CN1307983C - Mai-an dripping pill for treating hyperlipoproteinemia and its preparing method - Google Patents

Mai-an dripping pill for treating hyperlipoproteinemia and its preparing method Download PDF

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Publication number
CN1307983C
CN1307983C CNB2005100515386A CN200510051538A CN1307983C CN 1307983 C CN1307983 C CN 1307983C CN B2005100515386 A CNB2005100515386 A CN B2005100515386A CN 200510051538 A CN200510051538 A CN 200510051538A CN 1307983 C CN1307983 C CN 1307983C
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polyethylene glycol
substrate
mixed
drug extract
matrix
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CN1682933A (en
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曲韵智
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Beijing Chia Tai Green Continent Pharmaceutical Co Ltd
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Beijing Chia Tai Green Continent Pharmaceutical Co Ltd
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Abstract

The present invention relates to a medical composition for treating disease symptoms, such as hyperlipoproteinemia, etc., particularly an oral preparation as a medical composition prepared from northern crataegus as a traditional Chinese medicine and malt as raw materials together with a medicinal carrier as a substrate. The medical composition performs the action of serum cholesterol reduction. The present invention aims to overcome the disadvantages of the existing oral medical preparation for treating hyperlipoproteinemia and provide a Mai-a dripping pill having the advantages of high bioavailability, quick medicine release, quick effect taking, high medicine contents, convenient administration, low price and no pollution in production. The Mai-a dripping pill related by the present invention is prepared from the northern crataegus as the traditional Chinese medicine and the malt as raw materials together with the medicinal carrier as the substrate.

Description

A kind of arteries and veins quieting drip pill for the treatment of hyperlipoproteinemia and preparation method thereof
Technical field
The present invention relates to a kind of serum cholesterol of reduction effect that has, the pharmaceutical composition that is used for the treatment of diseases such as hyperlipoproteinemia, being particularly related to Chinese medicine Fructus Crataegi, Fructus Hordei Germinatus is raw material, a kind of drug composition oral preparation that is prepared from the pharmaceutically suitable carrier as substrate.
Background technology
Pacify electuary according to the arteries and veins that the preparation method that provides among the drug standard WS3-B-0115-89 promulgated by the ministries or commissions of the Central Government is prepared from, it is a kind of reduction serum cholesterol that has, prevent atherosclerosis, to triglyceride reducing, beta lipoprotein also has certain effect, is used for the treatment of the oral granular formulation of diseases such as hyperlipoproteinemia, through clinical verification, determined curative effect is the common drug that clinical and family is used for the treatment of this type of disease.Below be prescription and technology and the brief description that provides among the drug standard WS3-B-0115-89:
Prescription: Fructus Crataegi 100g, Fructus Hordei Germinatus 100g
Method for making: above two flavors, Fructus Crataegi is smashed to pieces with Fructus Hordei Germinatus and is decocted with water secondary, and each 1 hour, collecting decoction filtered, and filtrate is concentrated into the clear paste that relative density is 1.30 (80 ℃), and it is an amount of to add ethanol, stirs evenly.1 part of qinghuo reagent, 2 parts of cane sugar powders, 1.2 parts in dextrin is made granule, and drying is sieved, promptly.
Function cures mainly; The treatment hyperlipoproteinemia.Be used to reduce serum cholesterol, prevent atherosclerosis, to triglyceride reducing, beta lipoprotein also has certain effect.
Owing to reasons such as technologies of preparing, the oral formulations of most drug, especially the oral formulations of Chinese medicine, exist all after taking that dissolve scattered time limit is long, dissolution is low, absorption is relatively poor, problem such as liver sausage first pass effect and bioavailability are lower, thereby influence the performance of drug effect, also directly affect therapeutic effect.Granule also has medicament contg also lower, takes deficiencies such as inconvenience.
In addition, conventional peroral dosage form is as tablet, capsule, granule (electuary) etc., in preparation process because the technology of granulation is arranged, therefore can produce bigger dust pollution, can staff's health be worked the mischief to a certain extent, also can cause certain pollution simultaneously to environment.Moreover, the complex manufacturing of conventional oral formulations, production cost is higher, thereby patient's drug cost is also improved thereupon, is unfavorable for improving the ability of seeking medical advice of extensive patients, also is unfavorable for improving the general health level of society.
