RU2412698C1 - Method of treating helminthiases in ruminants and medicinal agent for implementation thereof - Google Patents

Abstract

FIELD: medicine, veterinary science. ^ SUBSTANCE: group of inventions concerns veterinary science and can be used for treating helminthiases in ruminants. The method of treating involves oral introduction to small cattle and bovine animals of a medicinal agent containing praziquantel, ivermectin and a target additive. Also, the medicinal agent additionally contains sodium selenite in the following ratio of components (g in 1 tablet): praziquantel - 0.25, ivermectin - 0.01, sodium selenite - 0.0036, target additive - 0.9364. It is followed by preparing a tabletted dosage form of the medicinal agent which is introduced to animals in a single dose at 1 tablet per 50 kg of body weight. ^ EFFECT: group of inventions allows reducing toxic action of the used medicinal agent with maintaining its high therapeutic anthelmintic effect. ^ 6 cl, 2 tbl, 5 ex

Description

The group of inventions relates to the field of veterinary medicine, in particular to the treatment of helminthiases of cattle and small cattle.

A known method of treating animal helminthiasis by using a medicament containing a compound from the group of avermectins, praziquantel and target additives (patent RU 2279874 C9, 07.20.2006).

The disadvantage of this invention is that it is a comprehensive drug for horses. This drug is made in the form of a paste and cannot be used for deworming of small and cattle.

A known method of treating animal helminthiasis by using a medicinal product containing a compound from the group of avermectins, pyrantel or its salt, praziquantel and target additives (patent RU 2287332 C2, 20.11.2006).

Also known is a method of treating animal helminthiasis by using a medicament containing a compound from the group of avermectins, praziquantel, levamisole and targeted additives (patent RU 2367435 C1, 09/20/2009).

However, the known methods and means are not only highly effective in the treatment of helminthiasis, but also have toxicity and immunosuppressive activity.

The objective of the present group of inventions is to increase the effectiveness of the treatment of cestodose-nematode dose mixtinvasions in ruminants by reducing the toxic effect of the drug used.

The problem in the method for the treatment of helminthiases of ruminants, including the oral administration to small and cattle of a drug containing praziquantel, ivermectin and the target additive, is solved by the fact that according to the invention, sodium selenite is additionally introduced into the composition of the drug in the following ratio of ingredients (in g per 1 tablet): praziquantel - 0.25, ivermectin - 0.01, sodium selenite - 0.0036, target additive - 0.9364, then a tablet form of the drug is prepared, which is administered here once at the rate of 1 tablet per 50 kg of body weight.

The problem is also solved by the fact that, as a target additive, potato starch, lactose, polyvinylpyrrolidone and calcium stearate are introduced into the drug in the following ratio of ingredients (in g per 1 tablet): potato starch - 0.308, lactose - 0.5405, polyvinylpyrrolidone - 0, 07, calcium stearate - 0.0179.

In addition, the problem is also solved by the fact that the drug in the form of tablets is administered to animals individually forcibly to the root of the tongue.

The problem is also solved by the fact that before use, the tablets are ground in a mill and introduced to the animals in a mixture with food in a group method.

The problem in terms of the drug for the treatment of helminthiases of ruminants containing praziquantel, ivermectin and the target additive is solved by the fact that according to the invention, the drug additionally contains sodium selenite in the following ratio of ingredients (in g per 1 tablet): praziquantel - 0.25, ivermectin - 0.01, sodium selenite - 0.0036, target additive - 0.9364.

The problem is also solved by the fact that the target additive contains (in g per 1 tab.): Potato starch - 0.308, lactose - 0.5405, polyvinylpyrrolidone - 0.007, calcium stearate - 0.0179.

The claimed method and drug are intended for the treatment of cestodoses, nematodoses and mixtinvasions of ruminants.

The technical result of the claimed group of inventions is to reduce the toxic effects of the drug used while maintaining a high anthelmintic activity.

The invention is illustrated by the following examples, which, however, do not limit the scope of the claims of the applicant.

