CN101108246B - Thymus gland pentapeptide oral intestine-dissolved formulated product and method of preparing the same and use thereof - Google Patents

Thymus gland pentapeptide oral intestine-dissolved formulated product and method of preparing the same and use thereof Download PDF

Info

Publication number
CN101108246B
CN101108246B CN2006100214294A CN200610021429A CN101108246B CN 101108246 B CN101108246 B CN 101108246B CN 2006100214294 A CN2006100214294 A CN 2006100214294A CN 200610021429 A CN200610021429 A CN 200610021429A CN 101108246 B CN101108246 B CN 101108246B
Authority
CN
China
Prior art keywords
thymopentin
parts
preparation
enteric
adjuvant
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.)
Active
Application number
CN2006100214294A
Other languages
Chinese (zh)
Other versions
CN101108246A (en
Inventor
叶兵
武勇
刘忠荣
及元乔
王若竹
黄瑜
岑国栋
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.)
CHENGDU DIAO JIUHONG PHARMACEUTICAL FACTORY
Original Assignee
CHENGDU DIAO JIUHONG PHARMACEUTICAL FACTORY
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 CHENGDU DIAO JIUHONG PHARMACEUTICAL FACTORY filed Critical CHENGDU DIAO JIUHONG PHARMACEUTICAL FACTORY
Priority to CN2006100214294A priority Critical patent/CN101108246B/en
Publication of CN101108246A publication Critical patent/CN101108246A/en
Application granted granted Critical
Publication of CN101108246B publication Critical patent/CN101108246B/en
Active legal-status Critical Current
Anticipated expiration legal-status Critical

Links

Images

Abstract

The invention provides a Thymopentin Oral Enteric-coated Agent, which takes thymopentin of effective dosage as the active ingredient and enteric-coated agent as its accessories. Each dosage contains 5mg to 150 mg thymopentin. The invention also provides the preparation method and usage of the enteric-coated agent. The medicine effect tests prove that the medicine has the same indication and efficacy as the injections and can overcome that the gastrointestinal enzyme will easily degrade the thumopentin into amino acid and small peptide so as to lose the activity when orally taking the Thymopentin; the thumopentin can not easily penetrate the gastrointestinal mucosa, resulting in low bioavailability; and the liver has the First-pass effect on the thymopentin. The invention opens a new way to apply thumopentin and increases the patients' compliance.

