UA63137A - FORIDON-GEL û REMEDY FOR TREATING AND PREVENTING CARDIOVASCULAR DISEASES - Google Patents

Abstract

The remedy for treating the cardiovascular diseases comprises Foridon as an active ingredient and pharmaceutically acceptable carrier, namely the gel base.

Description

Description of the invention

The invention relates to medicine and the chemical and pharmaceutical industry, in particular, to the creation, 2 production and use of means for the treatment of cardiovascular diseases.

A well-known remedy for the treatment of cardiovascular diseases "Ointment "Nitro", containing 295 nitroglycerin and an ointment base (arafin, ethanol, oxypropyl cellulose, petroleum jelly). The ointment belongs to drugs of prolonged action (the effect appears after 30-4 hours and continues for 2-5 hours) and is prescribed as an additional means for the prevention of angina attacks in combination with nitrates used orally (1). 70 The well-known medicine "Izomak" in the form of a spray containing 1.25 mg of the active substance isosorbide dinitrate in one dose ( 200 doses in a bottle). "Izomak" is used as an anti-anginal agent (2).

The well-known cardiovascular drug "Isoket" in the form of tablets containing 20, 40 and 100 mg of isosorbide dinitrate; in the form of an aerosol (300 doses in a bottle with a capacity of 15 ml for 1.25 mg of the active substance in one dose); In the form of a solution for infusions (0.195 of the active substance in an ampoule of 10 ml); in the form of a cream (50 g each in a bottle of 12 containing 100 mg of the active substance in 1 g of ointment). "Izoket" is used as an anti-anginal agent (3).

The well-known remedy "Digoxin" for the treatment of diseases of the cardiovascular system in the form of tablets of 0.00025 g, 0.0001 g and in the form of 0.02595 injection solution in ampoules of ml. The tool is used in the treatment of heart failure, it has a high cardiotonic effect. A significant disadvantage of "Digoxin" is a fairly large range of contraindications, in particular, the presence of a cumulative effect with long-term use, which leads to significant disturbances in the activity of the cardiovascular system (4).

The well-known cardiovascular drug "Digitoxin" is available in the form of tablets of 0.0001 g and in the form of suppositories of 0.00015 g. The tool is used for heart failure, which requires long periods of treatment, especially with a tendency to tachycardia. "Digitoxin" has a high cardiotonic effect, the dose of the drug and the duration of treatment with it must be strictly individualized, because due to the cumulative properties of the drug, 22 patients have side effects that are characteristic of overdose and long-term use of "the drug, which leads to to severe disorders of the cardiovascular system (5).

The drug "Foridon" in the form of tablets containing 0.01 g of the active ingredient foridon (2,6-dimethyl-3,5-dimethoxycarbonyl-4-(-2-difluoromethoxyphenyl)-1,4-dihydropyridine) is the closest to the claimed agent. ), and a pharmaceutically acceptable carrier. Foridon belongs to the antagonists of calcium ions, it is used as a hypotensive, antispasmodic, coronary dilator in the treatment of diseases of the cardiovascular system. The term of treatment with Foridon depends on the severity of the disease and can be several months.

The initial therapeutic effect occurs at the end of the first week, lasting after 2-3 weeks. The half-life of the drug from the body is 2-4 hours. It is taken internally three times a day, the daily dose is up to 150 mg. "95

Possible side effect in the form of facial redness, headache, tachycardia, which passes after reducing the dose or canceling the drug (b). eh

The shortcomings of the prototype include the short duration of its action (the half-life of the drug from the body is 2-4 hours), a side effect in the form of facial redness, headache, tachycardia, which passes after reducing the dose or canceling the drug. To a large extent, such manifestations can be attributed to the "negative properties of the dosage form of foridon - tablets, which is a short-acting form, and which is not sufficiently acceptable for preparations based on calcium antagonists due to the rapid rise and fall of the concentration of the active substance in blood plasma and reflex reactions accompanying this phenomenon (see

From" recommendations of the Cardiology Research Center of the Russian Academy of Sciences: New Medical Journal. - 1996. - Mo3-4. - P.12-16).

