CN101843790A

CN101843790A - Medicinal composition

Info

Publication number: CN101843790A
Application number: CN 201010108732
Authority: CN
Inventors: 李瑞菊; 李惠冬; 陈子雷; 丁蕊艳; 杜红霞
Original assignee: Individual
Current assignee: Individual
Priority date: 2010-02-10
Filing date: 2010-02-10
Publication date: 2010-09-29

Abstract

The invention discloses a medicinal composition for assisting in treating hepatitis and application thereof in preparation of medicaments for assisting in treating the hepatitis. The medicinal composition contains dichloroacetic acid diisopropylamine and Chinese medicament extracts. By combining western medicaments and Chinese medicaments, the medicinal composition has synergistic functions, and can bring the gospel to hepatopath.

Description

A kind of Pharmaceutical composition

Invention field

The present invention relates to a kind of Pharmaceutical composition, be specifically related to the Pharmaceutical composition formed by diisopropylamine dichloroacetate and Chinese medicine extract, and the purposes of said composition in the medicine of preparation adjuvant treating hepatitis, medical technical field belonged to.

Background technology

Hepatitis (formal name used at school: Hepatitis) be the inflammation of liver.The reason of hepatitis has a variety of, and modal is that virus causes, and also has autoimmune to cause in addition.Excessive drinking also can cause hepatitis.Medically hepatitis can be divided into first, second, third, fourth, penta, oneself, seven types of heptan, and wherein hepatitis B is the most extensive popular, a kind of infectious hepatitis that harm is the most serious.Hepatitis B (abbreviation hepatitis B) is the liver inflammatory damage that is caused by hepatitis B virus (abbreviation hepatitis B virus), the primary disease extend over the entire globe, clinical manifestation is weak, loss of appetite, feels sick, vomits, detests oil, diarrhoea and abdominal distention, some cases has heating, jaundice, the concealment of half patient onset is arranged approximately, in inspection, find.China is the most popular country of hepatitis B, reaches more than 35% some local crowd infection rate, is that the most serious of current harm people ' s health specially catches an illness.According to investigations, China's hepatitis B patient is about 2,700 ten thousand, and annual New Development patient about 9,000,000.The hepatitis B clinical manifestation is various, easily develops into chronic hepatitis and liver cirrhosis, and a few peoples finally develop into hepatocarcinoma.Hepatic fibrosis is the total pathological change of many chronic hepatopathy evolutions, and give birth to slowly, the persistence damage is the prerequisite that hepatic fibrosis forms.

Cause the factor of hepatic injury a lot,, hepatitis B, liver cirrhosis, take some drugs for a long time and all can cause acute and chronic hepatic injury generally because of factors such as medicine, a large amount of ethanol, allergy cause acute liver damage.By reducing detrimental effect to liver function, can adjuvant treating hepatitis.

The medicine that is used for the treatment of acute and chronic hepatic injury at present, commonly used have diisopropylamine dichloroacetate, tiopronin, a diammonium glycyrrhizinate etc.These chemicalses generally have certain side effect, and cause that therapeutic effect at a specified future date is poor, problem such as Strain produces after drug resistance phenomenon, the drug withdrawal relapse rate height.

The curative effect of Chinese medicine hepatitis B is proved by a large amount of clinical trials.Chinese medicine all can be brought into play curative effect preferably at aspects such as antiviral, adjusting immunity of organisms, protection hepatocyte.But Chinese medicine preparation ubiquity onset at present is slow, needs problems such as life-time service.Therefore, Western medicine and Chinese Medicine and Clavicular need be got up, i.e. synergism is played in Chinese medicine and western medicine combination, solves the problem that above-mentioned Western medicine and Chinese medicine exist in auxiliary treatment all kinds hepatitis separately, produces synergistic therapeutic effect simultaneously.

Summary of the invention

The object of the present invention is to provide the Pharmaceutical composition of forming at 1: 107 with weight ratio by diisopropylamine dichloroacetate and a kind of Chinese medicine extract, wherein be prepared as follows on the method basis of the Chinese medicine extract of said composition according to claim 1-2 among the Chinese patent CN1259944C: the medicine material combination back of following proportioning is dropped in the extractor, add 10 liters in water, under 50-70 ℃ of temperature, decoct and obtained the water extract in 45 minutes, gained water extract proportion is 1.04-1.05g/l, concentrating under reduced pressure, get dry extract, this Chinese medicine the water extracted immersing paste is called " the described Chinese medicine extract of this paper (or above) " hereinafter.Described medicine material mixing ratio by weight is: Herba Hyperici Japonici: Herba Sedi: Herba Patriniae: Radix Salviae Miltiorrhizae: the five tastes give: Fructus Crataegi: Semen Cassiae: Rhizoma Alismatis: Radix Bupleuri: Radix Glycyrrhizae=6: 6: 4: 4: 3: 3: 3: 2: 2: 1.