Description

Thymus gland pentapeptide oral intestine-dissolved formulated product and its production and use
Technical field
The present invention relates to a kind of oral enteric preparation of peptide medicament, particularly, is the oral enteric preparation that forms take Thymopentin as active fraction preparation, belongs to drug world.
Background technology
Present nearly 40 peptide species class medicines on the domestic and international market enjoy the patient to favor owing to polypeptide drug has high activity, low dosage, hypotoxic characteristics.But owing to peptide medicament is easily become aminoacid, little peptide to lose activity by the enzymatic degradation in gastric acid, the gastrointestinal when oral, also being difficult for seeing through gastrointestinal mucosa is absorbed by the body, simultaneously, the peptide medicament of gastrointestinal tract, liver oral disposition has the characteristics such as first pass effect impact, and having limited the oral administration of peptide medicament, the large absolutely number of the route of administration of existing peptide medicament is injection type, uses rather inconvenience, half-life in the body is short low with bioavailability, and has seriously limited its market potential.
Thymopentin (Thymopoietin, TP5) be the pentapeptide of synthetic, its amino acid sequence and structure and thymopoietin II (Thymopoietin II, the pentapeptide fragment at immunocompetence center TP II), namely 32-36 amino acids sequence (essence-Lai-Radix Asparagi-figured silk fabrics-tyrosine) forms identical, it is the important functional activity part of thymopoietin II, Thymopentin has the whole physiological functions identical with thymopoietin II, namely has the immune function of two-ways regulation (Goldstein G, et al.Surv Immunol Res, 185:2 (SI): 1).Thymopentin can promote the Differentiation and development of thymus and periphery T cell, and the immunologic function of body is had dual regulation, can make too high or too low immunoreation trend normal.Thymopentin is mainly used in treating tumor, immunologic hypofunction and autoimmune disease at present, and can regulate the thymus function that goes down, and makes the unbalance immunologic function normalization of body, promotes growth and the differentiation of thymocyte cell.Atrophy of thymus gland and the hypofunction that causes because of age and other factors had important regulating action.Thymopentin is a kind of very safe drugs, no matter subcutaneous injection or intravenously administrable, all toxic and side effects rarely.Therefore Thymopentin is a kind of immunomodulator of new type of safe, and its immune system class drug use person that is developed as has increased a kind of safely and effectively selection.
The same with most peptide medicaments, the Thymopentin preparation that has gone on the market at present both at home and abroad is injection, and using method is: each 1mg, and once a day, 15-30mg is a course for the treatment of, intramuscular injection; Before the operation, and after the operation, once a day; Radiotherapy, chemotherapy, once a day.Because the patient is significantly smaller than oral formulations to the compliance of ejection preparation, the route of administration of medicine changes, for concrete indication and drug effect all can not determine, and for different molecular weight, its supplementary product kind of different types of peptide, consumption difference, the relevant report of the new route of administration of Thymopentin is not arranged at present.
Summary of the invention
In order to overcome above-mentioned deficiency, technical problem to be solved by this invention has provided a kind of thymus gland pentapeptide oral intestine-dissolved formulated product, and it is the oral enteric preparation that forms take Thymopentin as active fraction preparation.The present invention also provides preparation method and the purposes of this oral enteric preparation.
The invention provides a kind of oral Thymopentin enteric coated preparation, it is that Thymopentin by effective dose is active component, add the enteric coated preparation that pharmaceutically acceptable enteric coated preparation is prepared from adjuvant, wherein, Thymopentin 5~150mg is contained in every preparation unit, take every day 1 time, each serving with 1 preparation unit.
Described preparation unit refers to the dosage forms unit of the pharmacy conventional formulation such as every of tablet, every capsules of capsule, granule every bag.
Further, every preparation unit contains Thymopentin 15~50mg.
Wherein, the oral Thymopentin enteric coated preparation of the present invention is to be prepared from by the adjuvant that contains the following weight proportioning: 5~100 parts of absorption enhancers, 7~70 parts of enzyme inhibitors, 5~15 parts of coating materials.
Wherein, described absorption enhancer is one or more in tristerin, polyacrylic acid crosslinked polymer, fatty acid, cholic acid, deoxycholic acid and its esters; Described enzyme inhibitor is one or more in AKOLINE aprotinin, aprotinin, pepsin inhibitor, sodium glycocholate, camostat mesilate camostat mesilate, bacitracin bacitracin, the Semen sojae atricolor pancreatin inhibitor etc.
Wherein, described coating materials is the adjuvant that contains the following weight proportioning: 1~5 part of antiplastering aid, 0.4~3 part of plasticizer, 3.6~7 parts of enteric solubility adjuvants.Described antiplastering aid is one or more in Pulvis Talci, magnesium stearate, the micropowder silica gel; Plasticizer is one or more in propylene glycol, glycerol, Polyethylene Glycol, glycerol triethyl, triethyl citrate, acetyl monoglyceride, phthalate, the Oleum Ricini; The enteric solubility adjuvant is one or more in crylic acid resin, hydroxypropyl cellulose class, arabic gum, the Lac.
Further, described enteric coated preparation also comprises the adjuvant of following weight proportioning:
7~700 parts of filleies, 0~100 part of disintegrating agent, 0~10 part of lubricant, 0~10 part of fluidizer.
Wherein, described filler is one or more in microcrystalline Cellulose, mannitol, lactose, the amylum pregelatinisatum; Described disintegrating agent is one or more in crospolyvinylpyrrolidone, low-substituted hydroxypropyl cellulose, carboxymethyl starch sodium, microcrystalline Cellulose, the sodium alginate; Described lubricant, fluidizer are one or more in Pulvis Talci, micropowder silica gel, hydrogenated vegetable oil, Polyethylene Glycol, stearic acid, magnesium stearate, the dicalcium phosphate dihydrate.