Summary of the invention
Purpose of the present invention is to replenish the existing deficiency that is used for the treatment of the oral drug preparation of hyperlipoproteinemia, and a kind of bioavailability height is provided, and has a quick release, produce effects fast, medicament contg height, taking convenience, cheap, and free of contamination aborning arteries and veins quieting drip pill.Arteries and veins quieting drip pill involved in the present invention is a raw material with Chinese medicine Fructus Crataegi, Fructus Hordei Germinatus, after extraction obtains containing the extract of pharmaceutically active ingredient in above 2 flavors, is prepared from the pharmaceutically suitable carrier as substrate again.Be prepared by the following technical solutions, can obtain arteries and veins quieting drip pill involved in the present invention:
[preparation method]
1. the preparation of drug extract: with g or kg is unit, according to the weight portion meter; get 1 part of Fructus Crataegi, 1 part in Fructus Hordei Germinatus; above two flavors, Fructus Crataegi is smashed to pieces with Fructus Hordei Germinatus and is decocted with water secondary, each 1 hour; collecting decoction; filter, and filtrate is 1.25~1.35 thick paste being condensed into relative density below 80 ℃, promptly; Or, be ground into dry powder, promptly continuing to make drying below 80 ℃;
2. substrate: Polyethylene Glycol (1000~20000), one or more the mixture in pharmaceutically suitable carrier such as polyoxyethylene stearate 40 esters, betacyclodextrin, poloxamer, carboxymethyl starch sodium, sodium lauryl sulphate, stearic acid, sodium stearate, glycerin gelatine, Lac;
3. proportioning: with g or kg is unit, by weight, and drug extract: substrate=1: 1~1: 9;
4. according to the given ratio of prescription, accurately take by weighing drug extract and substrate, be placed on heating while stirring in the heating container, standby until the fused solution that obtains containing drug extract and substrate and/or emulsion and/or suspension;
5. adopt homemade or general drop pill machine (as the TZDW-1 type drop pill machine of Changzheng Tianmin High Science ﹠ Technology Co., Ltd., Beijing's production), and the temperature control system of adjustment drop pill machine, make the water dropper temperature heating of drop pill machine and remain on (50~90) ℃, the temperature cooling of condensing agent also remains on (40~-5) ℃;
6. when treating that the temperature of condensing agent in dropping-pill machine head and the condensation column is stable respectively and reaching desired state of temperature, fused solution and/or the emulsion and/or the suspension that will contain drug extract and substrate, place in the water dropper jar of drop pill machine, splash in the condensing agent, condensing agent can be any one in liquid paraffin, methyl-silicone oil, the vegetable oil;
7. will shrink the drop pill taking-up of molding by the outlet of drop pill machine, remove the surface condensation agent, be drying to obtain.
Beneficial effect
Pacify electuary according to the arteries and veins that the preparation method that provides among the drug standard WS3-B-0115-89 promulgated by the ministries or commissions of the Central Government is prepared from, it is a kind of reduction serum cholesterol that has, prevent atherosclerosis, to triglyceride reducing, beta lipoprotein also has certain effect, is used for the treatment of the oral granular formulation of diseases such as hyperlipoproteinemia, through clinical verification, determined curative effect is the common drug that clinical and family is used for the treatment of this type of disease.
Owing to reasons such as technologies of preparing, the oral formulations of most drug, especially the oral formulations of Chinese medicine, exist all after taking that dissolve scattered time limit is long, dissolution is low, absorption is relatively poor, problem such as liver sausage first pass effect and bioavailability are lower, thereby influence the performance of drug effect, also directly affect therapeutic effect.Granule also has medicament contg also lower, takes deficiencies such as inconvenience.
In addition, conventional peroral dosage form is as tablet, capsule, granule (electuary) etc., in preparation process because the technology of granulation is arranged, therefore can produce bigger dust pollution, can staff's health be worked the mischief to a certain extent, also can cause certain pollution simultaneously to environment.Moreover, the complex manufacturing of conventional oral formulations, production cost is higher, thereby patient's drug cost is also improved thereupon, is unfavorable for improving the ability of seeking medical advice of extensive patients, also is unfavorable for improving the general health level of society.
Arteries and veins quieting drip pill involved in the present invention is compared with arteries and veins peace electuary has following beneficial effect:
1. arteries and veins quieting drip pill involved in the present invention; utilize surfactant to be substrate; the extract of pharmaceutically active ingredient is made solid dispersion in containing Fructus Crataegi, Fructus Hordei Germinatus 2 flavors, makes medicine be molecule, colloid or microcrystalline state and is scattered in the substrate, and the total surface area of medicine increases; and substrate is hydrophilic; medicine is had wetting action, can make that medicine is rapidly molten to loose into microgranule or solution, thereby make the dissolving of medicine and absorb and accelerate; thereby improved bioavailability, brought into play efficient, quick-acting effects etc.