Example 1. Preparation of a medicinal product

The preparation of the drug takes place in a granulator dryer. Raw materials are prepared for the preparation of the granulate; before mixing, the raw materials are weighed and sieved through a metal sieve. Weighed and sifted raw materials are loaded into a granulator dryer, mixed until a homogeneous moistened mass is obtained. The resulting mass is dried and removed from the installation. Add starch and reload into the installation.

Set the necessary parameters of the tablet press and produce tableting. Get tablets weighing 1.2 g. During tabletting periodically check the average weight of the tablets and disintegration.

The obtained drug in the form of tablets contains in its composition per 1 tablet, g: praziquantel - 0.25, ivermectin - 0.01, sodium selenite - 0.0036, target additive - 0.9364. The target supplement contains 1 tablet, g: potato starch - 0.308, lactose - 0.5405, polyvinylpyrrolidone - 0.07, calcium stearate - 0.0179.

Example 2. Evaluation of the therapeutic efficacy of a drug in the form of a tablet in case of moenisia of calves and sheep.

In the experiment, 20 heads of sheep and 16 heads of calves invaded by Moniezia expansa, M. benedeni were taken. The drug in the form of tablets was given to animals of the first and second experimental groups once individually in the morning at the rate of 1 tablet per 50 kg of body weight. At the same time, the drug in the form of tablets was administered to animals by force on the root of the tongue. A special diet and the use of laxatives to animals before deworming is not required. 18 animals of the control groups did not receive the drug.

The effectiveness of the proposed anthelmintic agent was determined according to the results of helminthoscopy studies conducted 7 days after the drug was given.

The results of the example are presented in table 1.

Table 1 No. Group of animals Number of goals Dosage form Efficiency% Side effects one. Experienced - cattle 8 pills one hundred are absent 2. Experienced - Sheep 10 pills one hundred are absent 3. Control - cattle 8 - - - four. Control - Sheep 10 - - -

Animals of the control group were invaded throughout the entire period of the experiment.

Example 3. Evaluation of the therapeutic efficacy of tablets with mixtinvasions.

22 cattle spontaneously invaded by Hypoderma bovis and gastrointestinal strongilates were taken into the experiment. The drug in the form of tablets was given to the animals of the experimental group once individually in the morning at the rate of 1 tablet per 50 kg of body weight, animals of the control group (n = 10) did not receive the drug.

After 40-50 days, the experimental and control animals were slaughtered, hides, carcasses were examined for the presence of gadfly larvae, the gastrointestinal tract was subjected to complete helminthological dissection. The results of the example are presented in table 2.

table 2 No. Group of animals Dose Skins and carcasses examined Detected Intensity Efficiency (IE),% Nematode Hypoderm Larvae Nematodoses Hypodermatosis one. Experienced pills 1 tablet per 50 kg 22 Ostertagia 8 99.6 98.4 2. Control - 10 285 - -

Example 4

The experiment was carried out on June 24, 2009 on 250 lambs of the current year of birth, naturally invaded by moniesiosis, strictilatoses of the gastrointestinal tract, dictiocauliasis, and estrosis. The drug was asked at the rate of 1 tablet per 50 kg of animal weight. Before use, the tablets were ground in a mill and given to the animals in a mixture with feed as a group method.

The efficacy of the drug against moniesiosis, strong gastrointestinal tract and lungs was determined by ovoscopy of feces samples before and 10 days after deworming. The efficacy of the drug against estrosis was determined by clinical signs and opening of the nasal passages of 9 lambs.

In all fecal samples, before giving the drug, eggs of strongilate were found in an amount of 57 to 135 ind. in three drops, in 120 samples, single nematodir eggs, 108 samples of dictiocaulus larva from 23 to 75 specimens, 90 samples — moniesia eggs.

During larvoscopic examinations 10 days after the drug was given, in all samples, Strongilata, nematodir, moniesia, and dictyocaulus larvae were not found. When opening the nasal passages and frontal sinuses of 9 lambs, no estrosis larvae were found.

In the control group, the invasion of animals remained unchanged.

Thus, the drug in a dose of 1 tablet per 50 kg of live weight of sheep has shown 100% effectiveness in helminthiases such as moniesiosis, strictilatosis of the gastrointestinal tract, dictiocaulosis and estrosis.

