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Novel paclitaxel emulsion for intravenous injection and its preparation method

A technology of paclitaxel emulsion and oil for injection, applied in the field of medicine, can solve the problems of unknown clinical prospects, liposome stability is greatly affected by temperature, low solubility, etc., and achieves simple and easy preparation process and good bioavailability. , the effect of preventing intermediate pollution

Inactive Publication Date: 2005-07-06
重庆华立药业股份有限公司
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Problems solved by technology

[0003] The solubility of paclitaxel in water is very small, almost insoluble in water (<0.004mg / ml), and the bioavailability of oral administration is poor, so it can only be administered by intravenous injection
The solubility of paclitaxel in commonly used injection oils is also very small, and the current clinical commonly used paclitaxel preparation is an oil preparation (Cremophor® EL) made by mixing polyoxyethylene castor oil and absolute ethanol 1:1, that is, paclitaxel Cremophor preparation. Before the medicine is diluted to the administration concentration with normal saline or 5% glucose solution, ethanol has greater irritation during injection, and polyoxyethylene castor oil has side effects, which can cause severe allergic reactions, and patients need antiallergic precautions before injection. The whole process is extremely inconvenient. In addition, Cremophor preparations tend to form precipitates after dilution, which affects the absorption and utilization of paclitaxel.
A variety of new formulations of paclitaxel have been reported. For example, Bissery et al. used ethanol, Tween-80, polypropylene glycol, etc. as paclitaxel co-solubilizers, diluted with glucose solution before administration, and used for intravenous infusion of paclitaxel (Bissery MC , et al., Cancer Res, 1991,51:4845), but the ethanol and Tween-80 and other irritating substances are contained in the co-solubilized substance, and Tween-80 has a certain hemolytic effect and has a relatively large adverse reaction, and After this dilution, it is extremely unstable, and paclitaxel is easy to separate out; Pan Linlin et al. adopt mixed surfactant and mixed solvent to solubilize paclitaxel, and have prepared paclitaxel injection (Pan Linlin et al., Journal of Shenyang Pharmaceutical University, 2004, 21 (2): 101-104), the injection needs to be diluted with normal saline or glucose injection before injection, and sometimes flocculation and particle precipitation will occur. Clinical outlook unknown
Shama A, Zhang Jingqing, Wei Fengying, Zhang Changying, etc. have done research on paclitaxel liposomes (Sharma A, et al.Int JCancer, 1997, 71 (1): 103; Zhang Jingqing, West China Pharmaceutical Journal, 2001, 16 (1) : 23; etc.), the stability of liposomes is greatly affected by temperature, and the storage time is short. Due to the large particle size of liposomes, its main target sites are liver and spleen, and the distribution of other parts is very low. The efficacy of some tumors can not meet the requirements; Csethati prepared a variety of paclitaxel coatings with various cyclodextrins (Cserhati T, et al., J PharmBiomed Anal, 1995, 13: 533-541.), but cyclodextrins have relatively Large allergic reactions and hemolysis, large adverse reactions limit the wide application of paclitaxel cyclodextrin coating; Kan et al. prepared paclitaxel O / w emulsion with non-ionic surfactant and phospholipid (Kan P, et al. , Controlled Release, 1999, 58:271-278), but the emulsion contains Tween-80, and the patient has hemolysis after intravenous injection, which has a relatively large adverse reaction; Zhang Yuru et al. dissolve paclitaxel, phospholipids and bile salts in In an organic solvent, the needle powder is made by freeze-drying (Zhang Hairu et al., CN1148957, 1997). When in use, directly add 5% glucose or 0.9% sodium chloride injection to dissolve and inject it intravenously, but paclitaxel is easy to separate out when diluted
In short, including other preparations such as microemulsions, proliposomes, topical administration, etc., because there are certain problems in terms of encapsulation efficiency, stability, side effects, bioavailability or convenience of administration, and paclitaxel As with Cremophor preparations, satisfactory results cannot be obtained

Method used

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Examples

Experimental program
Comparison scheme
Effect test

Embodiment 1

[0026] Example 1 Preparation of Paclitaxel Emulsion Containing 0.01% Paclitaxel

[0027] Weigh 100 mg of paclitaxel, 50 g of linseed oil, 1 g of soybean lecithin and 0.1 g of tocopherol, heat in a water bath to 75°C, stir and dissolve to obtain an oil phase. Measure 960 ml of water for injection, add 22.5 g of glycerin, heat to 75°C and stir to dissolve to obtain an aqueous phase. Mix the oil phase and the water phase at a temperature of 75°C, emulsify with a shear emulsification mixer (model RJ-300-1, manufactured by Shanghai Standard Model Factory) for 50 minutes (rotating speed 800 rpm), and mix the oil phase and the water phase . Use sodium hydroxide solution (0.1mol) to adjust its pH to 8.5 to obtain colostrum. The colostrum was homogenized and emulsified (pressure 10,000 psi, temperature 75°C) with a micro-jet high-pressure homogenizer (model M-110EH, manufactured by Anpac Corporation, USA) three times, subpackaged, filled with nitrogen, sterilized by high-pressure ste...