2. arteries and veins quieting drip pill involved in the present invention, contact promptly with saliva and to dissolve rapidly, and absorb by oral mucosa, not only rapid-action, and the influence of not taken food, promptly all can containing take after meal ante cibum, can not produce any residual harmful substance at gastric yet, thereby make that patient's medication is safer, also have medication convenience, characteristic of accurate simultaneously.
3. arteries and veins quieting drip pill involved in the present invention mixes the extract that contains active constituents of medicine mutually with molten matrix, splashes in the not miscible condensed fluid and makes.Therefore, the stability of drug height, not facile hydrolysis, oxidation, and the operation be under liquid state, to carry out, no dust pollution is not subject to the influence of crystal formation, thereby has guaranteed the quality of medicine, has increased stability.
4. production technology, the equipment of preparation drop pill are simple, easy to operate, the automaticity height, and labor intensity is low, the production efficiency height.Workshop does not have dust simultaneously, helps labor protection and environmental protection yet.
5. the production cost of preparation drop pill is usually with about 50% of other oral formulations of kind, and compares with oral liquid, and the dosage of drop pill is accurate, thereby makes the patient take metering control easily.
The specific embodiment
Now with several groups of specific embodiments, be described further with regard to the preparation method of arteries and veins quieting drip pill of the present invention:
First group: the test of single-matrix
1. raw material: it is standby to make drug extract dry powder earlier according to preparation method 1;
2. substrate: Polyethylene Glycol (1000,2000,4000,6000,8000,10000,20000), polyoxyethylene stearate 40 esters, betacyclodextrin, poloxamer, carboxymethyl starch sodium, sodium lauryl sulphate, stearic acid, sodium stearate, glycerin gelatine, Lac etc.;
3. proportioning: with g or kg is unit, by weight, and drug extract: substrate=1: 1~1: 9;
4. the process that provides according to [preparation method] 4~7 is prepared, and can obtain the arteries and veins quieting drip pill of different size.
[result of the test]
Test 1: for observe drug extract and different substrates when 1: 1 the proportioning prepared arteries and veins quieting drip pill in qualitative difference, according to 1: 1 ratio, with drug extract respectively with Polyethylene Glycol 1000, Polyethylene Glycol 2000, Polyethylene Glycol 4000, Polyethylene Glycol 6000, Polyethylene Glycol 8000, Polyethylene Glycol 10000, Polyethylene Glycol 20000, pharmaceutically suitable carrier such as polyoxyethylene stearate 40 esters, betacyclodextrin, poloxamer, carboxymethyl starch sodium, sodium lauryl sulphate, stearic acid, sodium stearate, glycerin gelatine, Lac matches, be prepared according to the step of stipulating in the preparation method, can obtain 16 pharmaceutical compositions experiments that contain drug extract and different substrates, and obtain 16 groups of different experimental results and see Table 1.
Test 2: for observe drug extract and different substrates when 1: 3 the proportioning prepared arteries and veins quieting drip pill in qualitative difference, according to 1: 3 ratio, with drug extract respectively with Polyethylene Glycol 1000, Polyethylene Glycol 2000, Polyethylene Glycol 4000, Polyethylene Glycol 6000, Polyethylene Glycol 8000, Polyethylene Glycol 10000, Polyethylene Glycol 20000, pharmaceutically suitable carrier such as polyoxyethylene stearate 40 esters, betacyclodextrin, poloxamer, carboxymethyl starch sodium, sodium lauryl sulphate, stearic acid, sodium stearate, glycerin gelatine, Lac matches, be prepared according to the step of stipulating in the preparation method, can obtain 16 pharmaceutical compositions experiments that contain drug extract and different substrates, and obtain 16 groups of different experimental results and see Table 2.