Described preparation is tablet, capsule, pilule, pellet, granule, dry suspension, suspensoid.
Described tablet is enteric coatel tablets, and it is that the Thymopentin and the adjuvant that contain the following weight proportioning are prepared from:
15~50 parts of Thymopentin, 5~30 parts of NaTDCs, 15~30 parts of tristerins, 10~20 parts in polyacrylic acid crosslinked polymer, 7~70 parts of aprotiniies, 10~700 parts of amylum pregelatinisatums, 20~100 parts of crospolyvinylpyrrolidone, 2~10 parts of micropowder silica gels, 2~10 parts of magnesium stearate, 5~15 parts of coating materials.
Further, it is that Thymopentin and the adjuvant that contains the following weight proportioning is prepared from:
5 parts of Thymopentin, 10 parts of NaTDCs, 30 parts of tristerins, 10~20 parts in polyacrylic acid crosslinked polymer, 7 parts of aprotiniies, 700 parts of amylum pregelatinisatums, 20 parts of crospolyvinylpyrrolidone, 10 parts of micropowder silica gels, 10 parts of magnesium stearate, 5~15 parts of coating materials.
Further, it is prepared from by Thymopentin and the adjuvant of following weight proportioning:
5 parts of Thymopentin, 10 parts of NaTDCs, 30 parts of tristerins, 10~20 parts in polyacrylic acid crosslinked polymer, 7 parts of aprotiniies, 700 parts of amylum pregelatinisatums, 20 parts of crospolyvinylpyrrolidone, 10 parts of micropowder silica gels, 10 parts of magnesium stearate, 5~15 parts of coating materials.
Wherein, weightening finish is behind the coating of described tablet: 5~15mg/cm 2, enteric coated tablet hardness be 3~7kgN.
Can carry out being reprocessed into corresponding dosage form behind the full powder coating to material, wherein the coating weightening finish be 5~15mg/cm 2Perhaps material is prepared into granule, to being reprocessed into corresponding dosage form after the granule coating, wherein the coating weightening finish is 5~15mg/cm 2Another kind method is that Thymopentin and absorption enhancer, enzyme inhibitor and enteric material are prepared into liposome jointly, gets after drying liposome micropill (ball) or granule, is prepared into corresponding dosage form by further processing again.
The present invention also provides a kind of preparation method for preparing this oral Thymopentin enteric coated preparation, it is take Thymopentin as active component, adds absorption enhancer, enzyme inhibitor, is pressed into plain sheet, by the enteric coated enteric coatel tablets that are prepared into of coating materials, comprise following concrete steps again:
A, the Thymopentin that takes by weighing following weight proportion and adjuvant:
5~50 parts of Thymopentin, 5~100 parts of absorption enhancers, 7~70 parts of enzyme inhibitors, 10~700 parts of filleies, 0~100 part of disintegrating agent, 0~10 part of lubricant, 0~10 part of fluidizer are crossed respectively the pharmacopeia sieve No. 3, and be for subsequent use;
B, Thymopentin and each the adjuvant equivalent mix homogeneously that progressively increases is surveyed intermediate content, calculates sheet heavy, dry powder direct tabletting, during tabletting the hardness of control strip at 3~7kg N, for subsequent use;
C, preparation coating materials carry out coating to the tablet that has suppressed, and the coating weightening finish is: 5~15mg/cm2, pack and get final product.
The present invention also provides the purposes of this oral Thymopentin enteric coated preparation in the immunoregulatory medicine of preparation.
The present invention also provides a kind of preparation method for preparing this oral Thymopentin enteric coated preparation, it is take Thymopentin as active component, adds absorption enhancer, enzyme inhibitor, is pressed into plain sheet, by the enteric coated enteric coatel tablets that are prepared into of coating materials, comprise following concrete steps again:
A, the Thymopentin that takes by weighing following weight proportion and adjuvant:
5~50 parts of Thymopentin, 5~100 parts of absorption enhancers, 7~70 parts of enzyme inhibitors, 10~700 parts of filleies, 0~100 part of disintegrating agent, 0~10 part of lubricant, 0~10 part of fluidizer are crossed respectively the pharmacopeia sieve No. 3, and be for subsequent use;
B, Thymopentin and each the adjuvant equivalent mix homogeneously that progressively increases is surveyed intermediate content, calculates sheet heavy, dry powder direct tabletting, during tabletting the hardness of control strip at 3~7kg N, for subsequent use;
C, preparation coating materials carry out coating to the tablet that has suppressed, and the coating weightening finish is: 5~15mg/cm2, pack and get final product.
The present invention also provides the purposes of oral Thymopentin enteric coated preparation in the immunoregulatory medicine of preparation.
Oral enteric preparation of the present invention solved well the thymopentin oral administration the time easily become aminoacid, little peptide by the enzymatic degradation in gastric acid, the gastrointestinal and lose activity; Be difficult for to see through gastrointestinal mucosa and bioavailability is very low; Liver oral disposition Thymopentin has the shortcomings such as first pass effect impact.
To sum up, oral enteric preparation of the present invention can solve the problem of thymopentin oral administration, for Thymopentin has increased to new route of administration, prove by the test of pesticide effectiveness, medicine of the present invention has the indication identical with injection and drug effect, for the utilization of clinical Thymopentin preparation provides a kind of new selection to increase patient's compliance.
Description of drawings
Fig. 1 embodiment 2 Thymopentin enteric coatel tablets vitro release curve charts;
Fig. 2 embodiment 6 Thymopentin enteric coated preparation vitro release curve charts;
The little micropill release in vitro of Fig. 3 embodiment 11 Thymopentin colon slowbreaks curve chart.
Obviously, according to foregoing of the present invention, according to ordinary skill and the customary means of this area, not breaking away under the above-mentioned basic fundamental thought of the present invention prerequisite, can also make modification, replacement or the change of other various ways.
