Biodegradable implantation controlled-release microsphere using vibration membrane technique
A biodegradable and microsphere technology, which is applied in the direction of medical preparations of non-active ingredients, drug combinations, powder delivery, etc., can solve the problems of low drug loading, easy degradation and failure of raw materials, etc., to reduce residues and avoid raw materials Effects of drug loss, non-degradability and failure
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Embodiment 1
[0035] Embodiment 1 Preparation of polylactic acid microparticles of the present invention
[0036] The raw material drug is 5-fluorouracil. First make 5-fluorouracil into 10-50nm particles for later use.
[0037] Using chloroform as a solvent, polylactic acid is dissolved to prepare a polylactic acid solution with a concentration of 30% by weight. The above-mentioned nanoscale 5-fluorouracil was mixed into the polylactic acid solution, stirred evenly, and the chloroform in the solution was vacuum-sucked to let it volatilize rapidly. The drug-loaded polylactic acid solution is solidified into particles with a diameter of 2-3 mm by extrusion, mixed with liquid nitrogen as a coolant, and then added to a vibration mill to reduce the temperature of the drug-loaded particles to -60°C. machine. Sieve to collect drug-loaded particles with a size of 20-200 microns for later use.
[0038] It is detected by the method on page 395 of the Pharmacopoeia of the People's Republic of China ...
Embodiment 2
[0040] Embodiment 2 Preparation of polylactic acid-glycolic acid microparticles of the present invention
[0041] The raw material drug is carboplatin. First make carboplatin 10-50nm for use.
[0042] Polylactic acid-glycolic acid was dissolved in chloroform as a solvent to make a 20% solution. Mix the above-mentioned nanoscale carboplatin into the polylactic acid solution, stir evenly, and vacuum the chloroform in the solution to let it volatilize rapidly. The method of extrusion solidifies the drug-loaded polylactic acid solution into particles with a diameter of 2-3 mm, mixes with liquid nitrogen, and then puts it into a vibrating mill so that the temperature of the drug-loaded particles drops to -50°C. After repeated crushing, it is discharged from the machine. Sieve to collect drug-loaded particles with a size of 20-100 microns for later use.
[0043] It is detected by the method on page 108 of the Pharmacopoeia of the People's Republic of China 2005 edition, and its d...
Embodiment 3
[0045] Embodiment 3 Preparation of polylactic acid microparticles of the present invention
[0046] Cisplatin was made into 10-50nm microparticles for use. The polylactic acid is heated slowly in the temperature control box, and the solid polylactic acid becomes viscous after melting, and the interior lacks convection and conduction similar to water heating, mainly due to the lack of convective internal heat exchange. In order to prevent uneven heating, the heating rate was controlled at 25°C / hour. At 175°C, polylactic acid is in a liquid state, add nano-sized cisplatin, and stir well. Pour into the mold, cool slowly at room temperature, and make 5mm square particles. Pulverize into a particle size of 0.1-0.5 mm in a pulverizer, mix with coolant liquid nitrogen, add to a vibrating mill for fine pulverization, and keep the temperature below 0°C. Sieve, select particles with a particle size of 30-100 microns and bottle them for later use. All operations were carried out unde...
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