CN1919246B - Traditional Chinese medicine for treating cardiovascular diseases - Google Patents

Traditional Chinese medicine for treating cardiovascular diseases Download PDF

Info

Publication number
CN1919246B
CN1919246B CN2005100148495A CN200510014849A CN1919246B CN 1919246 B CN1919246 B CN 1919246B CN 2005100148495 A CN2005100148495 A CN 2005100148495A CN 200510014849 A CN200510014849 A CN 200510014849A CN 1919246 B CN1919246 B CN 1919246B
Authority
CN
China
Prior art keywords
extract
tanshinone
salviae miltiorrhizae
radix salviae
chinese medicine
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Expired - Fee Related
Application number
CN2005100148495A
Other languages
Chinese (zh)
Other versions
CN1919246A (en
Inventor
叶正良
李旭
张文生
魏峰
李德坤
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Tasly Pharmaceutical Group Co Ltd
Original Assignee
Tianjin Tasly Pharmaceutical Co Ltd
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by Tianjin Tasly Pharmaceutical Co Ltd filed Critical Tianjin Tasly Pharmaceutical Co Ltd
Priority to CN2005100148495A priority Critical patent/CN1919246B/en
Publication of CN1919246A publication Critical patent/CN1919246A/en
Application granted granted Critical
Publication of CN1919246B publication Critical patent/CN1919246B/en
Expired - Fee Related legal-status Critical Current
Anticipated expiration legal-status Critical

Links

Landscapes

  • Medicines Containing Plant Substances (AREA)

Abstract

The invention discloses a Chinese medicinal composition for treating cardiovascular diseases, which comprises 2.5-12.0% of tanshinone extract containing tanshinone 55-85%, 57.0-90.0% of total savianolic acid extract containing total savianolic acid 70-98%, 2.5-25.0% of ginseng saponin extract containing total saponins 75-98%, and natural borneol or rosewood oil 2.5-15.0%. The composition has evident functions in resisting cerebral ischemia and myocardial ischemia, the curative effect is better than the application of single extract of tanshinone, total savianolic acid or ginseng saponin, thus providing a more effective and more convenient Chinese medicinal composition and preparation clinically.

