Lornoxicam microsphere and preparation method thereof
A technology of lornoxicam and microspheres, which is applied in the direction of pharmaceutical formulations, medical preparations with non-active ingredients, medical preparations containing active ingredients, etc., and can solve problems such as toxic side effects, short half-life of drugs, and increased pain for patients , to achieve the effect of increasing drug concentration, reducing toxic and side effects, and strong and lasting effect
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Embodiment 1
[0023] Embodiment 1: the preparation of lornoxicam microsphere
[0024] Dissolve 80mg of polylactic acid-glycolic acid copolymer in 2mL of dichloromethane to form an organic phase with a concentration of 40mg / mL; suspend 4mg of sustained-release drug in 0.4mL of distilled water to form an inner water phase, and then add the inner water phase dropwise to In the organic phase, shear at high speed for 1 min to obtain colostrum; then use a syringe to inject colostrum into 10 mL of the outer aqueous phase gelatin solution (concentration 40 g / L), shear at high speed for 2 min to obtain W / O / W double emulsion, and stir After 3 hours, the dichloromethane was completely volatilized; centrifuged, discarded the upper liquid, washed 3 to 5 times with distilled water to obtain microspheres, and dried in vacuum for 72 hours to obtain dry powder of lornoxicam microspheres. Wherein, the high-speed shearing speed is 12000r / min.
Embodiment 2
[0025] Embodiment 2: the preparation of lornoxicam microsphere
[0026] Dissolve 80mg of polylactic acid-glycolic acid copolymer in 2mL of dichloromethane to form an organic phase with a concentration of 40mg / mL; suspend 4mg of sustained-release drug in 0.4mL of distilled water to form an inner water phase, and then add the inner water phase dropwise to In the organic phase, shear at high speed for 1 min to obtain colostrum; then use a syringe to inject colostrum into 10 mL of the external aqueous phase polyvinyl alcohol solution (concentration 40 g / L), and shear at high speed for 2 min to obtain W / O / W double emulsion. Stir for 4 hours to completely volatilize the dichloromethane; centrifuge, discard the upper liquid, wash with distilled water for 3 to 5 times to obtain microspheres, and vacuum dry for 90 hours to obtain dry powder of lornoxicam microspheres. Wherein, the high-speed shearing speed is 16000r / min.
Embodiment 3
[0027] Embodiment 3: the preparation of lornoxicam microsphere
[0028] Dissolve 20 mg of polylactic acid-glycolic acid copolymer in 2 mL of dichloromethane to form an organic phase with a concentration of 10 mg / mL; suspend 2 mg of sustained-release drug in 0.4 mL of distilled water to form an inner water phase, and then add the inner water phase dropwise to In the organic phase, high-speed shearing is performed for 5 seconds to obtain colostrum; then the colostrum is injected into 20 mL of gelatin solution (concentration: 20 g / L) with a syringe, and high-speed shearing is performed for 1 min to obtain W / O / W double emulsion, which is then stirred for 2 hours. Completely volatilize the dichloromethane; centrifuge, discard the upper liquid, wash with distilled water for 3 to 5 times to obtain microspheres, and vacuum dry for 48 hours to obtain dry powder of lornoxicam microspheres. Wherein, the high-speed shearing speed is 8000r / min.
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