferred to a mixer, and lubricated with 8.75 g of magnesium stearate to produce a therapeutic hydromo...
example 3
[0082]The hydromorphone-acetaminophen analgesic tablets are coated with an interior wall then coated by an exterior wall as follows. First, 154 g of ethyl cellulose having a molecular weight of 220,000 grams per mole and an ethoxyl content of 48.0 to 49.5 weight percent, and 112 g of hydroxypropylcellulose having a 80,000 molecular weight and a molar substitution of 3, and then 14 g of polyoxyethylene (40) stearate were dissolved with stirring in 3,720 g of anhydrous ethanol. The solution resulting was allowed to stand without stirring for 3 days, to provide the interior wall-forming composition. Next, the exterior wall forming composition was prepared by dissolving 162.5 g of cellulose acetate having an acetyl content of 39.8 wt % and a molecular weight of 40,000 grams per mole, and 87.5 g of ethylene oxide-propylene oxide-ethylene oxide triblock copolymer having a molecular weight of approximately 8,400 grams per mole and an ethylene oxide content of 82 wt % in 4,750 g of anhydrou...
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