Description

The Chinese medicine of treatment cardiovascular disease
Technical field
The present invention relates to a kind of Chinese medicine composition for the treatment of cardiovascular disease and preparation method thereof.
Background technology
According to China's Epidemiological study, though over nearly 50 years in the rural area or the city, the M ﹠ M of cardiovascular and cerebrovascular disease is all in rising trend.50~sixties, China's population cause of death central vessel disease and cerebrovascular occupied the five or six respectively, then rose to the two or three respectively later in 1975, and cardiovascular and cerebrovascular disease death person has accounted for first of whole disease cause of the death.China accounts for the percentage ratio of total dead population because of cardiovascular and cerebrovascular disease death person, rise to 42.6% of calendar year 2001 by 12.07% of nineteen fifty-seven, the person reaches 2,000,000 though die from the cardiovascular and cerebrovascular disease every year has the part patient to survive through rescue in addition, but majority stays deformity, can't take care of oneself, cause serious burden to relatives and society.Cardiovascular and cerebrovascular disease also is western countries crowd main causes of death.Infer that according to present existing epidemiologic data advancing of disease trend is: to the year two thousand twenty, the human diseases cause of the death puts in order will have great change, but coronary heart disease and apoplexy will be first and second of the human cause of the death.Till that time, estimate that global coronary heart disease death number will increase to 1,100 ten thousand from 6,300,000 of nineteen ninety; Apoplexy increases to 7,700,000 from 4,400,000.Blood circulation cause of the death formation will increase 59.6% in 30 years, and coronary heart disease and apoplexy increase 74.6% and 75% respectively.These data prove absolutely that cardiovascular and cerebrovascular disease is not only the principal disease of harm humans health, especially human " the No.1 killer " who causes death, disables at present and in following 20 years.
In the medicine of cardiovascular and cerebrovascular disease, the application of Chinese medicine and western medicine emphasizes particularly on different fields, and Chinese medicine also occupies the bigger market share with the little advantage of its side effect.In the Chinese patent medicine of present numerous treatment cardiovascular and cerebrovascular diseases, compound red sage root preparation occupies important position, is that the Chinese patent medicine of main active such as Radix Notoginseng total arasaponins, Radix Salviae Miltiorrhizae total phenolic acids, Radix Puerariae flavone, Herb Gynostemmae Pentaphylli total glycosides etc. also more and more is subject to people's attention in addition with effective site.The effect of the various effective ingredient in Chinese of treatment cardiovascular and cerebrovascular disease is had nothing in common with each other and is stressed, the great demand that has drug combination clinically, therefore, the compound red sage root preparation with the effective site preparation will have characteristics such as dosage is little, good effect, steady quality, broad market prospect.
Summary of the invention
The purpose of this invention is to provide the little Chinese medicine composition efficiently of a kind of amount.
Another object of the present invention provides the preparation method of said composition.
The present invention is implemented by following technical proposals.
Chinese medicine composition of the present invention comprises following component by weight percentage:
The tanshinone extract 2.5%~12.0% that contains 55%~85% TANSHINONES,
The Radix Salviae Miltiorrhizae total phenolic acids extract 57.0%~90.0% that contains 70%~98% Radix Salviae Miltiorrhizae total phenolic acids,
The ginsenoside extract 2.5%~25.0% that contains 75%~98% total saponins,
Natural Broneolum Syntheticum or Lignum Dalbergiae Odoriferae oil 2.5%~15.0%.
Chinese medicine composition of the present invention is preferably and comprises following component by weight percentage:
The tanshinone extract 3.0%~8.0% that contains 55%~85% TANSHINONES,
The Radix Salviae Miltiorrhizae total phenolic acids extract 72.0%~82.0% that contains 70%~98% Radix Salviae Miltiorrhizae total phenolic acids,
The ginsenoside extract 6.0%~15.0% that contains 75%~98% total saponins,
Natural Broneolum Syntheticum or Lignum Dalbergiae Odoriferae oil 4.0%~10.0%.
Chinese medicine composition of the present invention more preferably comprises following component by weight percentage:
The tanshinone extract 4% that contains 55%~85% TANSHINONES,
The Radix Salviae Miltiorrhizae total phenolic acids extract 76% that contains 70%~98% Radix Salviae Miltiorrhizae total phenolic acids,
The ginsenoside extract 13% that contains 75%~98% total saponins,
Natural Broneolum Syntheticum or Lignum Dalbergiae Odoriferae oil 7%.
The above-mentioned tanshinone extract that contains 55%~85% TANSHINONES, available following method obtains:
(1) CO 2Extraction: the Radix Salviae Miltiorrhizae of getting after the pulverizing drops into CO 2Extraction kettle in the extraction equipment after system's each several part all reaches design temperature, boosts to setting pressure with extraction kettle. 75%~95% alcoholic solution is added system by the flow of setting, with CO 2Mix back circulation in whole system and carry out dynamic extraction; The condition of extraction is extracting pressure 15MPa~25Mpa, 30 ℃~55 ℃ of extraction and separation temperatures, and separation temperature is lower than extraction temperature, ethanol flow 0.5mL/min~1.5mL/min; After extraction is finished, emit extracting solution, concentrate, vacuum drying gets tanshinone extract, and its total tanshinone content is more than 55%.Medical material residue after the extraction is standby.
(2) ethanol extract from water precipitation: the Radix Salviae Miltiorrhizae of getting salvia piece or pulverizing, add 85~95% soak with ethanol 2 hours, then 65~85 ℃ of following reflux, extract, 3 times, each quantity of solvent is 5 times of crude drug weight, each 0.5~1.5 hour extraction time, the medical material residue after the extraction is standby; Merge extractive liquid,, extracting solution is being evaporated to 1/35~1/45 of original volume below 50 ℃, get concentrated solution; The water that adds 2~4 times of volumes in the concentrated solution was placed 6~24 hours, filtered; Filtrate gets tanshinone extract in dry below 50 ℃, and its total tanshinone content is more than 55%.
Get above-mentioned tanshinone extract, use an amount of dissolve with ethanol, join in the saturated hydroxypropyl solution, 25~50 ℃ stir after, restir 0.5~2 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl beta~cyclodextrin.
The assay of total tanshinone (ultraviolet spectrophotometry) method is as follows in the above-mentioned tanshinone extract:
Instrument: Tianjin, island UV-250 spectrophotometer
The preparation of reference substance solution: getting tanshinone 10mg is 1,2,4,6 with the methanol compound concentration, the standard solution of 8ug/ml.
The preparation of standard curve: with the reagent corresponding is the blank absorbance of measuring at 268nm wavelength place, is vertical coordinate with the absorbance, and the concentration of tanshinone is abscissa, the drawing standard curve.