Another object of the present invention is to provide the purposes of above-mentioned Pharmaceutical composition in preparation auxiliary treatment all kinds hepatitis medicament.

Above-mentioned composition and mixing acceptable accessories can be made acceptable forms clinically, as tablet, capsule, granule, soft capsule, drop etc.

For ease of understanding the useful medical value of Pharmaceutical composition of the present invention, provide the pharmacological experiments of the present composition below in the adjuvant treating hepatitis disease.

Experimental example: the main pharmacodynamics of Pharmaceutical composition of the present invention studies confirm that it has strong transaminase lowering effect, i.e. function for protecting liver and reducing enzyme activity." modern pharmacology test method " (volume two) with reference to the Zhang Juntian chief editor, combined publication society of China Concord Medical Science University of Beijing Medical University, the 1397th～1398 page, disclosed method in " first segment chmice acute chemical liver injury model ", set up the acute chemical liver injury model of mouse carbon tetrachloride, carry out the pharmacodynamics test of Pharmaceutical composition anti-liver injury of the present invention.

The test grouping:

1, normal control group: animal does not do any processing, and normal physiological saline is irritated stomach;

2, model control group: after the animal model modeling success, normal physiological saline is irritated stomach;

3, pure Chinese drug-treated group: the water extracted immersing paste 1.07g/kg body weight as indicated above;

4, diisopropylamine dichloroacetate group: the 10mg/kg body weight is irritated stomach;

5, compositions group: 10mg/kg body weight diisopropylamine dichloroacetate+the water extracted immersing paste 1.07g/kg body weight mentioned above is irritated stomach.

Following table has shown the influence of each group to Mouse Liver function leading indicator GOT, GPT.

Table one

Group	Number of animals	GOT (active unit)	GPT (active unit)
Group	Number of animals	GOT (active unit)	GPT (active unit)	The normal control group	??10	??21.78±16.55	??48.61±15.35
Model control group	??10	??248.76±74.58	??312.25±60.47	The normal control group	??10	??21.78±16.55	??48.61±15.35
Model control group	??10	??248.76±74.58	??312.25±60.47	Pure Chinese drug-treated group	??10	??174.43±60.42	??242.63±54.22
The diisopropylamine dichloroacetate group	??10	??120.74±39.23	??192.78±29.20	Pure Chinese drug-treated group	??10	??174.43±60.42	??242.63±54.22
The diisopropylamine dichloroacetate group	??10	??120.74±39.23	??192.78±29.20	The compositions group	??10	??64.41±24.24	??108.12±49.23

This table shows that all there is significant difference (P＜0.05) in each group (pure Chinese drug-treated group, diisopropylamine dichloroacetate group, compositions group) of treatment with model control group, and all there are significant difference (P＜0.05) in compositions group and pure Chinese drug-treated group, compositions group and diisopropylamine dichloroacetate group.Show that there are cooperative effect in diisopropylamine dichloroacetate and described Chinese medicinal components in the compositions group.

Specific embodiment

The specific embodiment of form is described in further detail foregoing of the present invention by the following examples, but this should be interpreted as that the scope of above-mentioned theme of the present invention only limits to following embodiment.All technology that realizes based on foregoing of the present invention all belong to scope of the present invention.The adjuvant of each dosage form can substitute with acceptable accessories in following examples, perhaps reduces, increases.

The pharmaceutics test: the weight ratio of diisopropylamine dichloroacetate and Chinese medicine extract is 1: 107 in the Pharmaceutical composition.

Embodiment 1: the preparation of Pharmaceutical composition tablet of the present invention

Prescription 1:

Pharmaceutical composition 40g

Starch 120g

Microcrystalline Cellulose 40g

The 2%HPMC aqueous solution is an amount of

Magnesium stearate 2g

Carboxymethylstach sodium 4g

???????????????????????????????????????????