Embodiment 2

[0028] Example 2 Preparation of Paclitaxel Emulsion Containing 0.1% Paclitaxel

[0029]Weigh 1.0 g of paclitaxel, 100 g of evening primrose oil, 12 g of egg yolk phospholipid and 1 g of tocopherol, heat in a water bath to 45° C., stir and dissolve to obtain an oil phase. Measure 870 ml of water for injection, add 22.5 g of glycerin, heat to 45°C and stir to dissolve to obtain an aqueous phase. The oil phase and the water phase were mixed at a temperature of 45°C, and emulsified with a shear emulsification mixer for 200 minutes (300 rpm), so that the oil phase and the water phase were evenly mixed. Use sodium hydroxide solution (0.1mol) to adjust its pH to 9.5 to obtain colostrum. The colostrum was homogenized and emulsified three times with a high-pressure micro-fluidic homogenizer (pressure 3000 psi, temperature 45° C.), subpackaged, filled with nitrogen, sterilized with high-pressure steam, and sterilized at 115° C. for 30 minutes to obtain 990 ml of paclitaxel emulsion. T...

Embodiment 3

[0030] Example 3 Preparation of Paclitaxel Emulsion Containing 0.08% Paclitaxel

[0031] Weigh 800 mg of paclitaxel, 150 g of caprylic acid glyceride, 12 g of soybean lecithin and 5.0 g of tocopherol, heat in a water bath to 75° C., stir and dissolve to obtain an oil phase. Measure 870 ml of water for injection, add 22 g of mannitol, heat to 75°C and stir to dissolve to obtain an aqueous phase. The oil phase and the water phase were mixed at a temperature of 75° C., stirred and emulsified for 40 minutes (rotating speed 2000 rpm), and the oil phase and the water phase were mixed evenly. Use sodium hydroxide solution (0.1mol) to adjust its pH to 8.0 to obtain colostrum. The colostrum was homogenized and emulsified (pressure 10,000 psi, temperature 75° C.) three times with a micro-jet high-pressure homogenizer, subpackaged, filled with nitrogen, sterilized with high-pressure steam, and sterilized at 115° C. for 30 minutes to obtain 1010 ml of paclitaxel emulsion. The average pa...

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PUM

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Abstract

Disclosed is a novel paclitaxel emulsion for intravenous injection and its preparation method which consists of, dissolving yew alcohol with an oil for injection and preparing emulsion from medicinal adjuvant such as right amount of emulsifying agent, mixing yew alcohol, oil for injection, emulsifying agent and anti-oxidant so as to obtain the oil phase, mixing water for injection and isotonic conditioning agent to obtain aqueous phase, mixing the oil phase with the aqueous phase for emulsifying, carrying out further emulsifying, stirring, high-pressure homogenizing to prepare yew emulsion meeting venous injection.

Description

technical field [0001] The invention relates to the technical field of medicine, in particular to a paclitaxel emulsion for intravenous injection prepared by dissolving an anticancer drug paclitaxel with an injection oil and using a suitable emulsifier and other pharmaceutical auxiliary materials and a preparation method thereof. Background technique [0002] Paclitaxel (trade name Taxol) is a highly effective anticancer drug extracted from Taxus brevidolia, Pacific yew. It is a complex diterpenoid compound with a molecular formula of C 47 h 51 NO 14 , the relative molecular mass is 853.9. Paclitaxel has good anticancer activity, and has good curative effect for treating ovarian cancer, breast cancer, colon cancer, non-small cell lung cancer, neck cancer and melanoma. [0003] The solubility of paclitaxel in water is very small, almost insoluble in water (<0.004mg / ml), and the bioavailability of oral administration is poor, so it can only be ...

Claims

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Application Information

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Patent Type & Authority Applications(China)
IPC IPC(8): A61K9/107A61K31/337A61P35/00
Inventor 陈建明陈海生黄尊动宣伟东李丽肖琴黄成安
Owner 重庆华立药业股份有限公司
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