Algoscopy: get extract 20mg with methanol constant volume to 100ml, precision pipettes 5ml to 100ml standardize solution.Method working sample absorbance under the preparation of sighting target directrix curve calculates.
The above-mentioned preparation that contains the Radix Salviae Miltiorrhizae total phenolic acids extract of 70%~98% Radix Salviae Miltiorrhizae total phenolic acids, available following method obtains: get the medical material residue after the said extracted TANSHINONES, by the method preparation of embodiment one among Chinese patent application CN1459448A or the CN1384090A.Above-mentioned Radix Salviae Miltiorrhizae total phenolic acids assay and content of danshinolic acid B are measured referring to Chinese patent CN1600318A.
The above-mentioned ginsenoside extract that contains 75%~98% total saponins can obtain with following method: get the ginseng crude drug, pulverize, add 5~8 times of amounts of medical material weight, 50~90% ethanol, reflux or supersound extraction 2~3 times, merge extractive liquid; Extracting solution filters, and being concentrated into does not have the alcohol flavor, is dissolved in water, and filters; Macroporous resin column on the filtrate with the water flushing of 2~4 times of amount column volumes, is used 60~85% ethanol elutions of 2~4 column volumes then, collects ethanol elution, the eluent concentrating under reduced pressure, and drying promptly gets ginsenoside extract.
Above-mentioned macroporous resin is the macroporous resin of nonpolar or low pole, is preferably D101, AB-8 or ZTC type macroporous resin, and the best is an AB-8 type macroporous resin.
Above-mentioned Radix Ginseng total saponins content (in the ginsenoside Re) assay method is as follows:
1. instrument and reagent
1.1 instrument
Ultraviolet-uisible spectrophotometer.Chromatographic column.
1.2 standard substance, test sample and reagent
Standard substance: ginsenoside Re: Nat'l Pharmaceutical ﹠ Biological Products Control Institute
Test sample: ginsenoside extract
Reagent: AB-8 macroporous resin or G..D.X-101 macroporous resin (60~80 orders, Tianjin chemical reagent two factories)
The ethanol analytical pure
Vanillin solution takes by weighing the 5g vanillin, and the ice acetic acid dissolving also is settled to 100ml.
The perchloric acid analytical pure
The glacial acetic acid analytical pure
Ginsenoside Re's standard solution: precision takes by weighing ginsenoside Re's standard substance 0.0100g, and with dissolve with methanol and be settled to 10ml, promptly every milliliter contains ginsenoside Re 1.0mg.
2. experiment
2.1 sample treatment: get the 2mg ginsenoside extract, with certain water gaging dilution (being diluted to about 50ml).
2.2 column chromatography: make the chromatography pipe with the 10mL syringe, interior dress 4cm AB-8 macroporous resin is washed post with 20mL95% ethanol earlier, discards eluent, and reuse 25mL washes post, discards eluent.The accurate sample solution of having handled well (seeing 2.1) that adds, flow speed control is about 1mL/min.Earlier wash post with 15mL, discard eluent, reuse 20mL95% ethanol elution arasaponin is collected eluent in evaporating dish, places 75 ℃ of water-baths to volatilize.Doing colour developing with this uses.
2.3 the preparation of blank sample: in clean evaporating dish, accurately add 0.2mL5% vanillin glacial acetic acid solution, rotate evaporating dish, residue is all dissolved, add 0.8mL perchloric acid again, move into behind the mixing in the 10mL band plug graduated centrifuge tube; Add the 0.2mL glacial acetic acid in the evaporating dish again, rotate evaporating dish, make the residual liquid dissolving, move into again in the above-mentioned centrifuge tube, heat 10min in 60 ℃ of water-baths, take out, after the ice bath cooling, accurately add glacial acetic acid 5.0mL, after shaking up, promptly get blank sample.
2.4 colour developing: in the above-mentioned evaporating dish that has volatilized, accurately add 0.2mL5% vanillin glacial acetic acid solution, rotate evaporating dish, residue is all dissolved, add 0.8mL perchloric acid again, move into behind the mixing in the 10mL band plug graduated centrifuge tube; Add the 0.2mL glacial acetic acid in the evaporating dish again, rotate evaporating dish, make the residual liquid dissolving, move into again in the above-mentioned centrifuge tube, heat 10min in 60 ℃ of water-baths, take out, after the ice bath cooling, accurately add glacial acetic acid 5.0mL, after shaking up, carry out colorimetric determination (after with blank sample ultraviolet-uisible spectrophotometer being returned zero, measuring again) with standard pipe in 560nm wavelength place with the 1cm colorimetric pool.
2.5 standard pipe: draw ginsenoside Re's standard solution (1.0mg/mL) 0.1mL, with certain water gaging dilution (about 10ml), below operate from " A2.2 column chromatography ... " rise, identical with sample, measure absorbance.
3 calculate:
C sample=(A1 * C mark * 100)/(A2 * 6)
In the formula:
C sample: the amount of Radix Ginseng total saponins (in the ginsenoside Re) in the extract, mg/100mL
A1: the absorbance of test solution,
A 2: the absorbance of titer,
C Mark: the concentration of titer, mg/mL
Result of calculation keeps three position effective digitals.
Natural Broneolum Syntheticum in the above-mentioned Chinese medicine composition should meet the Chinese Pharmacopoeia standard.Natural Broneolum Syntheticum can replace with the Borneolum Syntheticum that meets the Chinese Pharmacopoeia standard.
Lignum Dalbergiae Odoriferae oil in the above-mentioned Chinese medicine composition is that the Lignum Dalbergiae Odoriferae medical material is through the distillation gained.
Chinese medicine composition of the present invention, the various dosage forms that can be mixed and made into adjuvant on any or more than one pharmaceuticss such as starch, dextrin, lactose, microcrystalline Cellulose, hydroxypropyl methylcellulose, Polyethylene Glycol, magnesium stearate, micropowder silica gel, xylitol, lactose, glucose, glycine, mannitol, glycine etc., for example, can be made into aqueous injection, tablet, slow releasing tablet, drop pill, granule, injectable powder, capsule, microgranule.Preferred dosage form is drop pill, injectable powder.
The preparation of Chinese medicine composition composition dropping pills of the present invention: get above-mentioned tanshinone extract, Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract and natural Broneolum Syntheticum (or Lignum Dalbergiae Odoriferae oil) to scale, Polyethylene Glycol-6000 or Polyethylene Glycol-4000 or both mixture mix homogeneously with 2~4 times of medicine gross weights, heating and melting, move in the dropping-pill machine jar after changing material, in medicine liquid droplet to 6~8 ℃ liquid paraffin or the methyl-silicone oil, oil removing, promptly.
The preparation of Chinese medicine composition injectable powder of the present invention: get above-mentioned tanshinone extract, Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract and natural Broneolum Syntheticum to scale, add an amount of adjuvant, the mixing postlyophilization, promptly.
