RU2442572C1 - The enteric cover and the composition for its preparation - Google Patents

Abstract

FIELD: pharmaceutical industry.

SUBSTANCE: invention refers namely to immunobiological drugs in the form of the capsules covered with the enteric cover. According to the declared invention the enteric cover on the basis of shellac for the firm demountable gelatinous capsule represents polymeric derivative in the form of a conglomerate of shellac and linen oil with participation of acetilsalicylic acid in the following ratio of the cover components, wgt. %: linen oil - 20,0-40,0; acetilsalicylic acid - 1,0-3,0; shellac - the rest, and the composition for the preparation of the enteric cover for the firm demountable gelatinous capsule contains shellac, linen oil, acetilsalicylic acid and spirit of ethyl 95 % in the following ratio of components, wgt. %: linen oil - 4,0-20,0; acetilsalicylic acid - 0,2-1,0; shellac - 8,0-40,0; spirit of ethyl 95 % - the rest.

EFFECT: technical result of the declared invention stipulates the preparation of the enteric cover for the firm demountable gelatinous capsules containing a porous filler with biological * active components of immunobiological drugs, providing effective separation of the case and a lid of a gelatinous capsule in the environment modeling the contents of small intestine, in case of simplification of the enteric cover preparation.

2 cl, 5 ex

Description

The invention relates to the pharmaceutical industry, namely to immunobiological preparations in the form of capsules coated with an enteric coating.

Immunobiological preparations (cytokines, immunoglobulins, probiotics, vaccines, bacteriophages) are increasingly used in the treatment of diseases of infectious and non-infectious origin. Comprehensive immunobiological preparations that accumulate the positive properties of single drugs in a specific finished dosage form are promising. In the vast majority of cases, the most physiological and therefore effective method of administering immunobiological mono- and complex preparations is their oral administration.

Of all the dosage forms of solid dosage forms, capsules are the optimal form that ensures the best preservation of the biological properties of the least stable active ingredients of the dosage immunobiological preparations intended for oral administration during manufacture and storage. An important task is to create conditions that protect the biologically active ingredients of the preparations from their inactivation during storage and after oral administration in the oral cavity, stomach and duodenum (RU patent No. 23232506, 04.20.2008).

The necessary tightness of a solid detachable capsule with respect to oxygen and atmospheric moist air, aggressive ingredients of the contents of the oral cavity, stomach and duodenum can only be achieved by applying an enteric coating after filling the capsule body and connecting it to the cap (US Patent No. 4816259, 03/28/1989).

Multilayer enteric coatings are known for capsules containing immunobiological preparations based on hydroxypropyl cellulose, cellulose acetate, beeswax and tween-20 or tween-80 wax (RU patent No. 2305541, September 10, 2007; RU patent No. 2308942, October 27, 2007).

One of the disadvantages of these analogues is the multilayer coating, which complicates the process of its application.

The disadvantage of these coatings is also that they are based on less physiological than natural chemically synthesized substances, in contrast to natural biologically active ingredients and targeted additives contained in capsules of immunobiological preparations.

In addition, the application of these enteric coatings used to prepare immunobiological preparations is associated with the use of toxic solvents, which, with initial capsule leakage and porosity of the filler (especially at optimal values of the equivalent pore diameter and particle size of the filler) and, accordingly, its permeability, can lead to partial loss biological properties of the active ingredients during coating, complicates the production process and increases the list controlled toxicants as part capsules.

An enteric coating based on shellac, a natural resin used in the pharmaceutical and food industries, is known for hard capsules containing 0.15% sulfur dioxide, which prevents their decay during production. In accordance with the known technical solution, before applying the enteric coating, a layer of the first coating is applied on the surface of the capsules, consisting of hydroxypropyl methylcellulose, 4 ÷ 9% polyethylene glycol and 0.5 ÷ 1% water. After that, at least one layer of enteric coating on the basis of confectionery glaze (food shellac) is applied to the purified capsules. When the capsules rotate above them, warm air with a temperature of about 75 ° C is passed. The capsules continue to rotate in warm air until all volatile solvents evaporate from their surface. After that, the capsules are unloaded from the machine and air dried on trays for 16-24 hours. The enteric coating contains a composition selected from the group consisting of fats, fatty acids, wax and mixtures thereof, shellac, ammonium shellac and cellulose acetate phthalate (US patent No. 4816259, 03/28/1989).

