TREA

Butylphtualide Soft Gel Capsule and Its Preperation Procedure

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Information

  • Patent Application
  • 20080020034
  • Publication Number
    20080020034
  • Date Filed
    December 03, 2004
    20 years ago
  • Date Published
    January 24, 2008
    16 years ago
Information
Abstract
The present invention discloses a novel dosage form of butylphthalide soft capsule and its preparation procedure. Butylphthalide soft capsule is composed of a coating material and a drug-containing oil. The drug-containing oil is basically composed of butylphthalide and diluent—vegetable oil, wherein the weight ratio of butylphthalide to oil ranges from 1:0-10. The coating material is composed of gelatin, plasticizer and water, wherein the weight ratio of gelatin to plasticizer to water is in the range of 1:0.2{tilde over ( )}0.4:0.8{tilde over ( )}0.3. The butylphthalide soft capsule described in this invention can mask the strong and specific flavor of butylphthalide, and overcome the difficulties associated with formulating oily active agents into other oral preparations. The disintegration time of the soft capsule complies with the requirement of Pharmacopoeia of P.R. China.
Description
MODES OF CARRYING OUT THE INVENTION

In this invention, butylphthalide soft gel capsule is comprised of capsule materials and drug-containing oil, in which the drug-containing oil is comprised basically of butylphthalide and diluent vegetable oil. A relatively better weight ratio of butylphthalide to diluent vegetable oil ranges from 1:1 to 1:8 (w/w). The further better selected weight ratio of butylphthalide to diluent vegetable oil ranges from 1:2 to 1:5 (w/w). In the best mode, the weight ratio of butylphthalide to diluent vegetable oil is 1:3.5 (w/w). Dibutyl carboxyl methylbenzene (dibutyl carboxyl toluene) as an antioxidant with the amount of 0 to 0.2% (weight ratio) can be further added to drug-containing oil.


A better choice of vegetable oil can be selected from a group of oils consisting of peanut oil, soybean oil, corn oil, and sesame oil. The best mode choice of oil is soybean oil.


Capsule materials are basically comprised of gel, plasticizer and water. Among them, the best mode choice of gel is gelatin, the best mode choice of plasticizer is glycerol.


The following implemented experiments are given to further describe the technical scheme of this invention better. The foregoing description is intended to illustrate and not limit the scope of the invention.


Experiment 1
Preparation of Butylphthalide Soft Gel Capsules

Preparation of Gelatin Liquid:


Gelatin 100 grams, glycerol 30 grams, water 130 grams and 200 mg ethyl p-hydroxybenzoate.


Took gelatin and add certain amount of water, let gelatin absorb water and expend. Meanwhile, put glycerol, ethyl p-hydroxybenzoate, and the rest of the water into a colloidal sol pot, heated them to the temperature of 70 to 80 degree C., mixed them well, then added the water absorbed and expended gelatin into the pot and stirred them thoroughly till they were melted. Kept the temperature of the pot stable for 1 to 2 hours, kept the gel liquid in the pot stable and let it settle down so that the air bubbles in the gel liquid floated to the surface of it. Scraped the bubbles off the gel liquid surface. Used a piece of clean white cloth filtering the gel liquid. Kept the gel liquid temperature stable and waited for its further use. The viscosity of the gelatin liquid is usually 2.8 to 3.2 degree.


Preparation of Drug-Containing Oil:


Weighed butylphthalide 100 grams, stirred it thoroughly and mixed it well with clear soybean oil 350 grams. The drug-containing oil was ready for use.


Press Preparation of Soft Gel Capsules:


Took prepared gelatin glycerol liquid and butylphthalide drug-containing oil and put each of them into automatic rotary molding capsule presser, controlled its working temperature at 40 to 50 degree C., pressed and produced butylphthalide soft gel capsules, each of them contains 450 mg of drug-containing oil.


The soft gel capsules press produced according to Experiment 1 method and contained Experiment 1 ratio of drug-containing oil, were in proper outside measurement sizes. The quality test result revealed that they contained uniformly distributed amount of drug-containing oil in each of the capsule. The detailed results were as follows:















Sample


















Capsule 1
Capsule 2
Capsule 3
Capsule 4
Capsule 5
Capsule 6
Capsule 7
Capsule 8
Capsule 9
Capsule 10





















Content
99.12
98.08
100.02
99.47
99.32
101.38
98.65
98.76
99.25
98.47


(%)








Range of
98.08-101.38


Content


(%)


Standard
0.93


Deviation


(%)









Experiment 2
Preparation of Butylphthalide Soft Gel Capsules

All the rest preparing steps were the same as the steps in Example 1, except that during the preparation of drug-containing liquid steps we did not add any vegetable oil, therefore the final press produced soft gel capsules contained 100 mg drug-containing liquid in each of the capsule.