Chinese medicine composition raw material sources of the present invention are easy to get, and are easy to industrialization; Can make various dosage forms as required, for clinical provide convenient, more effectively, the more controlled modern Chinese medicine of quality, for the patient brings more benefits, thereby produce the huge social benefit.
The present invention adopts rat experiment myocardial infarction model and external perfusion method, has compared the function of resisting myocardial ischemia of Chinese medicine composition of the present invention, tanshinone extract, Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract.The result shows that Chinese medicine composition of the present invention has tangible function of resisting myocardial ischemia, and its curative effect is better than using separately tanshinone extract, Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, shows that Chinese medicine composition of the present invention has stronger synergism.
The experimentation of several Chinese medicine extract function of resisting myocardial ischemia of experimental example
1, grouping and administration
70 of Wister male rats, body weight 250.8 ± 24.6 is divided into 7 groups at random by body weight: the normal saline matched group; The tanshinone extract group of embodiment one; The Radix Salviae Miltiorrhizae total phenolic acids extract group of experimental example one; The ginsenoside extract group of experimental example one; The Chinese medicine composition of embodiment one; The Chinese medicine composition of embodiment two.Each medicine all is diluted to desired concn with normal saline, and dosage is 4ml/kg, the tail intravenously administrable.
2, method
(1), rat experiment myocardial infarction model: animal pentobarbital sodium intraperitoneal injection of anesthesia (45mg/kg), it is fixing to face upward the position.Tracheal intubation is made the longitudinal incision of 2cm in breastbone left side, nearly breastbone side is cut off the 3rd, the 4th and reined in cartilage, open the thoracic cavity after, connect artificial respirator (ventilation 2ml/100g, 50 times/min).Cut off pericardium, expose heart, left anterior descending coronary artery root threading is in order to ligation, and record standard II lead electrocardiogram was stablized 10 minutes, and the ligation left anterior descending coronary artery is closed the thoracic cavity.With syringe sucking-off animal throat secretions, make animal recover autonomous respiration.Behind the ligation coronary artery 15min, intravenously administrable.Behind the ligation coronary artery 4 hours, win heart, 5 of the following crosscuts of ligature, carry out chlorination nitro blue tetrazolium (NBT) dyeing, calculating myocardium infarcted region area accounts for the percentage ratio of ventricle and heart area, and carries out statistical procedures (t check).
(2), stripped langendorff heart perfusion: carry out with reference to the pharmacological experimental methodology third edition.
3, result
(1), to the influence of rat experiment myocardial inyaretion scope, the results are shown in Table 1.
The various extracts of table 1 are to the influence of rat experiment myocardial inyaretion scope (x ± s)
Annotate: compare * P<0.05, * * P<0.01 with model group; Compare with the tanshinone extract group, #P<0.05, ##P<0.01; Compare with Radix Salviae Miltiorrhizae total phenolic acids extract group, ﹠amp;P<0.05, ﹠amp; ﹠amp;P<0.01; Compare with the ginsenoside extract group, @P<0.05, @@P<0.01
(2), to the influence of dirty coronary flow of guinea-pig heart and heart rate, the results are shown in Table 2.
The various extracts of table 2 are to the influence of dirty coronary flow of guinea-pig heart and heart rate (x ± s)
Figure G05114849520050906D000072
Annotate: compare * P<0.05, * * P<0.01 with the tanshinone extract group; Compare with Radix Salviae Miltiorrhizae total phenolic acids extract group,, #P<0.05, ##P<0.01; Compare with the ginsenoside extract group, ﹠amp;P<0.05, ﹠amp; ﹠amp;P<0.01.
The result of above table 1 and table 2 shows that each administration group all has tangible function of resisting myocardial ischemia, and the curative effect of active component composition of the present invention is best.
The specific embodiment
To be easier to understand the present invention with reference to the following example, and provide embodiment and be in order to illustrate the present invention, rather than in order to limit the scope of the invention.
Embodiment one
The preparation of tanshinone extract: the Radix Salviae Miltiorrhizae of getting after the pulverizing drops into CO 2Extraction kettle in the extraction equipment after system's each several part all reaches design temperature, boosts to setting pressure with extraction kettle.95% alcoholic solution is added system by the flow of setting, with CO 2Mix back circulation in whole system and carry out dynamic extraction; The condition of extraction is extracting pressure 20MPa, 45 ℃ of extraction temperature, 35 ℃ of separation temperatures, ethanol flow 1.0mL/min; After extraction is finished, emit extracting solution, concentrate, vacuum drying gets tanshinone extract, its total tanshinone content 64%.Medical material residue after the extraction is standby.
The preparation of Radix Salviae Miltiorrhizae total phenolic acids extract: get the medical material residue that extracts after the TANSHINONES, obtain by the preparation method of embodiment one among the Chinese patent application CN1459448A, its Radix Salviae Miltiorrhizae total phenolic acids content is 82.13%, and salvianolic acid B is 52.24%.
The preparation of ginsenoside extract: get the ginseng crude drug, pulverize, add 7 times of amounts of medical material weight, 70% ethanol, heating and refluxing extraction 2 times, merge extractive liquid; Extracting solution filters, and being concentrated into does not have the alcohol flavor, is dissolved in water, and filters; AB-8 type macroporous resin on the filtrate (production of Tianjin resin processing plant of Nankai University) post with the water flushing of 3 times of amount column volumes, is used 75% ethanol elution of 3 column volumes then, collects ethanol elution, the eluent concentrating under reduced pressure, and vacuum drying promptly gets ginsenoside extract.The Radix Ginseng total saponins content 82.3% of this ginsenoside extract.
Get above-mentioned tanshinone extract 0.3g, above-mentioned Radix Salviae Miltiorrhizae total phenolic acids extract 5.3g, above-mentioned ginsenoside extract 0.9g, natural Broneolum Syntheticum 0.5g, mix homogeneously, lyophilization gets Chinese medicine composition.
Embodiment two
The preparation of tanshinone extract: get the Radix Salviae Miltiorrhizae of salvia piece or pulverizing, add 95% soak with ethanol 2 hours, then 75 ℃ of following reflux, extract, 3 times, each quantity of solvent is 5 times of crude drug weight, and extraction time was respectively 60 minutes, 30 minutes and 30 minutes; Merge extractive liquid,, extracting solution is being evaporated to 1/40 of original volume below 50 ℃, get concentrated solution; Add the water of 3 times of volumes in the concentrated solution, placed 12 hours, filter; Filtrate gets tanshinone extract, its total tanshinone content 61% in dry below 50 ℃.Medical material residue after the extraction is standby.
The preparation of Radix Salviae Miltiorrhizae total phenolic acids extract: get the medical material residue that extracts after the TANSHINONES, obtain by the preparation method of embodiment one among the Chinese patent application CN1384090A, its Radix Salviae Miltiorrhizae total phenolic acids content is 80.35%, and salvianolic acid B is 51.33%.