Test 3: for observe drug extract and different substrates when 1: 9 the proportioning prepared arteries and veins quieting drip pill in qualitative difference, according to 1: 9 ratio, with drug extract respectively with Polyethylene Glycol 1000, Polyethylene Glycol 2000, Polyethylene Glycol 4000, Polyethylene Glycol 6000, Polyethylene Glycol 8000, Polyethylene Glycol 10000, Polyethylene Glycol 20000, pharmaceutically suitable carrier such as polyoxyethylene stearate 40 esters, betacyclodextrin, poloxamer, carboxymethyl starch sodium, sodium lauryl sulphate, stearic acid, sodium stearate, glycerin gelatine, Lac matches, be prepared according to the step of stipulating in the preparation method, can obtain 16 pharmaceutical compositions experiments that contain drug extract and different substrates, and obtain 16 groups of different experimental results and see Table 3.
Second group: the test of mixed-matrix
1. raw material: it is standby to make drug extract dry powder earlier according to preparation method 1;
2. substrate:
2.1 Polyethylene Glycol---English name Macrogol,
2.2 polyoxyethylene stearate 40 esters---English name Polyoxyl (40) Stearate,
Molecular formula is with C 17H 35COO (CH 2CH 2O) nH represents that n is about 40,
2.3 poloxamer---English name Poloxamer, polyoxyethylene poly-oxygen propylene aether,
Molecular formula HO (C 2H 4O) a(C 3H 6O) b(C 2H 4O) cH,
The sodium salt of the starch carboxymethyl ester that 2.4 carboxymethyl starch sodium---English name Carboxymethylstach Sodium, starch generates with the monoxone effect under alkali condition,
2.5 betacyclodextrin---English name Betacyclodextrin, molecular formula C 6H 10O 5, this product is that ring dextrin glucosyl transferase acts on 7 glucoses that starch generates with α-1, the bonded cyclic oligosaccharide of 4-glycosidic bond;
3. proportioning: with g or kg is unit, by weight, and drug extract: substrate=1: 1~1: 9;
4. the process that provides according to [preparation method] 4~7 is prepared, and can obtain the arteries and veins quieting drip pill of different size.
[result of the test]
Test 4: in order to observe the mass discrepancy of drug extract and mixed-matrix prepared arteries and veins quieting drip pill when 1: 1 the proportioning, with polyoxyethylene stearate 40 esters, poloxamer, carboxymethyl starch sodium, 4 kinds of carriers such as betacyclodextrin respectively with Polyethylene Glycol with 1: 1 mixed evenly as mixed-matrix, according to 1: 1 ratio different with the 4 kinds respectively mixing matrix phases of drug extract are mixed again and make evenly, be prepared according to the step of stipulating in the preparation method, can obtain the experiment of 4 pharmaceutical compositions that drug extract and mixed-matrix constituted, and obtain 4 groups of different experimental results and see Table 4.
Test 5: in order to observe the mass discrepancy of drug extract and mixed-matrix prepared arteries and veins quieting drip pill when 1: 3 the proportioning, with polyoxyethylene stearate 40 esters, poloxamer, carboxymethyl starch sodium, 4 kinds of carriers such as betacyclodextrin respectively with Polyethylene Glycol with 1: 1 mixed evenly as mixed-matrix, according to 1: 3 ratio different with the 4 kinds respectively mixing matrix phases of drug extract are mixed again and make evenly, be prepared according to the step of stipulating in the preparation method, can obtain the experiment of 4 pharmaceutical compositions that drug extract and mixed-matrix constituted, and obtain 4 groups of different experimental results and see Table 5.
Test 6: in order to observe the mass discrepancy of drug extract and mixed-matrix prepared arteries and veins quieting drip pill when 1: 9 the proportioning, with polyoxyethylene stearate 40 esters, poloxamer, carboxymethyl starch sodium, 4 kinds of carriers such as betacyclodextrin respectively with Polyethylene Glycol with 1: 1 mixed evenly as mixed-matrix, according to 1: 9 ratio different with the 4 kinds respectively mixing matrix phases of drug extract are mixed again and make evenly, be prepared according to the step of stipulating in the preparation method, can obtain the experiment of 4 pharmaceutical compositions that drug extract and mixed-matrix constituted, and obtain 4 groups of different experimental results and see Table 6.
Test 7: in order to observe the mass discrepancy of drug extract and mixed-matrix prepared arteries and veins quieting drip pill when 1: 1 the proportioning, with polyoxyethylene stearate 40 esters, poloxamer, carboxymethyl starch sodium, 4 kinds of carriers such as betacyclodextrin respectively with Polyethylene Glycol with 1: 5 mixed evenly as mixed-matrix, according to 1: 1 ratio different with the 4 kinds respectively mixing matrix phases of drug extract are mixed again and make evenly, be prepared according to the step of stipulating in the preparation method, can obtain the experiment of 4 pharmaceutical compositions that drug extract and mixed-matrix constituted, and obtain 4 groups of different experimental results and see Table 7.