The specific embodiment of form is described in further detail foregoing of the present invention again by the following examples.But this should be interpreted as that the scope of the above-mentioned theme of the present invention only limits to following example, all technology that realizes based on foregoing of the present invention all belong to scope of the present invention.
The specific embodiment
The preparation of embodiment 1 Thymopentin enteric coatel tablets of the present invention
(1) plain tablet recipe (per thousand consumptions):
Thymopentin 5g, NaTDC 10g, tristerin 30g, polyacrylic acid crosslinked polymer 10g, aprotinin 7g, microcrystalline Cellulose 100g, carboxymethyl starch sodium 10g, micropowder silica gel 10g, magnesium stearate 10g.
(2) coating materials prescription:
Pulvis Talci 20g, propylene glycol 20g, acrylic resin 60g.
(3) technique of Thymopentin enteric coatel tablets preparation
A, the Thymopentin of getting following weight proportion and adjuvant:
Thymopentin 5g, NaTDC 10g, tristerin 30g, polyacrylic acid crosslinked polymer 10g, aprotinin 7g, microcrystalline Cellulose 100g, carboxymethyl starch sodium 10g, micropowder silica gel 10g, magnesium stearate 10g cross respectively the pharmacopeia sieve No. 3, and be for subsequent use;
B, Thymopentin and each the adjuvant equivalent mix homogeneously that progressively increases is surveyed intermediate content, calculates sheet heavy, and dry powder direct tabletting (hardness of control strip is at 3~7kg N during tabletting) is for subsequent use;
The enteric coating agents that c, usefulness prepare is carried out coating to the tablet that has suppressed, and the coating weightening finish is: 5~15mg/cm 2, packing namely obtains Thymopentin enteric coatel tablets disclosed by the invention.
The preparation of embodiment 2 Thymopentin enteric coatel tablets of the present invention
(1) plain tablet recipe (per thousand consumptions):
Thymopentin 15g, sodium cholate 10g, tristerin 15g, polyacrylic acid crosslinked polymer 10g, pepsin inhibitor 15g, lactose 300g, sodium alginate 20g, micropowder silica gel 10g, magnesium stearate 10g.
(2) coating materials prescription:
Pulvis Talci 20g, propylene glycol 20g, acrylic resin 60g.
(3) technique of Thymopentin enteric coatel tablets preparation: with reference to embodiment 1.
The preparation of embodiment 3 Thymopentin enteric coatel tablets of the present invention
(1) plain tablet recipe (per thousand consumptions):
Thymopentin 50g, NaTDC 20g, tristerin 30g, polyacrylic acid crosslinked polymer 10g, sodium glycocholate 20g, mannitol 700g, low-substituted hydroxypropyl cellulose 50g, micropowder silica gel 10g, magnesium stearate 10g.
(2) coating materials prescription:
Pulvis Talci 20g, propylene glycol 20g, acrylic resin 60g.
(3) technique of Thymopentin enteric coatel tablets preparation: with reference to embodiment 1.
The preparation of embodiment 4 Thymopentin colon slowbreak sheets of the present invention
(1) plain tablet recipe (per thousand consumptions):
Thymopentin 30g, NaTDC 20g, tristerin 20g, polyacrylic acid crosslinked polymer 10g, aprotinin 15g, amylum pregelatinisatum 700g, crospolyvinylpyrrolidone 20g, micropowder silica gel 10g, magnesium stearate 10g.
(NaTDC, glyceryl stearate, polyacrylic acid crosslinked polymer can be as absorption enhancer, and three's consumption adds up in the absorbent amount ranges)
(2) coating materials prescription:
EUDRAGIT S 100 preparation solid contents are 10% coating solution.Wherein antiplastering aid Talc accounts for 50% in the EUDRAGIT polymer, and plasticizer TEC accounts for 10%, and all the other are resin.
(3) technique of Thymopentin colon slowbreak sheet preparation: with reference to embodiment 1.
The preparation of embodiment 5 Thymopentin enteric coated capsulees of the present invention
(1) capsule 's content prescription (per thousand consumptions):
Thymopentin 15g, NaTDC 20g, tristerin 30g, polyacrylic acid crosslinked polymer 10g, aprotinin 20g, micropowder silica gel 10g, starch 700g.
(2) coating materials prescription:
Pulvis Talci 20g, propylene glycol 20g, acrylic resin 60g.
(3) technique of Thymopentin enteric coated capsule preparation
A, the Thymopentin of getting following weight proportion and adjuvant:
Thymopentin 10g, NaTDC 20g, tristerin 30g, polyacrylic acid crosslinked polymer 10g, aprotinin 20g, micropowder silica gel 10g, starch 700g;
B, Thymopentin and each the adjuvant equivalent mix homogeneously that progressively increases is surveyed intermediate content, calculates loading;
C, by the loading that calculates capsule 's content is filled in the capsule;
D, capsule is carried out enteric coating, the coating weightening finish is: 5~15mg/cm 2, packing namely obtains Thymopentin enteric coated capsule disclosed by the invention.
The preparation of embodiment 6 Thymopentin enteric coated capsulees of the present invention
(1) capsule 's content prescription (per thousand consumptions):
Thymopentin 40g, NaTDC 20g, tristerin 30g, polyacrylic acid crosslinked polymer 10g, aprotinin 20g, hydroxypropyl emthylcellulose 5g.
(2) coating materials prescription:
Pulvis Talci 20g, propylene glycol 20g, acrylic resin 60g.
(3) technique of Thymopentin enteric coated capsule preparation: with reference to embodiment 5.
The preparation of embodiment 7 Thymopentin enteric pillers of the present invention (micropill)
(1) medicine layer prescription (per thousand preparation unit's consumptions)
Thymopentin 50g, NaTDC 20g, tristerin 30g, polyacrylic acid crosslinked polymer 10g, aprotinin 20g, hydroxypropyl emthylcellulose 5g.
(2) coating materials prescription:
Antiplastering aid 20g, plasticizer 20g, acrylic resin 60g.
(3) technique of Thymopentin enteric piller (micropill) preparation
A, the Thymopentin of getting following weight proportion and adjuvant:
Thymopentin 50g, NaTDC 20g, tristerin 30g, polyacrylic acid crosslinked polymer 10g, aprotinin 20g, hydroxypropyl emthylcellulose 5g.
B, with the above-mentioned g that respectively organizes with the dissolving of suitable quantity of water or certain density ethanol water, for subsequent use;
C, the blank pill heart is put in the fluid bed, the blank pill heart is carried out the medicine layer coating;
The medicament contg of medicine layer piller (micropill) has been wrapped in d, detection;