The preparation of ginsenoside extract: get the ginseng crude drug, pulverize, add 6.5 times of amounts of medical material weight, 65% ethanol, supersound extraction 2 times, merge extractive liquid; Extracting solution filters, and being concentrated into does not have the alcohol flavor, is dissolved in water, and filters; D101 type macroporous resin on the filtrate (production of Tianjin resin processing plant of Nankai University) post with the water flushing of 3 times of amount column volumes, is used 75% ethanol elution of 3 column volumes then, collects ethanol elution, the eluent concentrating under reduced pressure, and lyophilization promptly gets ginsenoside extract.The Radix Ginseng total saponins content 81.9% of this ginsenoside extract.
Get above-mentioned tanshinone extract 0.3g, above-mentioned Radix Salviae Miltiorrhizae total phenolic acids extract 5.3g, above-mentioned ginsenoside extract 0.9g, Lignum Dalbergiae Odoriferae oil 0.5g add 9.0g Polyethylene Glycol-6000 mix homogeneously, and fusion gets Chinese medicine composition after the cooling.
Embodiment three
The preparation of tanshinone extract: the Radix Salviae Miltiorrhizae of getting after the pulverizing drops into CO 2Extraction kettle in the extraction equipment after system's each several part all reaches design temperature, boosts to setting pressure with extraction kettle. 90% alcoholic solution is added system by the flow of setting, with CO 2Mix back circulation in whole system and carry out dynamic extraction; The condition of extraction is extracting pressure 250MPa, 45 ℃ of extraction temperature, 35 ℃ of separation temperatures, ethanol flow 0.8mL/min; After extraction is finished, emit extracting solution, concentrate, vacuum drying gets tanshinone extract, its total tanshinone content 59%.Medical material residue after the extraction is standby.
The preparation of Radix Salviae Miltiorrhizae total phenolic acids extract: get the medical material residue that extracts after the TANSHINONES, obtain by the preparation method of embodiment one among the Chinese patent application CN1459448A, its Radix Salviae Miltiorrhizae total phenolic acids content is 81.97%, and salvianolic acid B is 52.56%.
The preparation of ginsenoside extract: get the ginseng crude drug, pulverize, add 7 times of amounts of medical material weight, 75% ethanol, heating and refluxing extraction 2 times, merge extractive liquid; Extracting solution filters, and being concentrated into does not have the alcohol flavor, is dissolved in water, and filters; ZTC type macroporous resin on the filtrate (production of Tianjin resin processing plant of Nankai University) post with the water flushing of 3 times of amount column volumes, is used 75% ethanol elution of 3 column volumes then, collects ethanol elution, the eluent concentrating under reduced pressure, and vacuum drying promptly gets ginsenoside extract.The Radix Ginseng total saponins content 82.6% of this ginsenoside extract.
Get above-mentioned tanshinone extract 0.3g, above-mentioned Radix Salviae Miltiorrhizae total phenolic acids extract 6.6g, above-mentioned ginsenoside extract 0.8g, natural Broneolum Syntheticum 0.5g, mix homogeneously, lyophilization gets Chinese medicine composition.
Embodiment four
Get the tanshinone extract 0.4g of embodiment one, ginsenoside extract 1.0g, the natural Broneolum Syntheticum 0.4g of Radix Salviae Miltiorrhizae total phenolic acids extract 5.3g, the embodiment two of embodiment one; An amount of dissolve with ethanol of tanshinone extract joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.The clathrate powder of tanshinone extract and hydroxypropyl and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, natural Broneolum Syntheticum mix homogeneously, lyophilization gets Chinese medicine composition.
Embodiment five
Get the tanshinone extract 0.3g of embodiment one, ginsenoside extract 0.8g, the natural Broneolum Syntheticum 0.5g of Radix Salviae Miltiorrhizae total phenolic acids extract 4.8g, the embodiment three of embodiment one; An amount of dissolve with ethanol of tanshinone extract joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.The clathrate powder of tanshinone extract and hydroxypropyl and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, natural Broneolum Syntheticum mix homogeneously, lyophilization gets Chinese medicine composition.
Embodiment six
Get the tanshinone extract 0.4g of embodiment one, ginsenoside extract 0.8g, the Lignum Dalbergiae Odoriferae oil 0.4g of Radix Salviae Miltiorrhizae total phenolic acids extract 8.5g, the embodiment two of embodiment one add 12.0g polyethylene glycol 6000 mix homogeneously, and fusion gets Chinese medicine composition after the cooling.
Embodiment seven
Get the tanshinone extract 0.3g of embodiment one, ginsenoside extract 0.9g, the natural Broneolum Syntheticum 0.5g of Radix Salviae Miltiorrhizae total phenolic acids extract 5.3g, the embodiment one of embodiment one; An amount of dissolve with ethanol of tanshinone extract joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.The clathrate powder of tanshinone extract and hydroxypropyl and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, natural Broneolum Syntheticum and 18.5g Polyethylene Glycol-6000 mix homogeneously, heating and melting, move in the dropping-pill machine jar after changing material, in ℃ liquid paraffin of medicine liquid droplet to 6~8, oil removing makes 1000 of drop pill.
Embodiment eight
Get the tanshinone extract 0.3g of embodiment two, ginsenoside extract 0.8g, the natural Broneolum Syntheticum 0.5g of Radix Salviae Miltiorrhizae total phenolic acids extract 5.9g, the embodiment two of embodiment two; An amount of dissolve with ethanol of tanshinone extract joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.The clathrate powder of tanshinone extract and hydroxypropyl and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, natural Broneolum Syntheticum and 18.0g Polyethylene Glycol-4000 mix homogeneously, heating and melting, move in the dropping-pill machine jar after changing material, in ℃ liquid paraffin of medicine liquid droplet to 6~8, oil removing makes 1000 of drop pill.
Embodiment nine
Get the tanshinone extract 0.3g of embodiment three, ginsenoside extract 1.0g, the natural Broneolum Syntheticum 0.5g of Radix Salviae Miltiorrhizae total phenolic acids extract 4.9g, the embodiment one of embodiment three; An amount of dissolve with ethanol of tanshinone extract joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.The clathrate powder of tanshinone extract and hydroxypropyl and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, natural Broneolum Syntheticum and 19.0g Polyethylene Glycol-6000 mix homogeneously, heating and melting, move in the dropping-pill machine jar after changing material, in ℃ methyl-silicone oil of medicine liquid droplet to 6~8, oil removing makes 1000 of drop pill.
Embodiment ten