Test 8: in order to observe the mass discrepancy of drug extract and mixed-matrix prepared arteries and veins quieting drip pill when 1: 3 the proportioning, with polyoxyethylene stearate 40 esters, poloxamer, carboxymethyl starch sodium, 4 kinds of carriers such as betacyclodextrin respectively with Polyethylene Glycol with 1: 5 mixed evenly as mixed-matrix, according to 1: 3 ratio different with the 4 kinds respectively mixing matrix phases of drug extract are mixed again and make evenly, be prepared according to the step of stipulating in the preparation method, can obtain the experiment of 4 pharmaceutical compositions that drug extract and mixed-matrix constituted, and obtain 4 groups of different experimental results and see Table 8.
Test 9: in order to observe the mass discrepancy of drug extract and mixed-matrix prepared arteries and veins quieting drip pill when 1: 9 the proportioning, with polyoxyethylene stearate 40 esters, poloxamer, carboxymethyl starch sodium, 4 kinds of carriers such as betacyclodextrin respectively with Polyethylene Glycol with 1: 5 mixed evenly as mixed-matrix, according to 1: 9 ratio different with the 4 kinds respectively mixing matrix phases of drug extract are mixed again and make evenly, be prepared according to the step of stipulating in the preparation method, can obtain the experiment of 4 pharmaceutical compositions that drug extract and mixed-matrix constituted, and obtain 4 groups of different experimental results and see Table 9.
Test 10: in order to observe the mass discrepancy of drug extract and mixed-matrix obtained arteries and veins quieting drip pill when 1: 1 proportioning, with polyoxyethylene stearate 40 esters, poloxamer, carboxymethyl starch sodium, 4 kinds of carriers such as betacyclodextrin respectively with Polyethylene Glycol with 1: 10 mixed evenly as mixed-matrix, according to 1: 1 ratio drug extract is mixed mutually with 4 kinds of different mixed-matrixes respectively again and make evenly, be prepared according to the step of stipulating in the preparation method, can obtain the experiment of 4 pharmaceutical compositions that drug extract and mixed-matrix constituted, and obtain 4 groups of different experimental results and see Table 10.
Test 11: in order to observe the mass discrepancy of drug extract and mixed-matrix obtained arteries and veins quieting drip pill when 1: 3 proportioning, with polyoxyethylene stearate 40 esters, poloxamer, carboxymethyl starch sodium, 4 kinds of carriers such as betacyclodextrin respectively with Polyethylene Glycol with 1: 10 mixed evenly as mixed-matrix, according to 1: 3 ratio drug extract is mixed mutually with 4 kinds of different mixed-matrixes respectively again and make evenly, be prepared according to the step of stipulating in the preparation method, can obtain the experiment of 4 pharmaceutical compositions that drug extract and mixed-matrix constituted, and obtain 4 groups of different experimental results and see Table 11.
Test 12: in order to observe the mass discrepancy of drug extract and mixed-matrix obtained arteries and veins quieting drip pill when 1: 9 proportioning, with polyoxyethylene stearate 40 esters, poloxamer, carboxymethyl starch sodium, 4 kinds of carriers such as betacyclodextrin respectively with Polyethylene Glycol with 1: 10 mixed evenly as mixed-matrix, according to 1: 9 ratio drug extract is mixed mutually with 4 kinds of different mixed-matrixes respectively again and make evenly, be prepared according to the step of stipulating in the preparation method, can obtain the experiment of 4 pharmaceutical compositions that drug extract and mixed-matrix constituted, and obtain 4 groups of different experimental results and see Table 12.