One of the disadvantages of this analogue is the multilayer coating, which especially with different composition of the layers complicates the process of its application.

A disadvantage of the analogue is that when applying the known coating, a high, inactivating immunobiological preparation air temperature is used, which can lead to the loss of biological properties of their active ingredients.

In addition, in the composition of the ingredients of the known enteric coating there are no substances that ensure effective separation of the body and lid of the gelatin capsule in a medium simulating the contents of the small intestine.

The closest analogue is known - the prototype is a gastro-resistant shellac coating used to obtain a drug in the form of capsules containing lyophilized biomass of bifidobacteria, a protective drying environment, a bifidogenic component and an immobilizer (RU patent No. 2164143, March 20, 2001).

The disadvantage of the prototype is the inability to effectively separate the housing and the lid of the gelatin capsule in a medium simulating the contents of the small intestine.

The basis of the claimed invention is the task of obtaining an enteric coating for hard detachable gelatin capsules containing a porous filler with biologically active ingredients of immunobiological preparations, which ensures effective separation of the shell and lid of the gelatin capsule in a medium simulating the contents of the small intestine, while simplifying the preparation of the enteric coating.

The task is achieved due to the fact that the enteric shellac based on shellac for a hard detachable gelatin capsule is a polymer derivative in the form of shellac conglomerate and linseed oil with the participation of acetylsalicylic acid in the following ratio of shell components, wt.%: Linseed oil - 20.0 ÷ 40.0; acetylsalicylic acid - 1.0 ÷ 3.0; shellac - the rest, and also due to the fact that the composition for obtaining the enteric coating of a hard detachable gelatin capsule contains shellac, linseed oil, acetylsalicylic acid and ethyl alcohol 95% in the following ratio of components in the composition, wt.%: linseed oil - 4.0 ÷ 20.0; acetylsalicylic acid - 0.2 ÷ 1.0; shellac - 8.0 ÷ 40.0; ethyl alcohol 95% - the rest.

The basis of the claimed invention is based on providing a solution to the problem a new set of original distinctive features: a new composition and selected ratio of the enteric coating, as well as the composition and ratio of ingredients of the corresponding claimed composition necessary for its preparation.

The selected ingredients of the inventive composition for the preparation of enteric coatings relate to food products and drugs. They are non-toxic in amounts significantly exceeding their content in the enteric coating and the composition for its preparation. The content of acetylsalicylic acid in the dosage form obtained in accordance with the claimed invention is significantly lower than the minimum single therapeutic dose of this substance.

Moreover, the composition and ratio of the ingredients of the claimed composition to obtain an enteric coating allows the use of temperature, time and dynamic parameters of spraying and drying, which, in combination with the neutrality of the ingredients of the composition with respect to the active ingredients of the capsule contents, effectively preserve the biological properties of the active ingredients of the capsule contents when applied enteric coating.

An original combination of the properties of the resulting shell is, on the one hand, the complete isolation of the contents of the capsule from the effects of the secretion of the oral cavity, the contents of the stomach and duodenum by sealing the capsule cavity of the inventive enteric coating, which, on the other hand, provides an effective separation of the body and lid of the gelatin capsule in medium simulating the contents of the small intestine, which, in turn, is promising for the selection of conditions for the exact release of the contents of the capsule in the ass This section of the intestine, capable of providing high efficiency of the active ingredients.

From the patent technical literature and the practice of pharmaceutical production, it is not known about the enteric coating and compositions for its preparation, which would be identical to the claimed ones. Hence, the conclusion about the conformity of the proposed solution to the criterion of "novelty" is legitimate.