Thus, one of the reasons that prevent the prototype from obtaining the technical result achieved in the claimed invention is that its qualitative and quantitative composition does not allow to achieve a high level of prolongation of specific activity, reduce or eliminate negative side effects. b The invention is based on the task of creating a means based on phoridone in the form of a gel, the qualitative and quantitative composition of which would allow to achieve a high level of prolongation of specific activity, reduce or eliminate the negative side effects of the drug. - The task is solved by the fact that the remedy for the treatment of cardiovascular diseases contains

Ge) 20 active substance foridone and a pharmaceutically acceptable carrier, according to the invention, as a pharmaceutically acceptable carrier, a gel base is used with this ratio of components, wt. 90: phoridon (ФСА2У-4/37-1307-01) 3.00-6.00 gel base, the rest of» The task is also solved by the fact that, according to the invention, the gel base contains a thickener, non-aqueous hydrophilic solvents, hydrophobic solvents, preservative, neutralizing agent, emulsifier and purified water.

The task is also solved by the fact that, according to the invention, carbomer 60, or sacap, or axam is used as a thickener.

The task is also solved by the fact that, according to the invention, glycerin, or polyethylene oxide-200, or polyethylene oxide-400, or polyethylene oxide-600, or propylene glycol, or dimethyl sulfoxide, or ethyl alcohol, or propyl alcohol are used as non-aqueous hydrophilic solvents. or their mixtures.

The task is also solved by the fact that, according to the invention, vaseline oil, or sunflower oil, or olive oil, or peach oil, or sesame oil, or castor oil, or dimethicone are used as hydrophobic solvents.

The task is also solved by the fact that, according to the invention, formaldehyde solution, or nipagin, or nipazol, or triclosan, or their mixtures are used as a preservative.

The task is also solved by the fact that, according to the invention, as a neutralizing agent

Use 15-2595 solution of ammonia, or sodium hydroxide, or potassium hydroxide, or triethanolamine, or ethanolamine, or diisopropanolamine, aminomethylpropanol, or tris(hydroxypropylethylenediamine), or ethoxylated fatty aliphatic amines, or sodium hydroxymethylglycinate, or sodium tetraborate, or trometamol.

The task is also solved by the fact that, according to the invention, tween-80, 70 or tween-60, or tween-40, or pemulene is used as an emulsifier.

The task is also solved by the fact that, according to the invention, the carbomer is polyacrylic acid or its resins.

The technical result obtained by the implementation of the invention consists in achieving a high level of prolongation of the specific activity of the agent, reducing or eliminating negative side effects.

We give specific examples of the implementation of the invention.

Example 1. Purified water is loaded into the reactor, carbomer (Karbopol-934) is added while stirring and left for 10-12 hours, after which the resulting mixture is stirred again and 15-2595 ammonia solution is added to it while stirring to pH 5.0-7 ,0, obtaining a homogeneous transparent gel mass. Vaseline oil is loaded into the mixer, heated to a temperature of 55-65"C, crushed phoridone is added while stirring and it is dispersed in 2o, obtaining a suspension of phoridone in vaseline oil. Glycerin, propylene glycol, ethyl alcohol, twin- 80, a solution of formaldehyde and a suspension of phoridone, are mixed until homogeneous, obtaining the target product - phoridone gel, which is packaged in tubes.

The claimed agent has the following ratio of components, wt. 90: 25 phoridone 3.00 « carbomer (carbopol 934) 0.50 glycerin 5.00 propylene glycol 9.00 h- 30 2595 ammonia solution 0.20 ethyl alcohol 9695 6.50 o formaldehyde solution 0.05 «-- vaseline oil 8.00 twin-80 5.00 i) 35 purified water the rest I«o)

Example 2. The declared agent is obtained similarly to example 1 with this ratio of components, wt.

Fo: « foridon 3, BO0 - in carbomer (carbopol 974 RME) 0.70 s glycerin 5.40 ; - propylene glycol 4.00 2595 ammonia solution 0.30 45 ethyl alcohol 9695 9.50

Ge" formaldehyde solution 0.06, petroleum jelly 9.10 and twin-VO BBO, purified water, the rest (95) 50 Example 3. The declared agent is obtained similarly to example 1 with this ratio of components, wt. «m Fo: foridon 4.50 carbomer (carbopol 941) 2.50 glycerin 5.00 v. propylene glycol 4.00 1595 ammonia solution 2.00 ethyl alcohol 9695 10.50 formaldehyde solution 0.05 bo vaseline oil 8.00 tween-80 5.00 purified water the rest