Experiment 3
Preparation of Butylphthalide Soft Gel Capsules

Preparation of Gelatin Liquid:


gelatin 100 grams, glycerol 40 grams, water 120 grams and 200 mg ethyl p-hydroxybenzoate. The rest preparation steps were the same as in Experiment 1.


Preparation of Drug-Containing Oil:


Weighed butylphthalide 225 grams, stirred it thoroughly and mixed it well with clear peanut oil 225 grams. The drug-containing oil was ready for use.


Press Preparation of Soft Gel Capsules:


All the rest preparing steps were the same as the steps in above mentioned other Experiments, except that the final press produced soft gel capsules contained 200 mg drug-containing oil in each of the capsule.


The soft gel capsules press produced according to Experiment 3 method and contained Experiment 3 ratio of drug-containing oil, were tested. The test results were as follows:















Sample


















Capsule 1
Capsule 2
Capsule 3
Capsule 4
Capsule 5
Capsule 6
Capsule 7
Capsule 8
Capsule 9
Capsule 10





















Content
98.33
96.08
99.42
101.73
94.37
100.31
92.65
98.79
102.01
95.78


(%)








Range of
92.65-102.01


Content


(%)


Standard
3.14


Deviation


(%)









Experiment 4
Preparation of Butylphthalide Soft Gel Capsules

All the rest preparing steps were the same as the steps in Experiment 1, except during the preparation of drug-containing oil steps we weighed butylphthalide 56.25 grams, stirred it thoroughly and mixed it well with clear peanut oil 393.75 grams, therefore the final press produced soft gel capsules contained 800 mg drug-containing oil in each of the capsule.


The soft gel capsules pressed according to Experiment 4 method and contained Experiment 4 ratio of drug-containing oil, were tested.


The test results are as follows:















Sample


















Capsule 1
Capsule 2
Capsule 3
Capsule 4
Capsule 5
Capsule 6
Capsule 7
Capsule 8
Capsule 9
Capsule 10





















Content
100.03
99.08
99.42
101.73
98.57
100.31
99.55
98.99
100.11
99.98


(%)








Range of
98.57-101.73


Content


(%)


Standard
0.88


Deviation


(%)









Experiment 5
Preparation of Butylphthalide Soft Gel Capsules

Preparation of Gelatin Liquid:


Gelatin 100 grams, glycerol 20 grams, water 80 grams and 200 mg ethyl p-hydroxybenzoate. The rest preparation steps were the same as in Experiment 1.


Preparation of Drug-Containing Oil:


Weighed butylphthalide 45 grams, stirred it thoroughly and mixed it well with clear peanut oil 405 grams. The drug-containing oil is ready for use.


Press Preparation of Soft Gel Capsules:


All the rest preparing steps were the same as the steps in above mentioned Experiments, except that the final press produced soft gel capsules contained 1000 mg drug-containing oil in each of the capsule.


Experiment 6
Preparation of Butylphthalide Soft Gel Capsules

All the rest preparing steps were the same as the steps in Experiment 1, except that during the preparation of drug-containing oil steps we weighed butylphthalide 90 grams, stirred it thoroughly and mixed it well with clear soybean oil 360 grams, therefore the final press produced soft gel capsules contained 500 mg drug-containing oil in each of the capsule.


Experiment 7
Preparation of Butylphthalide Soft Gel Capsules

All the rest preparing steps were the same as the steps in Experiment 1, except that during the preparation of drug-containing oil steps we weighed butylphthalide 40.91 grams, stirred it thoroughly and mixed it well with clear soybean oil 490.09 grams, therefore the final press produced soft gel capsules contain 1100 mg drug-containing oil in each of the capsule.