E, in fluid bed, above-mentioned piller is carried out enteric coating, namely obtain Thymopentin enteric piller disclosed by the invention (micropill).
The preparation of embodiment 8 Thymopentin enteric coated capsulees of the present invention
Get the prepared Thymopentin enteric piller (micropill) of embodiment 7, need filled capsules according to dosage, namely obtain Thymopentin enteric coated capsule disclosed by the invention.
The preparation of embodiment 9 Thymopentin enteric coatel tablets of the present invention
Get the prepared Thymopentin enteric piller (micropill) of embodiment 7, need to carry out tabletting according to dosage, namely obtain Thymopentin enteric disclosed by the invention and release sheet.
The preparation of embodiment 10 Thymopentin colon slowbreak capsules of the present invention
(1) capsule 's content prescription (per thousand consumptions):
Thymopentin 30g, sodium cholate 20g, tristerin 30g, polyacrylic acid crosslinked polymer 10g, aprotinin 20g, micropowder silica gel 10g, starch 700g.
(2) coating materials prescription:
EUDRAGIT S 100 preparation solid contents are 10% coating solution.Wherein antiplastering aid Talc accounts for 50% in the EUDRAGIT polymer, and plasticizer TEC accounts for 10%, and all the other are resin.
(3) technique of Thymopentin colon slowbreak capsule preparation: with reference to embodiment 5
The preparation of embodiment 11 Thymopentin colon slowbreak pillers of the present invention (micropill)
(1) medicine layer prescription (per thousand preparation unit's consumptions):
Thymopentin 15g, NaTDC 20g, tristerin 30g, polyacrylic acid crosslinked polymer 10g, aprotinin 20g, hydroxypropyl emthylcellulose 5g.
(2) coating materials prescription:
EUDRAGIT S 100 preparation solid contents are 10% coating solution.Wherein antiplastering aid Talc accounts for 50% in the EUDRAGIT polymer, and plasticizer TEC accounts for 10%, and all the other are resin.
(3) technique of Thymopentin colon slowbreak piller (micropill) preparation: with reference to embodiment 7.
The preparation of embodiment 12 Thymopentin colon slowbreak capsules of the present invention
Get the prepared Thymopentin colon slowbreak piller (micropill) of embodiment 11, need filled capsules according to dosage, namely obtain Thymopentin colon slowbreak capsule disclosed by the invention.
Embodiment 13 Thymopentin colon slowbreaks of the present invention are released the preparation of sheet
Get the prepared Thymopentin colon slowbreak piller (micropill) of embodiment 11, need to carry out tabletting according to dosage, namely obtain Thymopentin colon slowbreak disclosed by the invention and release sheet.
The preparation of embodiment 14 Thymopentin colon slowbreak dry suspension of the present invention
Get the prepared Thymopentin colon slowbreak piller (micropill) of embodiment 11, it is carried out the waterproof coating, need to pack according to dosage, namely obtain Thymopentin colon slowbreak dry suspension disclosed by the invention.
The preparation of embodiment 15 Thymopentin enteric coated granules of the present invention
(1) granule prescription (per thousand preparation unit's consumptions):
Thymopentin 50g, NaTDC 20g, tristerin 30g, polyacrylic acid crosslinked polymer 10g, aprotinin 20g, micropowder silica gel 10g, starch 700g, binding agent 10~20g.
(2) coating materials prescription:
EUDRAGIT S 100 preparation solid contents are 10% coating solution.Wherein antiplastering aid Talc accounts for 50% in the EUDRAGIT polymer, and plasticizer TEC accounts for 10%, and all the other are resin.
(3) technique of Thymopentin colon slowbreak granule preparation
A, the Thymopentin of getting following weight proportion and adjuvant:
Thymopentin 50g, NaTDC 20g, tristerin 30g, polyacrylic acid crosslinked polymer 10g, aprotinin 20g, micropowder silica gel 10g, starch 700g.
B, Thymopentin and each the adjuvant equivalent mix homogeneously that progressively increases adds binding agent and makes soft material, by 20~24 mesh standard sieve granulations, and oven dry, granulate.
C, granule is carried out the colon delayed release coat, the coating weightening finish is: 5~15mg/cm 2, survey intermediate content.
D, by the amount of calculating, pack according to taking dose and namely to obtain Thymopentin colon slowbreak granule disclosed by the invention.
The preparation of embodiment 16 Thymopentin colon slowbreak powder of the present invention
(1) granule prescription (per thousand preparation unit's consumptions):
Thymopentin 50g, NaTDC 20g, tristerin 30g, polyacrylic acid crosslinked polymer 10g, aprotinin 20g, micropowder silica gel 10g, starch 700g, binding agent 10~20g.
(2) coating materials prescription:
EUDRAGIT S 100 preparation solid contents are 10% coating solution.Wherein antiplastering aid Talc accounts for 50% in the EUDRAGIT polymer, and plasticizer TEC accounts for 10%, and all the other are resin.
(3) technique of Thymopentin colon slowbreak granule preparation
A, the Thymopentin of getting following weight proportion and adjuvant:
Thymopentin 50g, NaTDC 20g, tristerin 30g, polyacrylic acid crosslinked polymer 10g, aprotinin 20g, micropowder silica gel 10g, starch 700g.
B, Thymopentin and each the adjuvant equivalent mix homogeneously that progressively increases.
C, by fluid bed powder is carried out the colon delayed release coat, the coating weightening finish is: 5~15mg/cm 2, survey intermediate content.
D, by the amount of calculating, pack according to taking dose and namely to obtain Thymopentin colon slowbreak powder disclosed by the invention.
The preparation of embodiment 17 Thymopentin colon slowbreak capsules of the present invention
Get the prepared Thymopentin colon slowbreak powder of embodiment 16, need filled capsules according to dosage, namely obtain Thymopentin colon slowbreak capsule disclosed by the invention.
The preparation of embodiment 18 Thymopentin colon slowbreak sheets of the present invention
Get the prepared Thymopentin colon slowbreak powder of embodiment 16, need to carry out tabletting according to dosage, namely obtain Thymopentin colon slowbreak disclosed by the invention and release sheet.
Embodiment 19 Thymopentin colon slowbreaks of the present invention are released the preparation of sheet