Example 4. The declared agent is obtained similarly to example 1 with this ratio of components, wt. 65 or;

foridon 5.00 carbomer (carbopol 934). 1.00 glycerin 6.00 propylene glycol 7.50 1595 ammonia solution 0.60 ethyl alcohol 9695 8.00 formaldehyde solution oo petroleum jelly 10.00 tween-80 7.00 purified water the rest

Example 5. The declared agent is obtained similarly to example 1 with this ratio of components, wt. uv foridon 5.50 carbomer (carbopol 940) 0.50 glycerin 12.00 propylene glycol 9.00 720 1595 ammonia solution 0.20 ethyl alcohol 9695 6.50 formaldehyde solution 0.20 petroleum jelly 12.00 tween-80 10.00 the water is purified the rest "

Example 6. The declared agent is obtained similarly to example 1 with this ratio of components, wt. 0/. ate: im foridon 6.00 so carbomer (carbopol 974 RME) 2.50 glycerin 12.00 - propylene glycol 5.00 Geo) 1595 ammonia solution 2.00

Ethyl alcohol 9695 10.50% Formaldehyde solution 0.20% Vaseline oil 12.00 Twin-80 10.00% Purified water, the rest Example 7. Purified water is loaded into the reactor, carbomer is added while stirring and left on 10-12 hours, after which the resulting mixture is mixed again and triethanolamine is added to it with stirring to pH 5.0-7.0, obtaining a homogeneous transparent gel mass. Vaseline oil is loaded into the mixer, heated to a temperature of 55-65"C, crushed phoridone is added while stirring and dispersed, obtaining a 75% suspension of phoridone in vaseline oil. To the reactor with the gel mass while stirring successively

Glycerin, propylene glycol, ethyl alcohol, Tween-80, formaldehyde solution and phoridone suspension are loaded into Ф, (95) mixed until homogeneous, obtaining the target product - phoridone gel, which is packaged in tubes. -z The declared agent has the following ratio of components, wt. 90: oz 20 foridon 5.00 carbomer (carbopol 940). 1.00

What. glycerin 6.00 propylene glycol 7.50 1595 ammonia solution 1.00 29 ethyl alcohol 9695 8.00 v. formaldehyde solution oo petroleum jelly 10.00 twin-80 7.00 in purified water the rest

Example 8. Purified water is loaded into the reactor, carbomer is added while stirring and left for 10-12 hours, after which the resulting mixture is stirred again and sodium hydroxide is added to it while stirring to a pH of 5.0-7.0, obtaining a homogeneous transparent gel mass . Vaseline oil is loaded into the mixer, heated to a temperature of 55-65"C, crushed foridone is added while stirring and dispersed, obtaining a suspension of foridone in vaseline oil. Glycerin, propylene glycol, ethyl alcohol, twin- 80, a solution of formaldehyde and a suspension of phoridone, are mixed until homogeneous, obtaining the target product - phoridone gel, which is packaged in tubes.

The claimed agent has the following ratio of components, wt. 90: foridon 5.00 carbomer (carbopol 934). 1.00 glycerin 6.00 propylene glycol 7.50 70 1595 ammonia solution 0.32 ethyl alcohol 9695 8.00 formaldehyde solution oo vaseline oil 10.00 tween-80 7.00 purified water the rest

Example 9. Purified water is loaded into the reactor, added with stirring and left for 10-12 hours, after which the resulting mixture is stirred again and, with stirring, 15 95% ammonia solution is added to it to a pH of 5.0-7.0, obtaining a homogeneous transparent gel mass. Vaseline oil is loaded into the mixer, heated to a temperature of 55-65"C, crushed foridone is added while stirring and dispersed, obtaining a suspension of foridone in vaseline oil. Propylene glycol, ethyl alcohol, Tween-8O0, solution are sequentially loaded into the reactor with a gel mass while stirring. formaldehyde and phoridone suspension, mixed until homogeneous, obtaining the target product - phoridone gel, which is packaged in tubes.