Experiment 8
Preparation of Butylphthalide Soft Gel Capsules

All the rest preparing steps were the same as the steps in Experiment 1, except that during the preparation of drug-containing oil steps we weighed butylphthalide 50 grams, stirred it thoroughly and mixed it well with clear soybean oil 400 grams, therefore the final press produced soft gel capsules contained 900 mg drug-containing oil in each of the capsule.


Experiment 9
Preparation of Butylphthalide Soft Gel Capsules

All the rest preparing steps were the same as the steps in Experiment 1, except that during the preparation of drug-containing oil steps we weighed butylphthalide 150 grams, stirred it thoroughly and mixed it well with clear soybean oil 300 grams and antioxidant ethyl p-hydroxybenzoate 0.45 grams, therefore the final press produced soft gel capsules contained 300.3 mg drug-containing oil in each of the capsule.


Experiment 10
Butylphthalide Content, Relevant Materials and Disintegrating Time Limit Assay

Assay Method


Disintegrating Time Limit Assay


Disintegrating time limit assay was performed according to Chinese Pharmacopoeia, Edition 2000, Part Two, Appendix VA's Disintegrating Time Limit Assay.


Took samples from Experiment 1, used diluted hydrochloric acid (9→1000) 1,000 ml as solvent, set testing temperature at 37 degree C.+/−1 degree C., set speed of raising and submerging the capsule at 30 to 32 times per minute, added baffle while testing, and observed the total disintegrating time of each soft gel capsule. The result indicated that the disintegrating time was less than 1 hour, which pass the standard of Chinese Pharmacopoeia.


Relevant Materials


Relevant materials were tested according to Chinese Pharmacopoeia, Edition 2000, Part Two, Appendix VD's HPLC (High Performance Liquid Chromatography) Assay.


Assay Method


Took adequate amount of content from this product, added proper amount chloroform until it was dissolved. Added methanol up to constant volume, diluted and prepared it with methanol until its concentration was 0.5 mg per 1 ml. This was the test solution.


Weighed butylphthalide adequate amount as assay control accurately, added methanol until it was dissolved, diluted and prepared it with methanol to the concentration of 15 micro gram (μg) butylphthalide per 1 ml. This was the assay control solution.


Measured assay control solution 20 micro liter (μl) accurately, ejected it into HPLC, tested it according to HPLC menu, adjusted the sensitivity of HPLC until the major composition peak measurement was 10 to 20% of the total measurement.


Measured test solution 20 micro liter (μl) accurately, tested it the same way as testing the assay control solution on HPLC. Recorded chromatogram up to two folds of the retention time of the chromatographic measurement of the major composition peak. If impurity peaks were existed on the chromatogram, calculated the areas of every impurity peak (except the solvent peak), and the total areas of the impurity peaks should be no larger than the area of the assay control solution peak.


Content Assay


Content was tested according to Chinese Pharmacopoeia, Edition 2000, Part Two, Appendix VD's HPLC (High Performance Liquid Chromatography) Assay.


Testing of Chromatographic Condition and System Serviceability


Employed octadecyl silane bonded silica gel as filling, methanol-water (65:35) as flow phase, set flow rate at 1.0 ml per minute, assay wave length at 280 nm, theoretical board calculated the number of butylphthalide peaks should be no less than 1500. Butylphthalide versus impurity separation levels should be within the standard.


Control Solution Preparation


Took butylphthalide control sample about 50 mg, weighed it accurately, put it into a 50 ml graduated flask, added methanol solution to dissolve it and diluted it up to the graduated mark, mixed the solution thoroughly. Accurately measured 5 ml solution from the flask and transferred it to another 50 ml graduated flask, diluted it with methanol up to the graduated mark. This was control solution.


Assay Solution Preparation


Took adequate amount of butylphthalide content from the packages under the stock packaging difference (equivalent to about butylphthalide 50 mg), weighed it accurately, put it into a 50 ml graduated flask, added proper amount chloroform to dissolve it and proper amount of methanol to dilute it up to the graduated mark, stirred and mixed the solution thoroughly. Accurately measured 5 ml solution from the flask and transferred it to another 50 ml graduated flask, diluted it with methanol up to the graduated mark. This was test solution.


Assay Method


Measured control solution 20 micro liter (μl) and test solution 20 micro liter (μl) accurately, ejected both of them into HPLC respectively, tested them according to HPLC menu, and recorded their chromatograms respectively. Calculated the peak areas of butylphthalide (C12H14O2) content according to external standard method, recorded the data.