Get the prepared Thymopentin colon slowbreak powder of embodiment 16, by fluid bed powder is carried out the waterproof coating, need to pack according to dosage, namely obtain Thymopentin colon slowbreak dry suspension disclosed by the invention.
Below by concrete physics and chemistry evidence beneficial effect of the present invention.
Embodiment 20 drug coating weight increment tests of the present invention
The present invention increases weight to control position and the time of drug release by coating, so coating weightening finish has certain impact to assimilation effect of the present invention, determines the scope that coating increases weight below by experiment.
Sample thief is an amount of, uses the coating solution for preparing to its coating that carries out different weightening finishes, then sample is carried out drug release determination under different pH value environment, and result's demonstration is worked as the coating weightening finish less than 5mg/cm 2The time, sample idol in the environment of pH value 1 has a small amount of release, and part begins to discharge in the environment of pH value 2~4, discharges rapidly in pH value 5~8 environment, and coating increases weight greater than 15mg/cm 2The time sample in pH value 1~7 environment 2 hours without discharging, in pH value 7.8~8.0 environment in 1 hour without discharging.When coating increases weight at 5~15mg/cm 2The time, sample 2 hours nothings in the environment of pH value 1 discharge, and 2 hours nothings discharge in pH value 2~6.8 environment, discharge rapidly in pH value 7.8~8.0 environment.Therefore in conjunction with absorption site pH value feature of the present invention, selecting the coating weightening finish is 5~15mg/cm 2
Embodiment 21 drug release in vitro degree tests of the present invention
The preparation of embodiment 1-19 preparation is carried out through the vitro release verification experimental verification, all can reach the regulation of 2005 editions enteric coated preparation of Chinese Pharmacopoeia and slowbreak preparation.
Following is each preparation vitro release result of the test of preparation:
Table 1 Thymopentin enteric coated preparation (embodiment 1-19) vitro release result of the test
Can be found out by above data, this product is stable in 2 hours in the 0.1mol/L hydrochloric acid solution, discharges substantially fully in 20 minutes in the phosphate buffer of pH7.0 (seeing Fig. 1).
Table 2 Thymopentin enteric coated preparation (embodiment 1-19) vitro release result of the test 1 (seeing Fig. 2)
Table 3 Thymopentin enteric coated preparation (embodiment 1-19) vitro release result of the test 2 (seeing Fig. 3)
Figure G2006121429420060809D000112
By above data and figure, can find out, medicine of the present invention is nothing release in 2 hours in the 0.1mol/L hydrochloric acid solution, and nothing discharges in 1 hour in the phosphate buffer of pH6.8, only discharges 3.05%, 2 hour and discharges 30.5% in 1.5 hours; Nothing discharges in 1 hour in the phosphate buffer of pH7.8~8.0, discharges 86%, 2 hour and discharges fully in 1.5 hours.
Below beneficial effect by pharmacodynamics test proof medicine of the present invention.
Test example 1 medicine effect test of the present invention
By normal dogs and two kinds of models of preparation immunologic hypofunction dog, measure 2 couples of canine peripheral blood CD4T of embodiment of the invention lymphocyte (being called for short CD4), CD8T lymphocyte (being called for short CD8), CD4/CD8 and lymphocyte transformation ability, positive group is selected thymopentin for injection (tp-5).
Table 4 the present invention is on the impact of normal canine peripheral blood T cell subsets
Group Dosage CD4 CD8 CD4/CD8
Blank group - 40.99±4.05 20.12±3.15 2.08±0.35
The present invention 5mg/ only 42.46±5.51 18.86±2.79 2.31±0.50
2mg/ only 41.92±5.39 19.92±2.83 2.20±0.43
Positive group 0.36mg/ only 44.32±5.71 17.93±3.15 2.60±0.82 *
Annotate: compare * P<0.05 with the blank group
Table 5 the present invention is on the impact of dog Function of lymphocyte transform
Figure G2006121429420060809D000113
Annotate: compare * * P<0.01, * P<0.05 with model group
Table 6 the present invention is on dog t lymphocyte subset group's impact
Figure G2006121429420060809D000121
Annotate: compare * * P<0.01 with model group
Experimental result shows: model group and blank group compare, and lymphocyte transformation ability, CD4, CD4/CD8 all significantly reduce; CD8 significantly raises, and shows that the immunomodulating of ASP group canine cells strengthens relatively, immunologic function degression, and namely the intravenous injection ASP can cause the dog immunodeficiency models.And positive drug group (thymopentin for injection (tp-5)) and model group are relatively, lymphocyte transformation ability, CD4/CD8 significantly rise, CD8 significantly descends, but show the dog immunocompromised effect that thymopentin for injection (tp-5) antagonism ASP causes, and have the forward immunoregulation effect; For normal beagle dog, thymopentin for injection (tp-5) has certain immunological enhancement equally.And the present invention all has and the identical pharmacological action of positive drug (thymopentin for injection (tp-5)) from above experimental result, when dosage of the present invention is 5-15 times of positive drug, demonstrates similar immunoregulation effect.Because safety non-toxic during thymopentin oral, according to thymopentin for injection (tp-5) dosage (1mg/ preparation unit and 10mg/ preparation unit), the every preparation unit dose of the present invention is decided to be 5~150mg/ preparation unit.The further preferable range of Thymopentin consumption is 15~30mg/ unit, preliminary test proves according to pharmacodynamics, when being 15 times of injection, the thymopentin oral consumption shows immunological enhancement, the dosage of injection is 1mg/ unit, show that when 1~2 times of consumption immunological enhancement is optimum, therefore preferred oral dosage is 15~30 times of injection, i.e. 15~30mg/ unit.
Above-mentioned pharmacodynamics test explanation, medicine of the present invention has the indication identical with injection and drug effect, well solved the problem of thymopentin oral administration, for Thymopentin has increased to new route of administration, increased patient's compliance, for the utilization of clinical Thymopentin preparation provides a kind of new selection.