The claimed agent has the following ratio of components, wt. 90: 29 phoridone 5.00 "sacap 1.60 propylene glycol 5.80 1595 ammonia solution 1.00 i.m. ethyl alcohol 710 formaldehyde solution 0.10 Ge) vaseline oil 10.50 "- tween - 80 7.70 purified water the rest so 35! ! not (se)

Example 10. Purified water is loaded into the reactor, akmid is added while stirring and left for 10-12 hours, after which the resulting mixture is mixed again and potassium hydroxide is added to it while stirring to pH 5.0-7.0, obtaining a homogeneous transparent gel mass . Vaseline oil is loaded into the mixer, heated to a temperature of 55-65"C, crushed phoridone is added while moving and dispersed, obtaining a suspension of phoridone in vaseline oil. Glycerin, ethyl alcohol, twin- 80, a solution of formaldehyde and a suspension of phoridone, are mixed until homogeneous, obtaining the target product - phoridone gel, which is packaged in tubes. :z" The declared agent has the following ratio of components, weight 90: phoridone 5.00 45 acmid 0.vo0 b glycerin 12.00

OO potassium hydroxide 0.30 - ethyl alcohol 710 formaldehyde solution 0.10 (95) 50 petroleum jelly 10.50 "M tween - 80 7.70 purified water the rest

Example 11. Purified water is loaded into the reactor, carbomer is added while stirring and left for 10-12 hours, after which the resulting mixture is mixed again and added to it while stirring. aminomethylpropanol to pH 5.0-7.0, obtaining a homogeneous transparent gel mass. Olive oil is loaded into the mixer, heated to a temperature of 55-65"C, crushed foridone is added while stirring and dispersed, obtaining a suspension of foridone in petroleum jelly. Polyethylene oxide-400, propylene glycol, ethyl alcohol, tween are sequentially loaded into the reactor with a gel mass while stirring. -80, nipagin 60 and the suspension of foridone, mixed until homogeneous, obtaining the target product - foridon gel, which is packaged in tubes. foridon 5.00 carbomer (carbopol 974 RME) 1.00 bo polyethylene oxide-400 6.90 propylene glycol 7.30 aminomethylpropanol 0.vo0 ethyl alcohol 8.00 nipagin 010 olive oil 8.50 twin-80 9.70 purified water the rest 70 Example 12. Purified water is loaded into the reactor, carbomer is added while stirring and left for 10-12 hours, after which the resulting mixture mix again and add to it while stirring potassium hydroxide to a pH of 5.0-7.0, obtaining a homogeneous transparent gel mass. Dimethicone is loaded into the mixer, heated to a temperature of 55-65"С, d add crushed foridone with stirring and disperse it, obtaining a suspension of foridone in dimethicone. 75 glycerol, propylene glycol, dimethylsulfoxide, pemulene, nipagin and foridone suspension are successively loaded into the reactor with the gel mass while stirring, mixed until homogenous, obtaining the target product - foridon gel, which is packaged in tubes.

The claimed agent has the following ratio of components, wt. 90: foridon 5.00 carbomer (carbopol 940). 1.00 720 glycerin 7.00 propylene glycol 7.30 potassium hydroxide 0.30 dimethyl sulfoxide 10.00 nipagin 010 dimethicone 10.00 " pemulene 5.00 purified water the rest

Example 13. Purified water is loaded into the reactor, carbomer is added while stirring and left for 10-12 hours, after which the resulting mixture is stirred again and ethanolamine is added to it while stirring to a pH of 5.0-7.0, obtaining a homogeneous transparent gel mass . Sunflower oil is loaded into the mixer, heated "- to a temperature of 55-65"C, crushed foridone is added while stirring and dispersed, obtaining a suspension of foridone in sunflower oil. Isopropyl alcohol, Tween-80, isopropyl alcohol, Tween-80, a mixture of nipagin and nipazol and a suspension of foridone, mixed until homogeneous, obtaining the target product - a gel of foridone, which is packaged in tubes.

