RU2036642C1 - Process for manufacture of long-acting broncholithic medicinal composition based on theophylline - Google Patents

Abstract

FIELD: medicine; pharmaceutical industry. SUBSTANCE: this process includes such steps as admixing of theophylline with interpolymer complex of polymethacrylic acid and polyethyleneglycol, wetting admixture by interpolymer complex solution in phosphate buffer, alcohol or water-alkali solution at pH value of 4.5 to 7.5, subjecting resulting stock to water-stream granulation, drying this stock, and finally carrying out subsequent steps of manufacture of finished medicinal form. According to another version, tablets may be manufactured by method of briquetting. Tablets are coated with film-forming solution based on same interpolymer complex. Medicinal preparation manufactured by disclosed method is effective when administered in dose of 450 to 600 mg/24 h and maintains therapeutic concentration of theophylline in plasma by two intakes. Mean absorption time is 12 h. EFFECT: more prolonged period of maintaining of effective concentration of medicinal preparation in blood. 3 cl, 3 tbl

Description

 The invention relates to medicine, and more specifically to a method for producing prolonged-acting theophylline tablets, which are used in medicine as a bronchodilator in all forms of bronchial obstruction: bronchial asthma, chronic obstructive bronchitis, obstructive enphysema and others.

 Currently, there is a wide variety of theophylline-based sustained release bronchodilator drug compositions containing various polymeric carriers of natural and synthetic origin, obtained by various technological methods: microencapsulation, microgranulation, tablet compression and others. These are well-known drugs manufactured by leading companies in various countries, such as Quibron, Slophillin, Teostat, Bronchoretard. "Teo-24." "Teo-Dur".

 A known method of obtaining a bronchodilator drug composition of prolonged action containing encapsulated theophylline, polyvinylpyrrolidone, sugar, ethyl cellulose. The drug in the form of tablets is obtained by applying a solution of theophylline with polyvinylpyrrolidone on sugar granules with a diameter of 0.71-0.84 mm, followed by evaporation of the solvent. The obtained theophylline-containing granules are coated with a solution of ethyl cellulose in ethyl alcohol. Granules are mixed with lactose and tableted, hydrogenated vegetable oil is used as a lipid coating. By changing the ratio of polyvinylpyrrolidone to cellulose, various dissolution rates are achieved. In patients after taking the indicated drug, a constant therapeutic concentration of theophylline in the blood is achieved for 12 hours. This drug is characterized by a large mass of auxiliary substances used and the complexity of the technological process for its preparation.

There is also a method of obtaining a medicinal composition based on theophylline of the following composition (in tablets), mg: Theophylline monohydrate 330
Oxypropylmethyl cellulose (100 cP) 92
Oxypropylmethyl cellulose (15,000 cps) 25 Lactose 80 Magnesium stearate 5 Silicon dioxide 3
The specified method consists in mixing the starting ingredients with subsequent tableting, and the composition is characterized by multicomponent and a large mass of excipients.

A known method of obtaining a medicinal composition based on theophylline, the following composition (in tablets), mg: Theophylline 300
Disubstituted Calcium Phosphate 300
Acetylphthalyl cellulose 30 Ethyl cellulose 30 Magnesium stearate 4.6
The specified method consists in mixing theophylline with disubstituted calcium phosphate. The resulting mixture is moistened with a solution of acetylphthalyl cellulose and ethyl cellulose in a mixture of organic solvents (50 ml of isopropyl alcohol and 150 ml of methylene chloride) and a granulate is obtained, which is dried, dusted (magnesium stearate) and tableted. A stable concentration of theophylline in the blood is provided for 12 hours. The resulting composition is characterized by multicomponent and high content of excipients (55% by weight of the tablet). In addition, the use of toxic fire and explosive organic solvents in the method for producing said composition complicates the process technology and requires additional equipment.

 Closest to the proposed technical essence and the achieved effect are theophylline tablets of prolonged action based on polyvinyl chloride and the method for their preparation. The tablets consist of a polymer matrix that provides controlled release of a single therapeutic dose of theophylline for about 8 hours. The tablets contain a therapeutically effective amount of about 100-1000 mg of anhydrous theophylline, 5-15 wt. polyvinyl chloride (PVC), based on the weight of the tablet, and 0-2 wt. hydrophobic rolling.