The experiment data as follows:
















Observation


Relevant



Condition

Content
Substance
Disintegration












Environment
Time
Appearance
(%)
(%)
Time















Initial
 0 Day
Yellow transparent soft gel capsule
98.8
0.61
 4′50″


Accelerated
 1 month
Yellow transparent soft gel capsule
98.7
0.66
 6′45″


Experiment
 2 month
Yellow transparent soft gel capsule
99.3
0.63
14′10″



 3 month
Yellow transparent soft gel capsule
98.4
0.62
28′30″



 6 month
Yellow transparent soft gel capsule
99.0
0.58
49′52″


Room
 1 month
Yellow transparent soft gel capsule
98.6
0.63
 5′15″


Temperature
 3 month
Yellow transparent soft gel capsule
98.8
0.67
 8′35″


Control
 6 month
Yellow transparent soft gel capsule
99.4
0.66
 9′45″


Sample
12 month
Yellow transparent soft gel capsule
99.1
0.62
17′50″



18 month
Yellow transparent soft gel capsule
98.5
0.64
27′25″



24 month
Yellow transparent soft gel capsule
98.5
0.65
29′35″









Most soft gel capsule dosage forms suffer from the problem of product disqualification due to disintegrating time limit when the capsules pass extended shelf storage time. Even though, the test results of accelerated assay and long term assay of the present product indicate that the soft gel capsule shell ages fast and disintegrating time changes more obviously under the heated condition, the disintegrating time is less than 60 minutes. These test results meet the standard of Chinese Pharmacopoeia, Edition 2000. All the indexes of appearance, content, relevant materials of the soft gel capsule have passed the standard levels, and the product's quality is guaranteed up to 2 years.

Claims
  • 1. A butylphthalide soft gel capsule characterized by a composition comprising capsule materials and pharmaceutical components in drug-containing oil form, wherein the pharmaceutical components in drug-containing oil comprising substantially butylphthalide and vegetable oil with the weight ratio in between 1:0 and 1:10.
  • 2. The butylphthalide soft gel capsule according to claim 1, wherein the characterized weight ratio between butylphthalide and vegetable oil ranges from 1:1 to 1:8.
  • 3. The butylphthalide soft gel capsule according to claim 2, wherein the characterized weight ratio of said butylphthalide and said vegetable oil ranges from 1:2 to 1:5.
  • 4. The butylphthalide soft gel capsule according to claim 3, wherein the characterized weight ratio between butylphthalide and vegetable oil is 1:3.5.
  • 5. The butylphthalide soft gel capsule according to claim 1, wherein the characterized vegetable oil is selected from the group consisting of sesame oil, corn oil, peanut oil, soybean oil, almond oil, peach kernel oil, cottonseed oil, sunflower seed oil, olive oil, or their mixture.
  • 6. The butylphthalide soft gel capsule according to claim 1, wherein the characterized butylphthalide includes the optically inactive, mixed L and D forms of butylphthalide, levorotatory optical isomer of butylphthalide, dextrorotatory optical isomer of butylphthalide.
  • 7. The butylphthalide soft gel capsule according to claim 1, wherein the characterized drug-containing oil further includes dibutyl carboxyl methyl benzene (dibutyl carboxyl toluene) as antioxidant with 0 to 0.2% weight ratio in respect to drug-containing oil.
  • 8. The butylphthalide soft gel capsule according to claim 1, wherein the characterized capsule materials includes the basic components of gel, plasticizer and water with the weight ratio of 1:0.2 to 0.4:0.8 to 1.3.
  • 9. The butylphthalide soft gel capsule according to claim 8, wherein the characterized gel is selected from the group consisting of gelatin or acacia gum (Gum Arabic), or a mixture of gelatin and acacia gum.
  • 10. The butylphthalide soft gel capsule according to claim 8, wherein the characterized plasticizer is selected from the group consisting of glycerol (glycerin) or sorbitol (sorbierite), or a mixture of glycerol and sorbitol.
  • 11. The butylphthalide soft gel capsule according to claim 8, wherein the characterized capsule materials further includes antiseptic agents.
Priority Claims (1)
Number Date Country Kind
200310119336.1 Dec 2003 CN national
PCT Information
Filing Document Filing Date Country Kind 371c Date
PCT/CN04/01411 12/3/2004 WO 00 9/12/2007