The above set of essential features is necessary and sufficient to obtain a technical result - to obtain an enteric coating for hard detachable gelatin capsules containing a filler with biologically active ingredients of immunobiological preparations, which ensures effective separation of the body and lid of the gelatin capsule in a medium simulating the contents of the small intestine, while simplifying the preparation enteric coating. There is a causal relationship between the existing features and the problem to be solved, where each feature is necessary and affects the receipt of a technical result, and together the features taken are sufficient to obtain it. Therefore, the conclusion that the proposed solution meets the criterion of "inventive step" is legitimate.

The technical result of the claimed invention is to obtain an enteric coating for hard detachable gelatin capsules containing a porous filler with biologically active ingredients of immunobiological preparations, which ensures effective separation of the housing and lid of the gelatin capsule in a medium simulating the contents of the small intestine, while simplifying the preparation of an enteric coating.

The inventive enteric coating can be obtained repeatedly by using the composition to obtain it, and therefore, the claimed technical solution meets the criterion of "industrial applicability".

The invention is illustrated by the following examples, showing the preparation of an enteric coating for hard detachable gelatin capsules containing a filler with biologically active ingredients of immunobiological preparations, which ensures effective separation of the shell and lid of the gelatin capsule in a medium simulating the contents of the small intestine, while simplifying the preparation of an enteric coating. Moreover, the examples of enteric coating and compositions for its preparation show a specific implementation of the claimed invention, but do not limit the scope of claims of the claims of the claimed invention.

Example 1. A freshly prepared composition to obtain an enteric coating of a hard detachable gelatin capsule containing shellac, linseed oil, acetylsalicylic acid and ethyl alcohol 95% in the following ratio of components in the composition, wt.%: Linseed oil - 4.0; acetylsalicylic acid - 0.2; shellac - 8.0; ethyl alcohol 95% - the rest was applied by spraying in a fluidized bed at a composition temperature of 20 ÷ 35 ° C and air 18 ° C on the surface of solid detachable gelatin capsules containing a porous filler with an equivalent pore diameter of 10-110 μm with a particle size of not more than 100 μm comprising a biologically active ingredient - recombinant interferon-α ₂ . The obtained enteric coating was a polymer derivative in the form of a shellac conglomerate and linseed oil with the participation of acetylsalicylic acid in the following ratio of shell components, wt.%: Linseed oil - 32.8; acetylsalicylic acid - 1.6; shellac - the rest. Enteric coated capsules were stored for 1.5 months. Tests of the stability of the enteric coating in an acidic environment and disintegration in an alkaline environment were carried out in accordance with the requirements of the XIth edition of the State Pharmacopoeia - GF XI (State Pharmacopoeia of the USSR. XI edition (issue 2). - M .: Medicine, 1990. - T. 2. - S.158-160). The obtained enteric coating before and after storage of the capsules met the requirements of GF XI: the stability time of the obtained enteric coating in a solution of 0.1 mol / L hydrochloric acid was 60 minutes, the disintegration time of the resulting enteric coating in a medium simulating the contents of the small intestine was a solution of sodium bicarbonate with pH 7.5 - amounted to 40 minutes. In this case, the breakdown of hard split gelatin capsules with an enteric coating occurred in the form of separation of their bodies and caps over the past 5 minutes. In the process of obtaining an enteric coating and storage of capsules coated with an enteric coating, the biological properties (antiviral activity of recombinant interferon-α ₂ ) of the biologically active ingredient of the immunobiological preparation did not decrease.