Get the tanshinone extract 0.3g of embodiment one, ginsenoside extract 0.9g, the natural Broneolum Syntheticum 0.5g of Radix Salviae Miltiorrhizae total phenolic acids extract 6.5g, the embodiment two of embodiment one; An amount of dissolve with ethanol of tanshinone extract joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.The clathrate powder of tanshinone extract and hydroxypropyl and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, natural Broneolum Syntheticum and 3.5g Polyethylene Glycol-4000 and 14.0g Polyethylene Glycol-6000 mix homogeneously, heating and melting, move in the dropping-pill machine jar after changing material, in ℃ liquid paraffin of medicine liquid droplet to 6~8, oil removing makes 1000 of drop pill.
Embodiment 11
Get the tanshinone extract 0.4g of embodiment three, ginsenoside extract 0.8g, the natural Broneolum Syntheticum 0.5g of Radix Salviae Miltiorrhizae total phenolic acids extract 7.5g, the embodiment one of embodiment three; An amount of dissolve with ethanol of tanshinone extract joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.The clathrate powder of tanshinone extract and hydroxypropyl and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, natural Broneolum Syntheticum and 16.5g Polyethylene Glycol-6000 mix homogeneously, heating and melting, move in the dropping-pill machine jar after changing material, in ℃ liquid paraffin of medicine liquid droplet to 6~8, oil removing makes 1000 of drop pill.
Embodiment 12
Get the tanshinone extract 0.3g of embodiment three, ginsenoside extract 0.8g, the Borneolum Syntheticum 0.4g of Radix Salviae Miltiorrhizae total phenolic acids extract 5.7g, the embodiment two of embodiment three; An amount of dissolve with ethanol of tanshinone extract joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.The clathrate powder of tanshinone extract and hydroxypropyl and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, natural Broneolum Syntheticum and 18.5g Polyethylene Glycol-6000 mix homogeneously, heating and melting, move in the dropping-pill machine jar after changing material, in ℃ liquid paraffin of medicine liquid droplet to 6~8, oil removing makes 1000 of drop pill.
Embodiment 13
Get the tanshinone extract 0.3g of embodiment one, ginsenoside extract 0.9g, the Lignum Dalbergiae Odoriferae oil 0.5g of Radix Salviae Miltiorrhizae total phenolic acids extract 5.3g, the embodiment one of embodiment one; An amount of dissolve with ethanol of tanshinone extract joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.The clathrate powder of tanshinone extract and hydroxypropyl and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, Lignum Dalbergiae Odoriferae oil and 18.5g Polyethylene Glycol-6000 mix homogeneously, heating and melting, move in the dropping-pill machine jar after changing material, in ℃ methyl-silicone oil of medicine liquid droplet to 6~8, oil removing makes 1000 of drop pill.
Embodiment 14
Get the tanshinone extract 0.3g of embodiment two, ginsenoside extract 0.8g, the Lignum Dalbergiae Odoriferae oil 0.5g of Radix Salviae Miltiorrhizae total phenolic acids extract 5.9g, the embodiment two of embodiment two; An amount of dissolve with ethanol of tanshinone extract, Lignum Dalbergiae Odoriferae oil joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract, Lignum Dalbergiae Odoriferae oil and hydroxypropyl.Above-mentioned clathrate powder and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract and 3.5g Polyethylene Glycol-4000 and 14.5g Polyethylene Glycol-6000 mix homogeneously, heating and melting moves in the dropping-pill machine jar behind the change material, in ℃ liquid paraffin of medicine liquid droplet to 6~8, oil removing makes 1000 of drop pill.
Embodiment 15
Get the tanshinone extract 0.8g of embodiment one, ginsenoside extract 2.5g, the natural Broneolum Syntheticum 1.2g of Radix Salviae Miltiorrhizae total phenolic acids extract 15.4g, the embodiment one of embodiment one; An amount of dissolve with ethanol of tanshinone extract joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.The clathrate powder of tanshinone extract and hydroxypropyl and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, natural Broneolum Syntheticum and mannitol 5.5g, calcium disodium edetate 0.9g and distilled water 1ml, behind the said components mixing, lyophilization, 1000 of packing, promptly.
Embodiment 16
Get the tanshinone extract 0.8g of embodiment two, ginsenoside extract 2.9g, the natural Broneolum Syntheticum 1.2g of Radix Salviae Miltiorrhizae total phenolic acids extract 14.7g, the embodiment two of embodiment two; An amount of dissolve with ethanol of tanshinone extract joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.The clathrate powder of tanshinone extract and hydroxypropyl and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, natural Broneolum Syntheticum and low molecular dextran 5.5g, calcium disodium edetate 0.9g and distilled water 1ml, behind the said components mixing, lyophilization, 1000 of packing, promptly.
Embodiment 17
Get the tanshinone extract 0.9g of embodiment three, ginsenoside extract 1.9g, the Borneolum Syntheticum 1.2g of Radix Salviae Miltiorrhizae total phenolic acids extract 15.6g, the embodiment one of embodiment three; An amount of dissolve with ethanol of tanshinone extract joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.The clathrate powder of tanshinone extract and hydroxypropyl and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, natural Broneolum Syntheticum and glucose 5.5g, sodium thiosulfate 0.9g and distilled water 1ml, behind the said components mixing, lyophilization, 1000 of packing, promptly.
Embodiment 18
Get tanshinone extract 0.8g, the Lignum Dalbergiae Odoriferae oil 1.5g of embodiment one, join in the saturated hydroxypropyl solution of 13ml, stirring and dissolving filters, the filtrate cold drying, the clathrate powder of tanshinone extract, Lignum Dalbergiae Odoriferae oil and hydroxypropyl.Except that above-mentioned clathrate powder, get ginsenoside extract 2.5g, mannitol 5.5g, calcium disodium edetate 0.9g and the distilled water 2ml of Radix Salviae Miltiorrhizae total phenolic acids extract 15.6g, the embodiment one of embodiment one again, behind the said components mixing, lyophilization, 1000 of packing, promptly.
Embodiment 19
Get the tanshinone extract 0.6g of embodiment one, ginsenoside extract 1.2g, the Borneolum Syntheticum 0.8g of Radix Salviae Miltiorrhizae total phenolic acids extract 11.7g, the embodiment one of embodiment one; An amount of dissolve with ethanol of tanshinone extract joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.The clathrate powder of tanshinone extract and hydroxypropyl and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, natural Broneolum Syntheticum and 210g microcrystalline Cellulose mix homogeneously, add 3% polyvidone alcoholic solution system soft material, cross 18 mesh sieve system granules, 60 ℃ of dryings 30~45 minutes, granulate adds the 24g Pulvis Talci, mixing, fill in 1000 capsules, promptly.
Embodiment 20
Get the tanshinone extract 0.6g of embodiment one, ginsenoside extract 1.2g, the natural Broneolum Syntheticum 0.8g of Radix Salviae Miltiorrhizae total phenolic acids extract 11.7g, the embodiment two of embodiment one; An amount of dissolve with ethanol of tanshinone extract joins in the saturated hydroxypropyl solution, after stirring, restir 1 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.The clathrate powder of tanshinone extract and hydroxypropyl and Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract, natural Broneolum Syntheticum and with 64g microcrystalline Cellulose and 20g magnesium stearate mix homogeneously, be pressed into 1000, promptly.

