RU2063227C1 - Medicinal agent for cardiovascular disease treatment and method of its preparing - Google Patents

Abstract

FIELD: medicine, pharmacy. SUBSTANCE: proposed agent has adenosine and riboxine at the following ratio, mas. p.: adenosine 1, and riboxine 1.5-2.5. Medicinal agent is prepared by dissolving adenosine and riboxine at heating, solution is kept at 50-65 C for 5-15 min, cooled and pH value is brought about to 6-8. Then solution is filtered, dosed into ampoules, sealed and sterilized. EFFECT: enhanced therapeutic effectiveness, stability at storage as an aqueous solutions.

Description

 The invention relates to medicine and the medical industry, in particular, to medicines intended for the treatment of cardiovascular diseases, as well as to the production of medicines of purine-containing compounds.

 It is known the use of an adenosine derivative as a cardiovascular drug, is issued in medical practice in the form of a solution of sodium adenosine triphosphate (ATP) 1 for intramuscular injection in ampoules (1), taken as a prototype.

 The inventive drug contains adenosine and riboxin (inosine) in certain proportions (mass parts): adenosine 1, riboxin 1.5-2.5. The combined use of adenosine and riboxin in a certain ratio made it possible to potentiate and prolong the effects of adenosine on the cardiovascular system, including with intramuscular injection. With experimental radiation, the claimed lek. The product was superior to the drug based on ATP phosphobion chemist company manufactured in Romania. In experimental myocardial infarction in rats in a chronic experiment, the claimed lek. Agent had a therapeutic effect in doses of 10 and 1 mg / kg of the animal’s weight (intramuscularly, for 30 days), exceeding the effect of phosphobion in doses of 30 and 3 mg / kg, respectively. The claimed lek.redstvo increased the survival of animals, normalized the level of ATP and creatine phosphate (CF) in the myocardium and reduced the size of the infarction zone (Table 1).

 In experimental myocarditis in rats caused by the introduction of adrenaline, the claimed lek. when administered intramuscularly at a dose of 10 mg / kg of the animal’s mass by 14 days, it significantly increased the survival of animals, normalized the content of ATP and CF in the myocardium, reduced myocardial hypertrophy, while the effect was achieved when the dosage of the claimed drug was 3 times lower compared to phosphobion ( table 2). The inventive drug is a low toxicity drug. When administered intramuscularly to mice at a dose of 5 mg / kg and rats at a dose of 10 mg / kg, which is 2 orders of magnitude higher than the therapeutic dose for humans, the death of animals, changes in their condition, appearance and behavior were not observed.

 It is known that nucleosides, in particular, adenosine and riboxin, are slightly soluble in water, the maximum concentration of adenosine reaches only 0.5 riboxin 1.6 These concentrations are insufficient to provide therapeutic dosages, solutions are aggregatively unstable. The solubility of these substances increases significantly only at extreme pH values, however, the use of such strongly acidic or alkaline salts in medical practice is impossible; nucleosides in such solutions, when heated, undergo acid or alkaline hydrolysis with cleavage of the heterocyclic base.

 Known methods for increasing the solubility of inosine by obtaining complexes with citrates, diethyl barbiturates; by dissolving in buffer solutions of alkali metal phosphates. A method for producing a concentrated solution of inosine using an aliphatic amine, diamine or alicyclic amine with less than six carbon atoms as a solubilizer is described, which is adopted as a technical prototype. The prototype method is as follows. Diethylamine and distilled water are added to the calculated amount of inosine (riboxin), heated, diluted with water to the required volume, ampouled, sterilized.

 The known method of the prototype is not suitable, since it does not increase the solubility of adenosine, as a result of which the required ratio of nucleosides and therapeutic efficacy are not achieved in the drug.

 In the course of the study, it was found that in aqueous solutions adenosine and riboxin in the claimed proportions have synergistic solubility (increase the solubility of each other). The optimal ratios at which the highest concentrations of adenosine and riboxin are observed are 1: 1.5-2.5, while the solubility of adenosine increases 5-6 times, riboxin 3-4 times compared with the solubility of individual substances.