Claims (2)

1. oral Thymopentin enteric coated preparation, it is characterized in that: described preparation is enteric coatel tablets, and it is that the Thymopentin and the adjuvant that contain the following weight proportioning are prepared from: 15 ~ 50 parts of Thymopentin, 5 ~ 30 parts of NaTDCs, 15 ~ 30 parts of tristerins, 10 ~ 20 parts in polyacrylic acid crosslinked polymer, 7 ~ 70 parts of aprotiniies, 10 ~ 700 parts of amylum pregelatinisatums, 20 ~ 100 parts of crospolyvinylpyrrolidone, 2 ~ 10 parts of micropowder silica gels, 2 ~ 10 parts of magnesium stearate, 5 ~ 15 parts of coating materials; Perhaps, 5 parts of Thymopentin, 10 parts of NaTDCs, 30 parts of tristerins, 10 ~ 20 parts in polyacrylic acid crosslinked polymer, 7 parts of aprotiniies, 700 parts of amylum pregelatinisatums, 20 parts of crospolyvinylpyrrolidone, 10 parts of micropowder silica gels, 10 parts of magnesium stearate, 5 ~ 15 parts of coating materials;
Wherein, coating materials is mixed and is formed by 1 ~ 5 part of antiplastering aid, 0.4 ~ 3 part of plasticizer, 3.6 ~ 7 parts of threes of enteric solubility adjuvant, and described antiplastering aid is Pulvis Talci, and plasticizer is propylene glycol or triethyl citrate, and the enteric solubility adjuvant is acrylic resin.
2. oral Thymopentin enteric coated preparation as claimed in claim 1 is characterized in that: weightening finish is behind the coating: 5 ~ 15mg/cm 2, enteric coated tablet hardness be 3 ~ 7KgN.
3, a kind of preparation method for preparing oral Thymopentin enteric coated preparation claimed in claim 1, it is take Thymopentin as active component, adds absorption enhancer, enzyme inhibitor, is pressed into plain sheet, by the enteric coated enteric coatel tablets that are prepared into of coating materials, comprise following concrete steps again:
A, get Thymopentin and adjuvant by weight ratio:
B, Thymopentin and each the adjuvant equivalent mix homogeneously that progressively increases is surveyed intermediate content, calculates sheet heavy, dry powder direct tabletting, during tabletting the hardness of control strip at 3 ~ 7KgN, for subsequent use;
5 ~ 15 parts of c, preparation coating materials, wherein, coating materials is the adjuvant that contains the following weight proportioning: 1 ~ 5 part of antiplastering aid, 0.4 ~ 3 part of plasticizer, 3.6 ~ 7 parts of enteric solubility adjuvants, described antiplastering aid is Pulvis Talci, plasticizer is propylene glycol or triethyl citrate, the enteric solubility adjuvant is acrylic resin, and the tablet that has suppressed is carried out coating, and the coating weightening finish is: 5 ~ 15mg/cm 2, pack and get final product.
4, the purposes of oral Thymopentin enteric coated preparation claimed in claim 1 in the immunoregulatory medicine of preparation.
CN2006100214294A 2006-07-20 2006-07-20 Thymus gland pentapeptide oral intestine-dissolved formulated product and method of preparing the same and use thereof Active CN101108246B (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
CN2006100214294A CN101108246B (en) 2006-07-20 2006-07-20 Thymus gland pentapeptide oral intestine-dissolved formulated product and method of preparing the same and use thereof