The group practices of table 1 drug extract and single-matrix
(drug extract: substrate=1: 1)
The substrate title Effective ingredient (%) Rounding rate (%) Dissolve scattered time limit (minute) The ball method of double differences different (%) Hardness
Polyethylene Glycol 1000 50.0 56 <30 >10 +
Polyethylene Glycol 2000 50.0 64 <30 >10 +
Polyethylene Glycol 4000 50.0 75 <30 >10 ++
Polyethylene Glycol 6000 50.0 73 <30 >10 ++
Polyethylene Glycol 8000 50.0 76 <30 >10 ++
Polyethylene Glycol 10000 50.0 78 <30 >10 ++
Polyethylene Glycol 20000 50.0 78 <30 >10 ++
Polyoxyethylene stearate 40 esters 50.0 73 <30 >10 ++
Betacyclodextrin 50.0 69 <30 >10 +
Poloxamer 50.0 75 <30 >10 ++
Carboxymethyl starch sodium 50.0 73 <30 >10 +
Sodium lauryl sulphate 50.0 68 >30 >10 ++
Stearic acid 50.0 55 >30 >10 ++
Sodium stearate 50.0 55 >30 >10 ++
Glycerin gelatine 50.0 57 >30 >10 +
Lac 50.0 56 >30 >10 +
The group practices of table 2 drug extract and single-matrix
(drug extract: substrate=1: 3)
The substrate title Effective ingredient (%) Rounding rate (%) Dissolve scattered time limit (minute) The ball method of double differences different (%) Hardness
Polyethylene Glycol 1000 25.0 64 <30 >10 +
Polyethylene Glycol 2000 25.0 85 <30 >10 ++
Polyethylene Glycol 4000 25.0 87 <30 <10 +++
Polyethylene Glycol 6000 25.0 91 <30 <10 +++
Polyethylene Glycol 8000 25.0 92 <30 <10 +++
Polyethylene Glycol 10000 25.0 90 <30 <10 +++
Polyethylene Glycol 20000 25.0 92 <30 <10 +++
Polyoxyethylene stearate 40 esters 25.0 90 <30 <10 ++
Betacyclodextrin 25.0 82 <30 >10 ++
Poloxamer 25.0 92 <30 <10 +++
Carboxymethyl starch sodium 25.0 87 <30 <10 +++
Sodium lauryl sulphate 25.0 83 <30 >10 ++
Stearic acid 25.0 78 >30 >10 +++
Sodium stearate 25.0 79 >30 >10 +++
Glycerin gelatine 25.0 73 >30 >10 +++
Lac 25.0 76 >30 >10 +++
The group practices of table 3 drug extract and single-matrix
(drug extract: substrate=1: 9)
The substrate title Effective ingredient (%) Rounding rate (%) Dissolve scattered time limit (minute) The ball method of double differences different (%) Hardness
Polyethylene Glycol 1000 10.0 68 <30 >10 +
Polyethylene Glycol 2000 10.0 84 <30 >10 ++
Polyethylene Glycol 4000 10.0 89 <30 <10 +++
Polyethylene Glycol 6000 10.0 92 <30 <10 +++
Polyethylene Glycol 8000 10.0 91 <30 <10 +++
Polyethylene Glycol 10000 10.0 92 <30 <10 +++
Polyethylene Glycol 20000 10.0 93 <30 <10 +++
Polyoxyethylene stearate 40 esters 10.0 93 <30 <10 ++
Betacyclodextrin 10.0 88 <30 <10 ++
Poloxamer 10.0 92 <30 <10 +++
Carboxymethyl starch sodium 10.0 90 <30 <10 +++
Sodium lauryl sulphate 10.0 80 <30 >10 +++
Stearic acid 10.0 82 >30 >10 +++
Sodium stearate 10.0 82 >30 >10 +++
Glycerin gelatine 10.0 78 >30 >10 +++
Lac 10.0 80 >30 >10 +++
The group practices of table 4 drug extract and mixed-matrix
(drug extract: mixed-matrix=1: 1)
The substrate title Effective ingredient (%) Rounding rate (%) Dissolve scattered time limit (minute) The ball method of double differences different (%) Hardness
Polyoxyethylene stearate 40 esters: Polyethylene Glycol=1: 1 50 83 <30 >10 ++
Poloxamer: Polyethylene Glycol=1: 1 50 82 <30 >10 ++
Carboxymethyl starch sodium: Polyethylene Glycol=1: 1 50 80 <30 >10 ++
Betacyclodextrin: Polyethylene Glycol=1: 1 50 72 <30 >10 +
The group practices of table 5 drug extract and mixed-matrix
(drug extract: mixed-matrix=1: 3)
The substrate title Effective ingredient (%) Rounding rate (%) Dissolve scattered time limit (minute) The ball method of double differences different (%) Hardness
Polyoxyethylene stearate 40 esters: Polyethylene Glycol=1: 1 25 87 <30 <10 +++
Poloxamer: Polyethylene Glycol=1: 1 25 89 <30 <10 +++
Carboxymethyl starch sodium: Polyethylene Glycol=1: 1 25 86 <30 <10 +++
Betacyclodextrin: Polyethylene Glycol=1: 1 25 84 <30 >10 ++
The group practices of table 6 drug extract and mixed-matrix
(drug extract: mixed-matrix=1: 9)