Claims (10)

1. Chinese medicine composition for the treatment of cardiovascular disease, form by following component by weight percentage:
The tanshinone extract 2.5%~12.0% that contains 55%~85% TANSHINONES,
The Radix Salviae Miltiorrhizae total phenolic acids extract 57.0%~90.0% that contains 70%~98% Radix Salviae Miltiorrhizae total phenolic acids,
The ginsenoside extract 2.5%~25.0% that contains 75%~98% total saponins,
Natural Broneolum Syntheticum or Lignum Dalbergiae Odoriferae oil 2.5%~15.0%;
Described ginsenoside extract is to be the extract of feedstock production with the Radix Ginseng.
2. according to the described Chinese medicine composition of claim 1, it is characterized in that the percentage by weight of described each component is:
The tanshinone extract 3.0%~8.0% that contains 55%~85% TANSHINONES,
The Radix Salviae Miltiorrhizae total phenolic acids extract 72.0%~82.0% that contains 70%~98% Radix Salviae Miltiorrhizae total phenolic acids,
The ginsenoside extract 6.0%~15.0% that contains 75%~98% total saponins,
Natural Broneolum Syntheticum or Lignum Dalbergiae Odoriferae oil 4.0%~10.0%.
3. according to the described Chinese medicine composition of claim 1, it is characterized in that the percentage by weight of described each component is:
The tanshinone extract 4% that contains 55%~85% TANSHINONES,
The Radix Salviae Miltiorrhizae total phenolic acids extract 76% that contains 70%~98% Radix Salviae Miltiorrhizae total phenolic acids,
The ginsenoside extract 13% that contains 75%~98% total saponins,
Natural Broneolum Syntheticum or Lignum Dalbergiae Odoriferae oil 7%.
4. according to the described Chinese medicine composition of the arbitrary claim of claim 1~3, it is characterized in that, with the alternative described tanshinone extract that contains 55%~85% TANSHINONES of the clathrate of tanshinone extract and hydroxypropyl; The clathrate of described tanshinone extract and hydroxypropyl prepares with following method: the weighting profit requires the tanshinone extract that contains 55%~85% TANSHINONES of predetermined weight percentage ratio, use an amount of dissolve with ethanol, join in the saturated hydroxypropyl solution, 25~50 ℃ stir after, restir 0.5~2 hour, cold preservation is spent the night, sucking filtration, the filtrate cold drying, the clathrate powder of tanshinone extract and hydroxypropyl.
5. according to the described Chinese medicine composition of the arbitrary claim of claim 1~3, it is characterized in that described tanshinone extract is prepared by following method: the Radix Salviae Miltiorrhizae of getting after the pulverizing is thrown CO 2Extraction kettle in the extraction equipment after system's each several part all reaches design temperature, boosts to setting pressure with extraction kettle, 75%~95% alcoholic solution is added system by the flow of setting, with CO 2Mix back circulation in whole system and carry out dynamic extraction; After extraction is finished, emit extracting solution, concentrate, vacuum drying gets tanshinone extract;
Wherein Cui Qu condition is: described extracting pressure is 15MPa~25Mpa, and extraction and separation temperature are 30 ℃~55 ℃, and separation temperature is lower than extraction temperature, and the ethanol flow is 0.5mL/min~1.5mL/min.
6. according to the described Chinese medicine composition of the arbitrary claim of claim 1~3, it is characterized in that, described tanshinone extract is prepared by following method: the Radix Salviae Miltiorrhizae of getting salvia piece or pulverizing, add 85~95% soak with ethanol 2 hours, then 65~85 ℃ of following reflux, extract, 3 times, each quantity of solvent is 5 times of crude drug weight, each 0.5~1.5 hour extraction time; Merge extractive liquid,, extracting solution is being evaporated to 1/35~1/45 of original volume below 50 ℃, get concentrated solution; The water that adds 2~4 times of volumes in the concentrated solution was placed 6~24 hours, filtered; Filtrate gets tanshinone extract in dry below 50 ℃.
7. according to the described Chinese medicine composition of the arbitrary claim of claim 1~3, it is characterized in that described ginsenoside extract is prepared by following method: get the ginseng crude drug, pulverize, add 5~8 times of amounts of medical material weight, 50~90% ethanol, reflux or supersound extraction 2~3 times, merge extractive liquid; Extracting solution filters, and being concentrated into does not have the alcohol flavor, is dissolved in water, and filters; Macroporous resin column on the filtrate with the water flushing of 2~4 times of amount column volumes, with 60~85% ethanol elutions of 2~4 times of amount column volumes, is collected ethanol elution then, the eluent concentrating under reduced pressure, and drying promptly gets ginsenoside extract.
8. Chinese medicine composition according to claim 7 is characterized in that, described macroporous resin is D101, AB-8 or ZTC type macroporous resin.
9. be the drop pill that active component is made according to the described Chinese medicine composition of the arbitrary claim of claim 1~3, it is characterized in that, described drop pill is prepared from by following method: get above-mentioned tanshinone extract, Radix Salviae Miltiorrhizae total phenolic acids extract, ginsenoside extract and natural Broneolum Syntheticum or Lignum Dalbergiae Odoriferae oil to scale, Polyethylene Glycol-6000 or Polyethylene Glycol-4000 or both mixture mix homogeneously with 2~4 times of medicine gross weights, heating and melting, move in the dropping-pill machine jar after changing material, in ℃ liquid paraffin of medicine liquid droplet to 6~8, oil removing, promptly.
10. be the injectable powder that active component is made according to the described Chinese medicine composition of the arbitrary claim of claim 1~3.
CN2005100148495A 2005-08-24 2005-08-24 Traditional Chinese medicine for treating cardiovascular diseases Expired - Fee Related CN1919246B (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
CN2005100148495A CN1919246B (en) 2005-08-24 2005-08-24 Traditional Chinese medicine for treating cardiovascular diseases