In the claimed method for producing a medicinal product, including filtering an aqueous solution of nucleosides, dosing into ampoules, sealing and sterilizing the ampoules, the solution is prepared as follows: adenosine and riboxin are dissolved in water when heated, kept at a temperature of 50-65 ^o C for 10-15 min, cooled to room temperature and set the pH of the solution in the range from 6 to 8. The properties of the claimed drug and prototype are presented in table.3.

To obtain the claimed lek.redstva used a glass reactor with a stirrer and a jacket for heating with a capacity of about 1.5 liters. When heated, 0.8 g of adenosine and 20 g of riboxin were dissolved in 0.8 L of water for injection, kept at a temperature of 50 to 65 ^o C for 10-15 minutes, cooled to room temperature, and the pH of the solution was adjusted from 6 to 8. Volume adjusted with water for injection to 1 liter The resulting drug solution was filtered, dosed into ampoules, ampoules were sealed and sterilized. The yield of the finished product is 90-95
The claimed pH range is due to the requirement that the drug should be as neutral as possible. The ratios of the active ingredients (adenosine and roboxin) are due to the therapeutic efficacy of the drug and its stability during storage. The rationale for the ratios of the main ingredients of the drug is presented in table. 3 and 4.

 When the amount of riboxin is less than 1.5 hours and more than 2.5 hours per 1 hour of adenosine, the aggregative stability of nucleosides decreases during long-term storage, and the pharmacological effect in experimental pathology of the animal cardiovascular system decreases.

 Examples of specific performance.

Example 1. In a glass reactor with a capacity of 1 l, equipped with a stirrer and a jacket for heating, load 0.7 l of water for injection, dissolve in it with heating 8 g of adenosine and 16 g of riboxin, set the temperature to 58-60 ^o C and continue stirring at At this temperature for 10 minutes, the solution was cooled and the pH was adjusted to 6.6. The volume of the solution was adjusted with water for injection to 0.8 liters. The resulting solution is filtered, poured into ampoules of 2 ml, the ampoules are sealed and sterilized. Get 370 ampoules of the finished product.

Example 2. In a glass reactor with a capacity of 1.5 l, equipped with a stirrer and a jacket for heating, load 1 l of water for injection and dissolve in it with heating 12 g of adenosine, 21.6 g of riboxin, set the solution temperature to 55-57 ^o C and continue to mix at this temperature for 10 minutes, the solution is cooled and the pH is adjusted to 7.0, the volume is adjusted with water for injection to 1.2 L. The solution is filtered, poured into ampoules of 2 ml, the ampoules are sealed and sterilized. Get 565 ampoules of the finished product.

Example 3. In a glass reactor with a capacity of 1 l, equipped with a stirrer and a jacket for heating, download 0.7 l of water for injection, in the indicated volume of water, dissolve 8 g of adenosine and 17.6 g of riboxin with heating, set the solution temperature to 60-62 ^o C, stirring is continued at this temperature for 15 minutes, the solution is cooled and the pH is adjusted to 7.5. The volume of the solution was adjusted with water for injection to 0.8 L, the solution was filtered, poured into 2 ml ampoules, the ampoules were sealed and sterilized. Get 370 ampoules of the finished product. TTT1 TTT2 TTT3 TTT4

Claims (1)

 1. The drug for the treatment of cardiovascular diseases based on adenosine, characterized in that it further comprises riboxin in the following components, wt.h. Adenosine 1
Riboxin 1.5 2.5
2. A method of obtaining a medicinal product for the treatment of cardiovascular diseases by preparing a drug solution, followed by filtering it, dosing into ampoules, sealing ampoules, sterilization, characterized in that adenosine and riboxin are dissolved in water when heated, kept at 50 65 ^o C for 10-15 minutes, cool and set the pH to 6-8.

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