The claimed agent has the following ratio of components, wt. 90: foridon 5.00 " carbomer (carbopol 940) 1.25 t0 ethanolamine 0.600 8 s isopropyl alcohol 30.00 ; - nipagin/nipazol 0.12mg/0.0Zmg sunflower oil 8.50 twina-80 9.70 b purified water the rest (95) Example 14. Purified water is loaded into the reactor, carbomer is added while stirring and left for 10-12 hours ., after which the resulting mixture is mixed again and potassium hydroxide is added to it with stirring to pH 5.0-7.0, obtaining a homogeneous transparent gel mass. Dimethicone is loaded into the mixer, heated to (95) 50 55-65"C, crushed phoridone is added while stirring and dispersed, obtaining a suspension of phoridone in dimethicone. Glycerin, propylene glycol, and ethyl alcohol are sequentially loaded into the reactor with a gel mass while stirring. , pemulen, triclosan and a suspension of foridone, mixed until homogeneity, obtaining the target product - gel of foridon, which is packaged in tubes. 10 potassium hydroxide 0.30 ethyl alcohol 0.00 60 triclosan 0.20 dimethicone 10.00 pemulene 5.00 purified water the rest bo yellowish shade of color, with a weak specific smell.

Cardiovascular diseases (ischemic heart disease, arterial hypertension and others) are one of the main causes of disability and mortality of the population. At the same time, there is not only an increase in the number of these diseases, but also the incidence of these types of pathology in increasingly younger groups of the population. The treatment of such patients should be complex and contain both the fight against the risk factors of coronary heart disease and those with clinical manifestations of angina pectoris. In the pathogenesis of coronary heart disease, along with atherosclerotic stenosis of coronary arteries, the role of dynamic coronary stenosis is recognized, the manifestations of which are reduced or eliminated by drugs based on calcium antagonists, one of whose representatives is foridone - the active substance of the claimed agent. It is necessary to take into account the high efficiency of calcium antagonists when using them as antihypertensive drugs.

Foridone /(2,6-dimethyl-3,5-dimethoxycarbonyl-4-(-2-difluoromethoxyphenyl)-1,4-dihydropyridine) is an antagonist of calcium ions, which exhibits hypotensive, antispasmodic and coronary dilating activity. Foridone is used for hypertension of the I-I degree, angina pectoris in a dose of 20 to 30 mg 3 times a day, daily dose - up to 1500 mg. The half-life of the drug from the body is 2-4 hours. A side effect of Foridone can be headache, dizziness, increased fatigue, facial redness, skin rash. In rare cases, nausea, vomiting, constipation, sleep disorder, nervousness, swelling of the lower extremities are noted. When using the main active substance - foridone in an amount less than the stated value, the necessary therapeutic effect is not achieved, and when using it in an amount greater than the stated values, there is no dose-dependent increase in the level of specific activity.

When conducting preclinical and clinical studies of the claimed agent, foridone in the form of tablets was used as the main drug of comparison. Among the various ways of introducing medicinal substances into the body, the use of a tablet form ensures relatively low bioavailability of active substances. Therefore, the way of introducing them through the skin is of great interest, in which a long and continuous supply of the active substance into the vascular bed is carried out, which contributes to the prolongation of the therapeutic effect.

The transdermal route of introduction of foridon into the body has many advantages compared to the oral method of use, namely: the possibility of reducing the dose of the drug; reduction or elimination of manifestations of toxicity of the drug or other side effects in the case of a need to increase the dose; elimination of the factor of biotransformation of foridone in the liver, as a result of which its bioavailability is М зо Total 20-50790; the possibility of a more accurate choice of the place of application. Until now, the use of foridone in the form of a gel was not known. at

The qualitative and quantitative composition of the proposed remedy for the treatment of cardiovascular diseases "is pharmacologically substantiated in experiments on animals by means of comparative studies of various gel samples in composition. The necessary and sufficient composition of the ingredients was determined and the conditions for carrying out i) of the technological process were selected, which in the complex ensures the multidirectional pharmacotherapeutic effect of the claimed agent, the necessary chemical-physical and mechanical-technological properties of its dosage form.

A preclinical study of the specific pharmacological activity of the claimed drug on animals (foridone tablets were used as a comparison drug) showed that the claimed drug exhibits antianginal, antiarrhythmic and hypotensive effects at the level of the comparison drug, but with a prolonged effect. The duration of the "antianginal effect" increases by approximately 2 times and its duration is 10-12 hours. (the duration of action of the drug from the comparison is 4-8 hours). The term of antiarrhythmic activity of the proposed agent increases to 8-10 hours.