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
CN2005100148495A CN1919246B (en) 2005-08-24 2005-08-24 Traditional Chinese medicine for treating cardiovascular diseases

Publications (2)

Publication Number Publication Date
CN1919246A CN1919246A (en) 2007-02-28
CN1919246B true CN1919246B (en) 2010-09-29

Family

ID=37777182

Family Applications (1)

Application Number Title Priority Date Filing Date
CN2005100148495A Expired - Fee Related CN1919246B (en) 2005-08-24 2005-08-24 Traditional Chinese medicine for treating cardiovascular diseases

Country Status (1)

Country Link
CN (1) CN1919246B (en)

Citations (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN1579462A (en) * 2003-08-08 2005-02-16 珠海经济特区新科应用研究所 Ready-made traditional Chinese medicine formed from compound red-rooted salvia root effective zontent
CN1596920A (en) * 2003-09-19 2005-03-23 天津天士力制药股份有限公司 Medicinal composition for treating cardiopathy and its preparation method and use

Patent Citations (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN1579462A (en) * 2003-08-08 2005-02-16 珠海经济特区新科应用研究所 Ready-made traditional Chinese medicine formed from compound red-rooted salvia root effective zontent
CN1596920A (en) * 2003-09-19 2005-03-23 天津天士力制药股份有限公司 Medicinal composition for treating cardiopathy and its preparation method and use

Non-Patent Citations (3)

* Cited by examiner, † Cited by third party
Title
宋启煌等.超临界CO2 从丹参中萃取丹参酮ⅡA 的研究.精细化工21.2004,21125-127. *
潘桂湘等.复方丹参中丹参、三七化学成分分析的研究概述.天津中医19 5.2002,19(5),75-78.
潘桂湘等.复方丹参中丹参、三七化学成分分析的研究概述.天津中医19 5.2002,19(5),75-78. *

Also Published As

Publication number Publication date
CN1919246A (en) 2007-02-28

Similar Documents

Publication Publication Date Title
CN100404035C (en) Combination of Chinese traditional medicine for curing cardiovascular diseases and cerebrovascular disease
CN1919248B (en) Traditional Chinese medicinal formulation for treating cardiovascular and cerebrovascular disease
CN1931236B (en) Medicine composition of red sage and rhodiola root
CN1919240B (en) Traditional Chinese medicine for treating cardiovascular and cerebrovascular diseases
CN104352624B (en) Application of the anaesthetic core fragrant plant n-butanol extract in preventing and treating diabetes medicament is prepared
CN1919239B (en) Traditional medicine composition for treating cardiovascular and cerebrovascular diseases
CN1919252B (en) Medicine for treating cardiovascular and cerebrovascular disease
CN1919238B (en) Medicine for treating cardiovascular and cerebrovascular disease
CN1919244B (en) Chinese traditional medicine for treating cardiovascular disease
CN1919247B (en) Chinese medicine for treating cardiovascular and cerebrovascular disease
CN1931233B (en) Medicine composition of red sage and epimedium for treating cardiac and cerebral vascular diseases
CN100467025C (en) Use of asiaticoside in preparation of medicines for diseases of cardio-cerebral blood vessels
CN1919242B (en) Traditional Chinese medicine composition for treating cardiac and cerebral vascular disease
CN1919251B (en) Traditional Chinese medicine composition for treating cardiac vascular disease
CN1919237B (en) Medicine for treating cardiovascular and cerebrovascular diseases
CN1919249B (en) Chinese traditional medicine for treating cardiovascular and cerebrovascular disease
CN1919246B (en) Traditional Chinese medicine for treating cardiovascular diseases
CN1919235B (en) Cardiac and cerebral vascular disease treating pharmaceutical composition
CN1919236B (en) Medicine for treating cardiovascular and cerebrovascular diseases
CN1919245B (en) Traditional medicine composition for treating cardiovascular and cerebrovascular diseases
CN1923229B (en) Pharmaceutical composition comprising notoginseng extract, Danshen extract and puerarin
CN1923228B (en) Pharmaceutical composition comprising notoginseng extract, Danshen extract and ligustrazine
CN1582946B (en) Use of centellosic acid derivative in preparation of medicines for diseases of cardio-cerebral blood vessels
CN1919241B (en) Chinese medicinal preparation for treating cardiovascular and cerebrovascular disease
CN1919243B (en) Traditional medicine composition for treating cardiovascular and cerebrovascular diseases

Legal Events

Date Code Title Description
C06 Publication
PB01 Publication
C41 Transfer of patent application or patent right or utility model
TA01 Transfer of patent application right

Effective date of registration: 20070608

Address after: Tianjin City Hedong District of Beichen Puji No. 2 in the modern Chinese medicine city

Applicant after: Tianjin Tianshili Pharmaceutical Co., Ltd.

Address before: The white road of Beichen science and Technology Park in Beichen District of Tianjin City Xinyi Liaohe Road No. 1

Applicant before: Tianshili Modern Traditional Chinese Medicine Research & Devleopment Co., Ltd.,

C10 Entry into substantive examination
SE01 Entry into force of request for substantive examination
C14 Grant of patent or utility model
GR01 Patent grant
C56 Change in the name or address of the patentee

Owner name: TASLY PHARMACEUTICAL GROUP CO., LTD.

Free format text: FORMER NAME: TIANJIN TASLY PHARMACEUTICAL CO., LTD.

CP01 Change in the name or title of a patent holder

Address after: 300402 Tianjin city Beichen District Puji Hedong No. 2 in the modern Chinese medicine city

Patentee after: Tasly Pharmaceutical Group Co., Ltd.

Address before: 300402 Tianjin city Beichen District Puji Hedong No. 2 in the modern Chinese medicine city

Patentee before: Tianjin Tianshili Pharmaceutical Co., Ltd.

CP01 Change in the name or title of a patent holder

Address after: 300402 Tianjin city Beichen District Puji Hedong No. 2 in the modern Chinese medicine city

Patentee after: Tasly Pharmaceutical Group Limited by Share Ltd

Address before: 300402 Tianjin city Beichen District Puji Hedong No. 2 in the modern Chinese medicine city

Patentee before: Tasly Pharmaceutical Group Co., Ltd.

CP01 Change in the name or title of a patent holder
CF01 Termination of patent right due to non-payment of annual fee

Granted publication date: 20100929

Termination date: 20190824

CF01 Termination of patent right due to non-payment of annual fee