The substrate title Effective ingredient (%) Rounding rate (%) Dissolve scattered time limit (minute) The ball method of double differences different (%) Hardness
Polyoxyethylene stearate 40 esters: Polyethylene Glycol=1: 1 10 88 <30 <10 +++
Poloxamer: Polyethylene Glycol=1: 1 10 86 <30 <10 +++
Carboxymethyl starch sodium: Polyethylene Glycol=1: 1 10 83 <30 >10 +++
Betacyclodextrin: Polyethylene Glycol=1: 1 10 82 <30 >10 +++
The group practices of table 7 drug extract and mixed-matrix
(drug extract: mixed-matrix=1: 1)
The substrate title Effective ingredient (%) Rounding rate (%) Dissolve scattered time limit (minute) The ball method of double differences different (%) Hardness
Polyoxyethylene stearate 40 esters: Polyethylene Glycol=1: 5 50 90 <30 <10 +++
Poloxamer: Polyethylene Glycol=1: 5 50 90 <30 <10 +++
Carboxymethyl starch sodium: Polyethylene Glycol=1: 5 50 90 <30 <10 +++
Betacyclodextrin: Polyethylene Glycol=1: 5 50 87 <30 <10 ++
The group practices of table 8 drug extract and mixed-matrix
(drug extract: mixed-matrix=1: 3)
The substrate title Effective ingredient (%) Rounding rate (%) Dissolve scattered time limit (minute) The ball method of double differences different (%) Hardness
Polyoxyethylene stearate 40 esters: Polyethylene Glycol=1: 5 25 93 <30 <10 +++
Poloxamer: Polyethylene Glycol=1: 5 25 92 <30 <10 +++
Carboxymethyl starch sodium: Polyethylene Glycol=1: 5 25 91 <30 <10 +++
Betacyclodextrin: Polyethylene Glycol=1: 5 25 88 <30 <10 +++
The group practices of table 9 drug extract and mixed-matrix
(drug extract: mixed-matrix=1: 9)
The substrate title Effective ingredient (%) Rounding rate (%) Dissolve scattered time limit (minute) The ball method of double differences different (%) Hardness
Polyoxyethylene stearate 40 esters: Polyethylene Glycol=1: 5 10 93 <30 <10 +++
Poloxamer: Polyethylene Glycol=1: 5 10 92 <30 <10 +++
Carboxymethyl starch sodium: Polyethylene Glycol=1: 5 10 92 <30 <10 +++
Betacyclodextrin: Polyethylene Glycol=1: 5 10 90 <30 <10 +++
The group practices of table 10 drug extract and mixed-matrix
(drug extract: mixed-matrix=1: 1)
The substrate title Effective ingredient (%) Rounding rate (%) Dissolve scattered time limit (minute) The ball method of double differences different (%) Hardness
Polyoxyethylene stearate 40 esters: Polyethylene Glycol=1: 10 50 92 <30 <10 +++
Poloxamer: Polyethylene Glycol=1: 10 50 91 <30 <10 +++
Carboxymethyl starch sodium: Polyethylene Glycol=1: 10 50 87 <30 <10 +++
Betacyclodextrin: Polyethylene Glycol=1: 10 50 86 <30 >10 +++
The group practices of table 11 drug extract and mixed-matrix
(drug extract: mixed-matrix=1: 3)
The substrate title Effective ingredient (%) Rounding rate (%) Dissolve scattered time limit (minute) The ball method of double differences different (%) Hardness
Polyoxyethylene stearate 40 esters: Polyethylene Glycol=1: 10 25 92 <30 <10 +++
Poloxamer: Polyethylene Glycol=1: 10 25 92 <30 <10 +++
Carboxymethyl starch sodium: Polyethylene Glycol=1: 10 25 89 <30 <10 +++
Betacyclodextrin: Polyethylene Glycol=1: 10 25 87 <30 <10 +++
The group practices of table 12 drug extract and mixed-matrix
(drug extract: mixed-matrix=1: 9)
The substrate title Effective ingredient (%) Rounding rate (%) Dissolve scattered time limit (minute) The ball method of double differences different (%) Hardness
Polyoxyethylene stearate 40 esters: Polyethylene Glycol=1: 10 10 91 <30 <10 +++
Poloxamer: Polyethylene Glycol=1: 10 10 92 <30 <10 +++
Carboxymethyl starch sodium: Polyethylene Glycol=1: 10 10 90 <30 <10 +++
Betacyclodextrin: Polyethylene Glycol=1: 10 10 91 <30 <10 +++
1. can be seen by the result in the table: when the ratio of drug extract and substrate was 1: 1, its rounding rate, the ball method of double differences was different and index such as hardness is all undesirable, and dissolve scattered time limit influenced not obvious.