With long-term use (within 3 months), the declared product did not reveal an allergenic effect, ;" local irritant effect and negative impact on vital organs of animals. The results of the study on animals of the acute toxicity of the drug indicate that the claimed agent belongs to practically non-toxic drugs. b The new pharmaceutical form of Foridon allows to reduce or eliminate the consequences of such negative manifestations, characteristic of drugs based on calcium antagonists, as a rapid rise and fall in the concentration of the active substance in the blood plasma and reflex reactions that accompany this phenomenon. - Thus, the claimed agent provides a slower achievement of the maximum concentration of foridon 5p in the blood plasma, a systemic effect of the drug, as well as a longer presence of the active substance in the body. o Clinical studies of the claimed agent were carried out on 45 patients with coronary heart disease with "M stable tension angina pectoris 1-P functional classes, as well as patients with hypertension of the I and I stages: 1 group (main - 3 patients), in complex therapy in which the claimed drug was used, group 2 (control - 15 patients), which received basic therapy with the exception of the claimed drug and other blockers in calcium channels. The average age of the patients was 52.2 years. Initially, 500 mg (25 mg of foridone) was prescribed daily 2 times a day ).Daily dose - 5Omg. The gel is applied and lightly rubbed either on the skin of the abdomen or on

P the upper part of the front surface of the chest, or on the skin of the forearm. When the initial therapeutic effect is achieved, the dose of the drug can be reduced to 25 mg (12.5 mg of foridone) within 2-3 weeks.

The daily dose is 25 mg of Foridone. It is used for the treatment of patients with ischemic heart disease, for patients with unstable angina, with hypertensive heart disease | and I stage, in the complex therapy of patients with acute myocardial infarction, with arterial hypertension, to increase tolerance to physical exertion.

Based on the data of the study of the dynamics of the indicators of clinical blood tests of patients of groups 1 and 2, it can be concluded that the claimed agent does not have any negative effect on these indicators. 65 The results of the study of the effect of the claimed agent and the comparison drug on the condition of patients with coronary heart disease (stable angina) are shown in Table 1.

1 and 2 groups re0.05 in comparison with the original data

Based on the analysis of the dynamics of the frequency of angina attacks in patients of groups 1 and 2, it can be concluded that in patients with coronary heart disease (stable angina), the claimed agent in combination with the means of basic therapy has a probable effect on the frequency of angina attacks, contributes to their reduction. 1 and 2 groups

Group of patients |The number of observations of the nyschistyna tire is 0.05 in comparison with the initial data и и и и

Studying the indicators of the dynamics of changes in the electrocardiograms of groups 1 and 2 of patients (table 2) made it possible to establish that in 86.9 95 cases in group 1 and in 81.8 95 cases in group 2, the indicators of the electrocardiogram improved. Dr

M o : i |se) re0.05 in comparison with the original data

The data in Table C show that patients with hypertension in both groups have a decrease in diastolic blood pressure (DBP), but this decrease is greater in group 1. At the same time, a decrease in systolic blood pressure (SBP) prevails in 1 group of patients. The obtained results are an indirect confirmation of the presence of the claimed drug with anti-ischemic, anti-anginal and hypotensive properties, because the claimed drug was used against the background of basic therapy, which includes drugs with the above-mentioned pharmacodynamic characteristics.

Table 4 shows the results of a clinical study of the antianginal effect of the claimed agent and the comparison drug. (22) m - Indicators of clinical examination su 20 t » The data of Table 4 show that the claimed agent exhibits a more significant antianginal effect than the comparison drug.

Table 5 shows the results of a clinical study of the dynamics of blood pressure indicators when using the claimed agent and the comparison drug. vv

Systolic BP 187.46.8 143.44.5" 189.559.6 1445556"

"- p»0.05 in the compared groups

The conducted studies show that the declared remedy corresponds to the optimal parameters of the drug's tolerability, does not cause pathological changes in laboratory parameters during clinical examinations of patients.

In order to determine the prolongation of the action of the suppository, studies of its clinical pharmacokinetics were conducted (on 6 patients with an average weight of 68.3 kg). The claimed agent was applied to the forearm in a dose of 1 g, which corresponds to bOmg of foridone. This dose was chosen based on the effectiveness of the doses and lies below the range of 70 toxic level of foridone. The obtained values of pharmacokinetic parameters testify to the gradual entry of foridone into the systemic bloodstream and confirm the optimality of the created dosage form, which allows to exclude the effect of a rapid increase in the concentration of the active substance in the blood, characteristic of calcium ion antagonists. The analysis of the study of the pharmacokinetic curve of the proposed agent showed that the period during which the concentration of foridone in the plasma is at the therapeutic level is 12 hours, which is significantly longer than when using tablets of foridone, the duration of which is 3-4 hours.