Prepare 1000 altogether

Prescription 2:

Pharmaceutical composition 60g

Starch 120g

Microcrystalline Cellulose 40g

The 2%HPMC aqueous solution is an amount of

Magnesium stearate 2g

Carboxymethylstach sodium 4g

?????????????????????????????????????????????????

Prepare 1000 altogether

Prescription 3:

Pharmaceutical composition 80g

Starch 120g

Microcrystalline Cellulose 40g

The 2%HPMC aqueous solution is an amount of

Magnesium stearate 2g

Carboxymethylstach sodium 4g

????????????????????????????????????????????

Prepare 1000 altogether

Prescription 4:

Pharmaceutical composition 100g

Starch 120g

Microcrystalline Cellulose 40g

The 2%HPMC aqueous solution is an amount of

Magnesium stearate 2g

Carboxymethylstach sodium 4g

?????????????????????????????????????????

Prepare 1000 altogether

Prescription 5:

Pharmaceutical composition 120g

Starch 120g

Microcrystalline Cellulose 40g

The 2%HPMC aqueous solution is an amount of

Magnesium stearate 2g

Carboxymethylstach sodium 4g

????????????????????????????????????????????

Prepare 1000 altogether

Preparation technology:

(1), takes by weighing supplementary material according to recipe quantity.Hypromellose 2% the aqueous solution made soluble in water is standby.

(2), with Pharmaceutical composition, starch, microcrystalline Cellulose mix homogeneously, it is an amount of to add the 2%HPMC aqueous solution, stirs, and makes suitable soft material.

(3), cross 20 mesh sieve system granules.

(4), granule is dried under 60 ℃ condition.

(5), dry good granule adds magnesium stearate and carboxymethylstach sodium, mistake 18 mesh sieve granulate, mix homogeneously.

(6), take a sample the semi-finished product chemical examination.

(7), the sheet weight sheet of determining according to chemical examination.

(8), finished product is examined the packing warehouse-in entirely.

Embodiment 2: the preparation of Pharmaceutical composition capsule of the present invention

Prescription 1:

Pharmaceutical composition 40g

Starch 120g

Microcrystalline Cellulose 40g

The 2%HPMC aqueous solution is an amount of

Magnesium stearate 2g

Carboxymethylstach sodium 4g

??????????????????????????????????????

Prepare 1000 altogether

Prescription 2:

Pharmaceutical composition 60g

Starch 120g

Microcrystalline Cellulose 40g

The 2%HPMC aqueous solution is an amount of

Magnesium stearate 2g

Carboxymethylstach sodium 4g

????????????????????????????????????????????

Prepare 1000 altogether

Prescription 3:

Pharmaceutical composition 80g

Starch 120g

Microcrystalline Cellulose 40g

The 2%HPMC aqueous solution is an amount of

Magnesium stearate 2g

Carboxymethylstach sodium 4g

????????????????????????????????????????????

Prepare 1000 altogether

Prescription 4:

Pharmaceutical composition 100g

Starch 120g

Microcrystalline Cellulose 40g

The 2%HPMC aqueous solution is an amount of

Magnesium stearate 2g

Carboxymethylstach sodium 4g

?????????????????????????????????????????????

Prepare 1000 altogether

Prescription 5:

Pharmaceutical composition 120g

Starch 120g

Microcrystalline Cellulose 40g

The 2%HPMC aqueous solution is an amount of

Magnesium stearate 2g

Carboxymethylstach sodium 4g

??????????????????????????????????????????????

Prepare 1000 altogether

Preparation technology:

(3), cross 20 mesh sieve system granules.

(4), granule is dried under 60 ℃ condition.

(5), dry good granule adds magnesium stearate, mistake 18 mesh sieve granulate, mix homogeneously.

(6), take a sample the semi-finished product chemical examination.

(7), the loading amount of determining according to chemical examination incapsulates.

(8), finished product is examined the packing warehouse-in entirely.

The preparation of embodiment 3 Pharmaceutical composition granules of the present invention

Prescription 1:

Pharmaceutical composition 40g

Sucrose 1800g

The 2%HPMC50% alcoholic solution is an amount of

???????????????????????????????????????????????????

Prepare 1000 bags altogether

Prescription 2:

Pharmaceutical composition 60g

Sucrose 1800g

The 2%HPMC50% alcoholic solution is an amount of

???????????????????????????????????????????????????