2. when the ratio of drug extract and substrate is 1: 3, the rounding rate, the ball method of double differences is different and index such as hardness slightly all begins to enter preferable state.
3. when the ratio of drug extract and substrate is 1: 9, the rounding rate, the ball method of double differences is different and index such as hardness improves not obvious.
4. the general effect of composite interstitial substance is better than single-matrix.
5. the hardness method for expressing in the subordinate list adopts drop pill is placed on the glass plate, press...withes one's finger it, observes its metamorphosis."+" expression flicking promptly is out of shape, " ++ " expression distortion of firmly pressing, and " +++" expression is indeformable by it.

Claims (2)

1. an arteries and veins quieting drip pill that is used for the treatment of hyperlipoproteinemia is a raw material with Fructus Crataegi, Fructus Hordei Germinatus, is prepared from the pharmaceutically suitable carrier as substrate, it is characterized in that:
(1) according to the weight portion meter, get 1 part of Fructus Crataegi, 1 part in Fructus Hordei Germinatus, more than two flavors, Fructus Crataegi is smashed to pieces with Fructus Hordei Germinatus and is decocted with water secondary, each 1 hour, collecting decoction filtered, filtrate is 1.25~1.35 thick paste being condensed into relative density below 80 ℃; Or, be ground into dry powder continuing to make drying below 80 ℃, and promptly get the extract that contains pharmaceutically active ingredient in above-mentioned 2 flavors, standby;
(2) described substrate is the mixture of Polyethylene Glycol and polyoxyethylene stearate 40 esters or carboxymethyl starch sodium, and the mixed proportion of polyoxyethylene stearate 40 esters or carboxymethyl starch sodium and Polyethylene Glycol is 1: 1~1: 10, and the ratio of described extract and substrate is 1: 3;
(3) according to aforementioned proportion, accurately take by weighing described extract and substrate, be placed in the heating container heating while stirring, standby until the fused solution that obtains containing described extract and substrate and/or emulsion and/or suspension;
(4) temperature control system of adjustment drop pill machine makes the water dropper heating of drop pill machine and maintains the temperature at 50 ℃~90 ℃, and the condensing agent cooling also maintains the temperature at 40 ℃~-5 ℃;
When (5) treating that dropping-pill machine head and condensing agent reach described state of temperature, will contain fused solution and/or the emulsion and/or the suspension of described extract and substrate, place in the water dropper jar of drop pill machine, splash in the condensing agent, shrink molding promptly.
2. arteries and veins quieting drip pill as claimed in claim 1 is characterized in that: described condensing agent be methyl-silicone oil or/and liquid paraffin or/and vegetable oil.
CNB2005100515386A 2005-03-04 2005-03-04 Mai-an dripping pill for treating hyperlipoproteinemia and its preparing method Expired - Fee Related CN1307983C (en)

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CN105477459A (en) * 2015-11-24 2016-04-13 梧州神冠蛋白肠衣有限公司 Maian granules and preparation method thereof

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CN1436527A (en) * 2002-02-07 2003-08-20 王志刚 Glimepiride dripping pills
CN1546027A (en) * 2003-12-02 2004-11-17 北京正大绿洲医药科技有限公司 Dripping pills for treating allergic disease and its preparation process
CN1546141A (en) * 2003-12-12 2004-11-17 北京科信必成医药科技发展有限公司 Blumea oil dripping pills and its preparation process

Patent Citations (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN1436527A (en) * 2002-02-07 2003-08-20 王志刚 Glimepiride dripping pills
CN1546027A (en) * 2003-12-02 2004-11-17 北京正大绿洲医药科技有限公司 Dripping pills for treating allergic disease and its preparation process
CN1546141A (en) * 2003-12-12 2004-11-17 北京科信必成医药科技发展有限公司 Blumea oil dripping pills and its preparation process

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