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Liposome combination drugs, industrial production process of liposome combination drug through molecular dispersion method, and quality control

A liposome and composition technology, which is applied in the field of large-scale industrial production of liposome combination drug preparation, can solve the problems of increasing leakage rate, batch fluctuation, energy consumption and time-consuming, etc. The effect of saving workshop

Inactive Publication Date: 2013-12-18
蔡海德
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Problems solved by technology

High-pressure homogenization method and ultrasonic method can control the particle size, but high-energy crushing will damage the raw material medicine; the latter four methods cannot control the particle size, and the particle size distribution is not concentrated, organic solvent residues, leakage, precipitation, coagulation, Quality problems such as phospholipid corruption;
[0005] 3. The existing liposome preparation method makes the encapsulation efficiency of the liposome-combined drug carrier not reach 85%, and each batch fluctuates and changes greatly; the leakage rate is large, and the significance of the liposome-combined drug is lost;
[0006] 4. The production process is troublesome, energy-consuming and time-consuming, equipment investment is large, the prescription and process are not reliable and immature, resulting in uncontrollable, unstable and poor reproducibility of the preparation quality;
[0007] 5. Improper methods of sterilization and depyrogenation, it is difficult to guarantee aseptic and pyrogen-free operation in the whole process, and the lack of a high degree of sterility concept for liposome combination drugs, resulting in the corruption of liposome combination drugs under bacterial erosion, and the encapsulation rate decreases , the leakage rate is increasing, the validity period is extremely short, and the medicinal value is almost lost;
[0008] 6. The number and size of insoluble particles in the injection exceed the standard;
[0009] 7. Most raw materials, phospholipids, excipients, and solvents are selected without national drug quality standards, and new drug certificates and production approval documents cannot be approved even if they have patents. Registration is very difficult and takes a long time;
[0010] 8. Breaking away from the real situation in China, it took nearly 10 years and more than 20 million yuan from the development to the approval of liposome new drug production. Even the best drug invention patents, most companies dare not invest in development

Method used

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  • Liposome combination drugs, industrial production process of liposome combination drug through molecular dispersion method, and quality control
  • Liposome combination drugs, industrial production process of liposome combination drug through molecular dispersion method, and quality control
  • Liposome combination drugs, industrial production process of liposome combination drug through molecular dispersion method, and quality control

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Experimental program
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Effect test

Embodiment 1

[0051] The raw material drug is a liposome combination drug with strong fat solubility. The molar ratio of each raw material component of the standard is as follows:

[0052]

[0053] 9. Water for injection, when it is dry, it will be evaporated to the utmost, and it will be equal to three parts of the volume of phosphate buffer for injection

[0054] The preparation steps and method are carried out according to the preparation steps and method of the liposome combination drug of the strong fat-soluble bulk drug described above.

Embodiment 2

[0056] The raw material drug is a liposome combination drug with strong fat solubility. The molar ratio of each raw material component of the standard is as follows:

[0057]

[0058]

[0059] 9. Water for injection, volatile to the maximum when dry, equal volume to phosphate buffer for injection

[0060] The preparation steps and method are carried out according to the preparation steps and method of the liposome combination drug of the strong fat-soluble bulk drug described above.

Embodiment 3

[0062] The raw material drug is a liposome combination drug with strong fat solubility. The molar ratio of each raw material component of the standard is as follows:

[0063]

[0064] 9. Water for injection, volatile to the maximum when dry, equal volume to phosphate buffer for injection

[0065] The preparation steps and method are carried out according to the preparation steps and method of the liposome combination drug of the strong fat-soluble bulk drug described above.

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Abstract

According to the invention, a liposome combination drug injection and an oral liposome combination drug preparation can be produced in a large industrialization manner through a molecular dispersion method with a unified formula, a unified process and unified equipment. The invention provides a formula of raw components for preparing liposome combination drugs in a molar ratio, provides freeze-drying injection and oral preparation processes for the prepared liposome combination drugs, and also provides twenty embodiments for preparing the liposome combination drugs, such as an anti-gastric-ulcer liposome combination drug, antibacterial and antifungal liposome combination drugs, an anti-tumor liposome combination drug, an anti-virus liposome combination drug, an anti-emetic liposome combination drug, a nutritional supplement liposome combination drug and hypoglycemic agent and cardiovascular medicine liposome combination drugs.

Description

technical field [0001] The invention relates to a method for preparing a liposome combination medicine in large-scale industrial production. Production of oral formulations of liposomal combination drugs. The implementation process is: excipient dissolution ultrafiltration-excipient spray drying-phospholipid and drug molecule dispersion coating-phospholipid and drug solid dispersion system hydration granulation-nano 1m particle size liposome drug body dispersion system freeze-drying to produce lipid Plastid Combination Drugs. Background technique [0002] The gap between my country's pharmaceutical technology and raw material drug preparation technology and the international advanced level is only within 5 years, and some have reached or exceeded the international advanced level, and the preparation technology is 10-20 years behind the international advanced level. At present, a large number of second-generation common preparations are produced, while third-generation sust...

Claims

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Application Information

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Patent Type & Authority Applications(China)
IPC IPC(8): A61K9/127A61K47/24A61K47/18A61K47/02A61K47/10A61K47/28A61K31/5575A61P1/04A61P31/04A61P31/10A61P35/00A61P31/12A61P1/08A61P3/02A61P3/10A61P9/00A61P9/10
Inventor 蔡海德蔡欣蔡强
Owner 蔡海德
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