The method comprises wet granulation of theophylline using a solvent containing ethyl alcohol, drying the granules at ¹¹⁰ ° C for 20-30 minutes, PVC moist granulation using a solvent containing ethyl alcohol and methylene chloride in an equal volume ratio, drying the granules at a temperature of PVC below 90 ^about C, mixing theophylline granules and PVC, optionally adding a sliding, for example magnesium stearate, re-mixing and pressing. The disadvantage of this technology is the use of organic solvents, which requires the protection of personnel from harmful vapors, as well as equipment for fire and explosion-proof measures.

 The aim of the invention is to remedy these disadvantages.

 This goal is achieved using a method of obtaining a bronchodilator composition of prolonged action, including mixing theophylline with a polymer matrix, introducing a moisturizing agent, granulating, drying the resulting mixture, followed by obtaining a dosage form, characterized in that an interpolymer complex of polymethacrylic acid and polyethylene glycol is used as a polymer matrix, the moisturizing agent is water or 5-15 wt. a solution of the interpolymer complex pH 4.5-7.5 in an aqueous alkaline solution, phosphate buffer or ethyl alcohol.

 It was found that if a solution of the interpolymer complex in phosphate buffer, in an aqueous alkaline medium, or in ethanol is used as a wetting agent, such technological parameters of granules as bulk density and flowability are improved, and the quality of the finished tablets is also improved. The same goal, as it turned out, can be achieved using another variant of the method, which consists in mixing theophylline and the interpolymer complex of polymethacrylic acid and polyethylene glycol in a dry state, then the mixture is briquetted, granulated by grinding, the obtained granules are dusted with magnesium or calcium stearate, and tableted.

 In both cases, in order to mask the bitter taste of the dosage form in the form of tablets and to increase the duration of the drug in the body, protective polymer coatings obtained from solutions of 5-15 wt. the same interpolymer complex, 0-4.5 wt. caustic soda or sodium bicarbonate, 1-5 wt. Tween-80 with the addition of 0-2 wt. titanium dioxide in distilled water or ethyl alcohol.

 In the table. 1 shows the technological characteristics of granules obtained according to the first embodiment of the proposed method, which prove the effectiveness of the use of CPN solutions as a moisturizing agent. Theophylline release rates are presented in table. 2.

 The inventive method allows for simplified technology to obtain the target product of high quality. The method is simple to implement, does not require the use of special equipment. The resulting bronchodilator drug composition has the pharmacological properties inherent in theophylline. The bronchodilator effect of the claimed drug develops gradually 3-6 hours after administration. Theophylline is dosed from the polymer matrix, which ensures a constant concentration of theophylline in the blood for 12-24 hours. A stable clinical effect is achieved after several days of treatment.

 Studies of the chronic toxicity of the composition prepared by the proposed method, conducted in experiments on dogs, showed that the drug when administered orally at a dose of 100 mg / kg for 6 months. does not cause any changes in the behavior of animals, weight gain, peripheral blood, as well as indicators of pathological and morphological studies of organs and tissues of experimental dogs.

 In the clinic, the drug is tested in comparison with the famous drug Theodur. Particular attention was paid to pharmacokinetic studies. Using strictly selected by age, weight, disease severity groups of patients, theophylline concentrations in the blood were determined by high performance liquid chromatography at 1, 2, 6, 9, 12 and 24 hours after taking a dose of 300 mg of the drug prepared by the present method, and also collected urine in the intervals of 0-6, 6-12 and 12-24 hours

 The results of calculations of pharmacokinetic parameters are presented in table. 3.

 Slow absorption of theophylline from prolonged forms is clearly seen when comparing the independent parameter "average absorption time". For a preparation prepared by the present method, the average absorption time is 12 hours, for theodur slightly less than 8.2 hours, for ordinary theophylline tablets, this parameter is only 1.4 hours. A similar ratio is obtained when comparing the absorption time of 75% of the dose. As a result of complete, but slow absorption, a significant increase in the duration of theophylline circulation occurs when taking prolonged forms. The integral parameter characterizing the "average retention time" of a drug substance in the body for a composition prepared by the present method is 21 hours on average, 16.8 hours for theodur tablets.

 Clinical examination in 95% of patients already on the 4-5th day of taking the composition showed an improvement in overall health, decreased the number and intensity of asthma attacks during the day, increased physical activity, decreased intensity, as well as the disappearance of nocturnal asthma attacks.