Prepare 1000 bags altogether

Prescription 3:

Pharmaceutical composition 80g

Sucrose 1800g

The 2%HPMC50% alcoholic solution is an amount of

??????????????????????????????????????????????????????

Prepare 1000 bags altogether

Prescription 4:

Pharmaceutical composition 100g

Sucrose 1800g

The 2%HPMC50% alcoholic solution is an amount of

?????????????????????????????????????????????????????

Prepare 1000 bags altogether

Prescription 5:

Pharmaceutical composition 120g

Sucrose 1800g

The 2%HPMC50% alcoholic solution is an amount of

??????????????????????????????????????????????????????

Prepare 1000 bags altogether

Preparation technology:

(1), it is standby sucrose to be pulverized 100 mesh sieves.

(2), take by weighing supplementary material according to recipe quantity.

(3), with the method mix homogeneously that Pharmaceutical composition and sucrose progressively increase with equivalent, it is an amount of to add the 2%HPMC50% alcoholic solution, stirs, and makes suitable soft material,

(4), cross 20 mesh sieve system granules.

(5), granule is dried under 60 ℃ condition.

(6), dried granule is crossed 18 mesh sieve granulate.

(7), sampling, the content of principal agent is determined loading amount in the semi-finished product chemical examinations granule.

(8), packing, finished product is examined entirely, packing warehouse-in.

Embodiment 4: the preparation of Pharmaceutical composition flexible glue of the present invention agent

Prescription 1:

Pharmaceutical composition 40g

Soybean oil 400g

Soybean phospholipid 20g

Cera Flava 12g

??????????????????????????????????????????????????

Prepare 1000 altogether

Prescription 2:

Pharmaceutical composition 60g

Soybean oil 400g

Soybean phospholipid 20g

Cera Flava 12g

????????????????????????????????????????????????????

Prepare 1000 altogether

Prescription 3:

Pharmaceutical composition 80g

Soybean oil 400g

Soybean phospholipid 20g

Cera Flava 12g

??????????????????????????????????????????????????????

Prepare 1000 altogether

Prescription 4:

Pharmaceutical composition 100g

Soybean oil 400g

Soybean phospholipid 20g

Cera Flava 12g

?????????????????????????????????????????????????????

Prepare 1000 altogether

Prescription 5:

Pharmaceutical composition 120g

Soybean oil 400g

Soybean phospholipid 20g

Cera Flava 12g

????????????????????????????????????????????????

Prepare 1000 altogether

Preparation technology: with the soybean oil of recipe quantity and soybean phospholipid, Cera Flava heating and melting, mixing is put coldly, adds Pharmaceutical composition and grinds well, and is pressed into soft capsule and gets final product.

Embodiment 5: the preparation of Pharmaceutical composition drop pill of the present invention

Prescription 1:

Pharmaceutical composition 40g

Polyethylene glycol 6000 600g

Prescription 2:

Pharmaceutical composition 60g

Polyethylene glycol 6000 600g

Prescription 3:

Pharmaceutical composition 80g

Polyethylene glycol 6000 600g

Prescription 4:

Pharmaceutical composition 100g

Polyethylene glycol 6000 600g

Prescription 5:

Pharmaceutical composition 120g

Polyethylene glycol 6000 600g

Preparation technology: with polyethylene glycol 6000 heating and melting in water-bath, treat to add Pharmaceutical composition after whole fusions, stirring and dissolving, 60 mesh sieves filter, and keep 60 ℃ to splash in the liquid paraffin that is chilled to below 10 ℃ and make ball.

Claims

1. Pharmaceutical composition, it is made up of with weight ratio diisopropylamine dichloroacetate and Chinese medicine extract at 1: 107, described Chinese medicine extract prepares by following method: the medicine material combination back of following proportioning is dropped in the extractor, add 10 liters in water, under 50-70 ℃ of temperature, decoct and obtained the water extract in 45 minutes, gained water extract proportion is 1.04-1.05g/l, concentrating under reduced pressure gets dry extract; Described medicine material mixing ratio by weight is: Herba Hyperici Japonici: Herba Sedi: Herba Patriniae: Radix Salviae Miltiorrhizae: the five tastes give: Fructus Crataegi: Semen Cassiae: Rhizoma Alismatis: Radix Bupleuri: Radix Glycyrrhizae=6: 6: 4: 4: 3: 3: 3: 2: 2: 1.

2. the purposes of compositions as claimed in claim 1 in the medicine of preparation adjuvant treating hepatitis.