Example 2. A freshly prepared composition to obtain an enteric coating of a hard detachable gelatin capsule containing shellac, linseed oil, acetylsalicylic acid and ethyl alcohol 95% in the following ratio of components in the composition, wt.%: Linseed oil - 16.0; acetylsalicylic acid - 1.0; shellac - 40.0; ethyl alcohol 95% - the rest was applied by spraying in a fluidized bed at a temperature of composition and air of 30 ÷ 40 ° C on the surface of solid detachable gelatin capsules containing a porous filler with an equivalent pore diameter of 10-110 microns with a particle size of not more than 100 microns, including biologically active ingredient is a complex immunoglobulin preparation for enteral use. The resulting enteric coating was a polymer derivative in the form of shellac conglomerate and linseed oil with the participation of acetylsalicylic acid in the following ratio of shell components, wt.%: Linseed oil - 28.0; acetylsalicylic acid - 1.8; shellac - the rest. Enteric coated capsules were stored for 1.5 months. Tests of the stability of the enteric coating in an acidic environment and disintegration in an alkaline environment were carried out in accordance with the requirements of the 11th edition of the State Pharmacopoeia - State Pharmacopoeia XI (State Pharmacopoeia of the USSR. XI edition (issue 2). - M .: Medicine, 1990. - T.2. - S.158-160). The obtained enteric coating before and after storage of the capsules met the requirements of Global Fund XI: the stability time of the obtained enteric coating in a solution of 0.1 mol / L hydrochloric acid was 60 minutes, the disintegration time of the obtained enteric coating in a medium simulating the contents of the small intestine was a solution of sodium bicarbonate with pH 7.5 - amounted to 40 minutes. At the same time, the breakdown of hard split gelatin capsules with an enteric coating occurred in the form of separation of their bodies and caps over the past 5 minutes. In the process of obtaining an enteric coating and storage of capsules coated with an enteric coating, the biological properties (antibody titers of the complex immunoglobulin preparation for enteral use) of the biologically active ingredient of the immunobiological preparation did not decrease.

Example 3. Freshly prepared composition to obtain an enteric coating of a hard detachable gelatin capsule containing shellac, linseed oil, acetylsalicylic acid and ethyl alcohol 95% in the following ratio of components in the composition, wt.%: Linseed oil - 20.0; acetylsalicylic acid - 0.8; shellac - 38.0; ethyl alcohol 95% - the rest was applied by spraying in a fluidized bed at a temperature of composition and air of 30 ÷ 40 ° C on the surface of solid detachable gelatin capsules containing a porous filler with an equivalent pore diameter of 10-110 microns with a particle size of not more than 100 microns, including biologically the active ingredient is recombinant interferon-α ₂ . The resulting enteric coating was a polymer derivative in the form of a shellac conglomerate and linseed oil with the participation of acetylsalicylic acid in the following ratio of shell components, wt.%: Linseed oil - 34.0; acetylsalicylic acid - 1.4; shellac - the rest. Enteric coated capsules were stored for 1.5 months. Tests of the stability of the enteric coating in an acidic environment and disintegration in an alkaline medium were carried out in accordance with the requirements of the 11th edition of the State Pharmacopoeia - State Pharmacopoeia XI (State Pharmacopoeia of the USSR. XI edition (issue 2). - M .: Medicine, 1990. - T. 2. - S.158-160). The obtained enteric coating before and after storage of the capsules met the requirements of Global Fund XI: the stability time of the obtained enteric coating in a solution of 0.1 mol / L hydrochloric acid was 60 minutes, the disintegration time of the obtained enteric coating in a medium simulating the contents of the small intestine was a solution of sodium bicarbonate with pH 7.5 - amounted to 40 minutes. In this case, the breakdown of hard split gelatin capsules with an enteric coating occurred in the form of separation of their bodies and caps over the past 5 minutes. In the process of obtaining an enteric coating and storage of capsules coated with an enteric coating, the biological properties (antiviral activity of recombinant interferon-α ₂ ) of the biologically active ingredient of the immunobiological preparation did not decrease.