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
CN2006100214294A CN101108246B (en) 2006-07-20 2006-07-20 Thymus gland pentapeptide oral intestine-dissolved formulated product and method of preparing the same and use thereof

Publications (2)

Publication Number Publication Date
CN101108246A CN101108246A (en) 2008-01-23
CN101108246B true CN101108246B (en) 2013-03-06

Family

ID=39040634

Family Applications (1)

Application Number Title Priority Date Filing Date
CN2006100214294A Active CN101108246B (en) 2006-07-20 2006-07-20 Thymus gland pentapeptide oral intestine-dissolved formulated product and method of preparing the same and use thereof

Country Status (1)

Country Link
CN (1) CN101108246B (en)

Families Citing this family (5)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN104861046A (en) * 2015-06-02 2015-08-26 河北科技大学 N-methyl cyclic pentapeptide compound as well as synthetizing method and application thereof
CN105288583A (en) * 2015-11-13 2016-02-03 海南森瑞谱生命科学药业股份有限公司 Oral thymopentin preparation and preparation method thereof
CN105709208A (en) * 2016-01-29 2016-06-29 陕西科技大学 Preparation technology of bitter gourd protein enteric-coated tablets
CN109575100A (en) * 2018-10-25 2019-04-05 大连大学 Glycocholic acid application in preparation of anti-tumor drugs
CN113058039A (en) * 2019-12-14 2021-07-02 苏州兰鼎生物制药有限公司 Oral medicine composition of thymalfasin or thymopentin

Citations (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN1714861A (en) * 2004-06-28 2006-01-04 中国医学科学院药物研究所 Thymus penta peptide slow releasing micro ball and preparation method thereof

Patent Citations (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN1714861A (en) * 2004-06-28 2006-01-04 中国医学科学院药物研究所 Thymus penta peptide slow releasing micro ball and preparation method thereof

Non-Patent Citations (2)

* Cited by examiner, † Cited by third party
Title
Jing Wang等.Pharmacokinetics, toxicity of nasal cilia and immunomodulating effects in Sprague–Dawley rats following intranasal delivery of thymopentin with or without absorption enhancers.《PEPTIDES》.2005,第27卷826-835. *
JingWang等.Pharmacokinetics toxicity of nasal cilia and immunomodulating effects in Sprague–Dawley rats following intranasal delivery of thymopentin with or without absorption enhancers.《PEPTIDES》.2005

Also Published As

Publication number Publication date
CN101108246A (en) 2008-01-23

Similar Documents

Publication Publication Date Title
CN102325526B (en) Extend the pharmaceutical preparation of release
JP6608319B2 (en) Abuse resistant pharmaceutical composition, method of use and preparation
US8703186B2 (en) Abuse-resistant oral dosage forms and method of use thereof
US7374781B2 (en) Sustained release formulations containing acetaminophen and tramadol
EP0941071B1 (en) Gastric-retentive, oral drug dosage forms for the controlled-release of sparingly soluble drugs and insoluble matter
ES2207977T3 (en) COMPOSITIONS EPLERENONA MICRONIZED.
US10555907B2 (en) Controlled-release solid dosage forms of mesalamine
KR102094631B1 (en) Modified release composition of orlistat and acarbose for the treatment of obesity and related metabolic disorders
CN101108246B (en) Thymus gland pentapeptide oral intestine-dissolved formulated product and method of preparing the same and use thereof
KR101858797B1 (en) Pharmaceutical compositions comprising hydromorphone and naloxone
JP2002521346A (en) Colon-selective drug delivery composition and pharmaceutical preparation utilizing polysaccharide
JP2002537321A5 (en)
JP2004501099A (en) Aldosterone antagonist composition for release during aldosterone vertex phase
CN103417544B (en) First ammonia folic acid compound preparation and its production and use
CN101380461B (en) Efficient thymosin enteric-coated tablets and thymosin for injection
US20020132002A1 (en) Sustained release pharmaceutical formulation
EP2340017A2 (en) Treatment of adrenal insufficiency
CN101023951A (en) Slow-released preparation containing hydrochlorothiazide and clonidine hydrochloride and its preparing method
CN104013634A (en) Capsule containing aspirin enteric part and dipyridamole quick-releasing part and preparation method thereof
CN101502516B (en) Glipizide enteric-coated formulation composition and method for preparing the same
CN101623287B (en) Novel drospirenone analogue medicinal composition for treating menopausal syndrome

Legal Events

Date Code Title Description
C06 Publication
PB01 Publication
C10 Entry into substantive examination
SE01 Entry into force of request for substantive examination
C14 Grant of patent or utility model
GR01 Patent grant