 As a result of a long clinical study of the composition, it was found that the drug is highly effective at a dose of 450-600 mg / day, is able to maintain a therapeutic concentration of theophylline in plasma at a 2-fold dose, to control bronchial patency for a long time, and reduce the need for other groups of medications used in treatment of bronchial asthma. The state of stable equilibrium of theophylline plasma concentration correlates with an improvement in the clinical condition of patients, which manifests itself in an increase in physical activity, a decrease in the frequency and intensity of asthma attacks, the disappearance of night attacks of dyspnea, as well as a decrease in the patient's need for inhaled sympathomimetics and systemic corticosteroids.

PRI me R 1. In the mixer load 3.0 kg of theophylline and 1.0 kg of the interpolymer complex, mix. To the resulting mixture was added 500 ml of a 10% solution of the interpolymer complex in phosphate buffer pH 7.5, with stirring. Then carry out wet granulation and drying of the granular mixture at a temperature of 50-60 ^about C to a residual moisture content of granulate 1-2% The yield of the finished product is 97 wt. The dried granular mixture was dusted with calcium stearate and tabletted.

 PRI me R 2. The process is carried out analogously to example 1, using as a moisturizing agent a 5% solution of the interpolymer complex in a 1.5% aqueous solution of sodium bicarbonate, the pH of the resulting solution of the complex is 4.5. The dried granular mixture was dusted with calcium stearate and tabletted.

 PRI me R 3. The process is carried out analogously to example 1, using as a moisturizing agent a 15% solution of the interpolymer complex in ethyl alcohol.

 PRI me R 4. In the mixer load 3.0 kg of theophylline and 1.0 kg of the interpolymer complex of polymethacrylic acid and polyethylene glycol, mix. The resulting mixture is briquetted, then granulation is carried out by grinding, obtaining granules with a size of 0.05-1.5 mm The granular mixture is dusted with calcium stearate and tabletted. Get tablets containing 0.1; 0.2; 0.3 g of theophylline each.

 Example 5. 3.0 kg of theophylline granulate and 0.98 kg of an interpolymer complex of polymethacrylic acid and polyethylene glycol are loaded into the mixer, mixed. The resulting mixture is briquetted, then granulation is carried out by grinding, obtaining granules with a size of 0.05-1.5 mm The granular mixture is dusted with calcium stearate and tabletted. Get tablets containing 0.1; 0.2; 0.3 g of theophylline each.

PRI me R 6. In the mixer load 3.0 kg of theophylline and 1.0 kg of the interpolymer complex is mixed. To the resulting mixture was added 500 ml of a 10% solution of an interpolymer complex of pH 7.5 in a solution of sodium hydroxide with stirring. Wet granulation is then carried out, and drying the granulated mixture at a temperature of 50-60 ^C to a residual moisture of 1-2% granulate Yield is 97 wt. The dried granular mixture was dusted with calcium stearate and tabletted. The resulting tablets are coated with a film-forming solution of the following composition, g / l:
Specified interpolymer complex 100 Caustic soda 20 Tween-80 10 Distilled water Up to 1 l
500 g of tablets are loaded into the hopper of the installation for coating in a fluidized bed. The coating is carried out at a temperature of the airflow at the inlet to 40-50 ^{° C,} exhaust air temperature of 20-30 ^{° C,} the coating film-forming rate of 10-20 ml / min or coating of tablets is carried out using a film-forming solution of the following composition, g / l:
Specified interpolymer complex 100 Tween-80 20 Ethyl alcohol Up to 1 L

Claims (3)

 1. METHOD FOR PRODUCING A BRONCHOLYTIC MEDICINAL COMPOSITION OF A LONG-TERM ACTION BASED ON THEOPHYLLIN, including mixing theophylline with a polymer matrix, moistening, granulation, drying and tabletting, characterized in that the polymeric polymethylene glycol polymethylene glycol (IPIC) is used as a polymer matrix and polymethylene glycol 5 a 15% solution of the same IPC with a pH of 4.5 to 7.5 in phosphate buffer, or in an aqueous-alkaline solution, or in ethanol.  2. A method of producing a theophylline-based prolonged-release bronchodilator drug composition, comprising mixing theophylline with a polymer matrix, granulation and tabletting, characterized in that IPC polymethacrylic acid and polyethylene glycol are used as the polymer matrix and the dosage form is obtained by dry granulation.  3. The method according to PP. 1 and 2, characterized in that the tablets are coated with a film-forming solution based on the specified IPC.

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