Example 4. Freshly prepared composition for obtaining an enteric coating of a hard detachable gelatin capsule containing shellac, linseed oil, acetylsalicylic acid and ethyl alcohol 95% in the following ratio of components in the composition, wt.%: Linseed oil - 10.0; acetylsalicylic acid - 0.25; shellac - 14.75; ethyl alcohol 95% - the rest was applied by spraying in a fluidized bed at a composition temperature of 30 ÷ 38 ° C and air 25 ÷ 30 ° C on the surface of solid detachable gelatin capsules containing a porous filler with an equivalent pore diameter of 10-110 μm with a particle size of not more than 100 μm, including dry biomass of the strain Lactobacillus acidophilus K3Sh24. The resulting enteric coating was a polymer derivative in the form of a shellac conglomerate and linseed oil with the participation of acetylsalicylic acid in the following ratio of shell components, wt.%: Linseed oil - 40.0; acetylsalicylic acid - 1.0; shellac - the rest. Enteric coated capsules were stored for 1.5 months. Tests of the stability of the enteric coating in an acidic environment and disintegration in an alkaline environment were carried out in accordance with the requirements of the 11th edition of the State Pharmacopoeia - State Pharmacopoeia XI (State Pharmacopoeia of the USSR. XI edition (issue 2). - M .: Medicine, 1990. - T.2. - S.158-160). The obtained enteric coating before and after storage of the capsules met the requirements of Global Fund XI: the stability time of the obtained enteric coating in a solution of 0.1 mol / L hydrochloric acid was 60 minutes, the disintegration time of the obtained enteric coating in a medium simulating the contents of the small intestine was a solution of sodium bicarbonate with pH 7.5 - amounted to 40 minutes. At the same time, the breakdown of hard split gelatin capsules with an enteric coating occurred in the form of separation of their bodies and caps over the past 5 minutes. In the process of obtaining an enteric coating and storage of capsules coated with an enteric coating, the biological properties (lactobacilli content in CFU) of the biologically active ingredient of the immunobiological preparation did not decrease.

Example 5. A freshly prepared composition for obtaining the enteric coating of a hard detachable gelatin capsule containing shellac, linseed oil, acetylsalicylic acid and ethyl alcohol 95% in the following ratio of components in the composition, wt.%: Linseed oil - 5.0; acetylsalicylic acid - 0.75; shellac - 19.25; ethyl alcohol 95% - the rest was applied by spraying in a fluidized bed at a composition temperature of 25 ÷ 30 ° C and air 25 ÷ 30 ° C on the surface of solid detachable gelatin capsules containing a porous filler with an equivalent pore diameter of 10-110 μm with a particle size of not more than 100 microns, including a biologically active ingredient - a complex immunoglobulin preparation for enteral use. The obtained enteric coating was a polymer derivative in the form of shellac conglomerate and linseed oil with the participation of acetylsalicylic acid in the following ratio of shell components, wt.%: Linseed oil - 20.0; acetylsalicylic acid - 3.0; shellac - the rest. Enteric coated capsules were stored for 1.5 months. Tests of the stability of the enteric coating in an acidic environment and disintegration in an alkaline environment were carried out in accordance with the requirements of the 11th edition of the State Pharmacopoeia - State Pharmacopoeia XI (State Pharmacopoeia of the USSR. XI edition (issue 2). - M .: Medicine, 1990. - T.2. - S.158-160). The obtained enteric coating before and after storage of the capsules met the requirements of Global Fund XI: the stability time of the obtained enteric coating in a solution of 0.1 mol / L hydrochloric acid was 60 minutes, the disintegration time of the obtained enteric coating in a medium simulating the contents of the small intestine was a solution of sodium bicarbonate with pH 7.5 - amounted to 40 minutes. At the same time, the breakdown of hard split gelatin capsules with an enteric coating occurred in the form of separation of their bodies and caps over the past 5 minutes. In the process of obtaining an enteric coating and storage of capsules coated with an enteric coating, the biological properties (antibody titers of the complex immunoglobulin preparation for enteral use) of the biologically active ingredient of the immunobiological preparation did not decrease.

Claims (2)

1. An enteric shellac-based shell for a hard detachable gelatin capsule containing a film-forming component and a plasticizer, characterized in that it is a polymer derivative in the form of shellac conglomerate and linseed oil with the participation of acetylsalicylic acid in the following ratio of shell components, wt.%:
linseed oil 20,0-40,0 acetylsalicylic acid 1.0-3.0 shellac rest 2. The composition for obtaining the enteric coating of a hard detachable gelatin capsule according to claim 1, characterized in that it contains shellac, linseed oil, acetylsalicylic acid and ethyl alcohol 95% in the following ratio of components in the composition, wt.%:
linseed oil 4.0-20.0 acetylsalicylic acid 0.2-1.0 shellac 8.0-40.0 ethyl alcohol 95% rest