Thus, the claimed agent exhibits an antianginal and antihypertensive effect and clinical tolerability at the level of the comparison drug, does not cause pathological changes in laboratory indicators during clinical examination of patients; provides a long-term systemic effect, in which the therapeutic concentration of foridon in the plasma is maintained for 12 hours.

The claimed remedy allows for more effective protection of patients with angina pectoris, attacks of which are most often observed at night and before dawn, due to the constant maintenance of the required concentration of foridone in the blood, as a result of which the effect is prolonged, a longer hypotensive effect is provided compared to tablets, the frequency decreases intake and amount of the claimed agent per day (for example, for Foridon tablets - 3-4 times a day, and for "Foridon-gel" - 2 times a day).

In the process of conducting clinical studies, the possibility of intranasal use of the claimed agent was discovered, in which the therapeutic effect of foridone is manifested after 10 minutes and continues for 8-1 hours.

Thus, the rational choice of the new dosage form and the combination of its ingredients in the claimed tool fulfills the task set in the invention of prolonging the therapeutic effect, reducing the dose of the active substance and the number of doses per day, reducing or eliminating negative side effects. co

References 1. Mashkovsky M.D. Medicines. Kharkov: Torsing, 1997, Vol. 1, p. 389. - 2. Directory Delete. Medicinal preparations in Russia: Directory. M.: AstraPharmService, 2001, "U

B-245. 3o Z. Directory Deleted. Medicinal preparations in Russia: Directory. M.: AstraPharmService, 2001, ee,

B-245. 4. Mashkovsky M.D. Medicines. Kharkiv: Torsing, 1997, Vol. 1, p. 360. 5. Mashkovsky M.D. Medicines. Kharkov: Torsing, 1997, Vol. 1, p. 359. 6. Mashkovsky M.D. Medicines. Kharkiv: Torsing, 1997, T.1, p.411 (prototype). From the village of

Claims (9)

The formula of the invention 1. Means for the treatment of cardiovascular diseases, containing the active substance foridone and a pharmaceutically acceptable carrier, which is characterized by the fact that as a pharmaceutically acceptable carrier Me. use a gel base with this ratio of components, wt. 9o: (95) phoridon 3.00-6.00 - gel base the rest. at 50 2. Means according to claim 1, which is characterized by the fact that the gel base contains a thickener, non-aqueous hydrophilic and solvents, hydrophobic solvents, a preservative, a neutralizing agent, an emulsifier and purified water. 3. Means according to claim 2, which differs in that carbomer or sacap or acmid is used as a thickener. 4. The tool according to claim 2, which differs in that glycerin or polyethylene oxide-200, or polyethylene oxide-400, or polyethylene oxide-b6OO0, or propylene glycol, or dimethyl sulfoxide, or ethyl alcohol, or propyl alcohol, or their mixtures are used as non-aqueous hydrophilic solvents . P 5. Means according to claim 2, which differs in that petroleum jelly or sunflower oil, or peach oil, or sesame oil, or castor oil, or dimethicone are used as hydrophobic solvents. 6. Means according to claim 2, which differs in that a formaldehyde solution or nipagin, 60 or nipazol, or triclosan, or their mixtures are used as a preservative. 7. Means according to claim 2, which differs in that a 15-25 95 solution of ammonia or sodium hydroxide, or potassium hydroxide, or triethanolamine, or ethanolamine, or diisopropanolamine, aminomethylpropanol, or tris(hydroxypropylethylenediamine), or ethoxylated fatty aliphatics are used as a neutralizing agent amines, or sodium tetraborate, or trometamol. 65 8. Means according to claim 2, which differs in that twin-80 or twin-60O, or twin-40, or pemulene is used as an emulsifier. 9. Means according to claim 3, which differs in that the carbomer is polyacrylic acid or its resins. Official bulletin "Industrial Property". Book 1 "Inventions, useful models, topographies of integrated microcircuits", 2004, M 1, 15.01.2004. State Department of Intellectual Property of the Ministry of Education and Science of Ukraine. « cha so «- so (Se) - with . and? (22) (95) - about 50 that 60 b5