Example 5. Assessment of toxicity of the claimed drug

2 preparations were prepared. The composition of the first drug is similar to the declared one, i.e. the preparation contains 1 tablet, g: praziquantel - 0.25, ivermectin - 0.01, sodium selenite - 0.0036, potato starch - 0.308, lactose - 0.5405, polyvinylpyrrolidone - 0.07, calcium stearate - 0.0179 .

The composition of the second drug was obtained by excluding sodium selenite from the composition of the first drug, i.e. The 2nd preparation contains 1 tablet, g: praziquantel 0.25, ivermectin 0.01, potato starch 0.308, lactose 0.5405, polyvinylpyrrolidone 0.07, calcium stearate 0.0179.

The study of the toxicity parameters of the two drugs was carried out on the basis of the “Methodological Recommendations for the Study of the General Toxic Effect of Pharmacological Substances” approved by the Russian Ministry of Health on December 29, 1997. The parameters of acute toxicity were determined on white mice by the probit analysis proposed by Litchfield and Wilcoxon in modification 3. Rota.

The study of the parameters of acute toxicity of the drug was carried out on 78 white mice of the BALB line weighing 18-20 g. The animals were kept on a starvation diet for 18-20 hours before the experiment. The drug was administered to two groups (n = 36, n = 42) using a club-shaped needle with a club-shaped thickening in the stomach of mice in various doses. The claimed drug was administered to the first group, and the second drug (i.e., the drug from which sodium selenite was excluded) was administered to the animals of the second group. At the same time, together with the 2nd preparation, the animals were injected with sodium selenite at a dose of 71 μg / kg.

After administration of the drug, observations were carried out for 14 days, taking into account the general condition of the animals, the condition of the coat, mobility and sensitivity to external stimuli.

As a result, lethal doses (LD ₁₆ , LD ₅₀ , LD ₈₄ , LD ₁₀₀ ) of the drug were determined in both groups of animals, which were in animals of the first experimental group receiving the drug - LD ₅₀ - 12500 mg / kg, in animals of the second experimental group receiving 2nd preparation and additional sodium selenite - LD ₅₀ - 10,000 mg / kg.

The clinical picture of intoxication of animals exposed to the drug in a dose range of LD ₅₀ -LD ₁₀₀ was expressed as inhibition, the coat was moist, no blood flow was observed. Death occurred in 5-12 hours.

During postmortem examination of these animals, no signs of pathology of the internal organs were noted. The stomach and intestines were weakly filled, hyperemic with a mushy consistency of contents.

Thus, the claimed method allows to reduce the toxic effect of the drug used while maintaining its high therapeutic anthelmintic effectiveness.

Claims (6)

1. A method for the treatment of helminthiases of ruminants, including the oral administration to small and cattle of a drug containing praziquantel, ivermectin and the target additive, characterized in that the composition of the drug is additionally administered sodium selenite in the following ratio of ingredients (in g per 1 tablet) : praziquantel - 0.25, ivermectin - 0.01, sodium selenite - 0.0036, target additive - 0.9364, then prepare a tablet form of the drug, which is administered to animals once at a rate of 1 tablet per 50 kg of body weight. 2. A method of treating ruminant helminthiases according to claim 1, characterized in that potato starch, lactose, polyvinylpyrrolidone and calcium stearate are introduced into the drug as a target additive in the following ratio of ingredients (in g per 1 tablet): potato starch - 0.308, lactose - 0.5405, polyvinylpyrrolidone - 0.07, calcium stearate - 0.0179. 3. A method for the treatment of helminthiases of ruminants according to claim 1, characterized in that the drug in the form of tablets is administered to animals individually forcibly to the root of the tongue. 4. A method for the treatment of helminthiases of ruminants according to claim 1, characterized in that before use, the tablets are ground and given to the animals in a mixture with food in a group method. 5. A medicine for the treatment of helminthiases of ruminants according to the method according to any one of claims 1 to 4, containing praziquantel, ivermectin and a target additive, characterized in that it additionally contains sodium selenite in the following ratio of ingredients (in g per 1 tablet):
praziquantel 0.25 ivermectin 0.01 sodium selenite 0.0036 target additive 0.9364 6. The drug for the treatment of helminthiases of ruminants according to claim 5, characterized in that the target additive contains (in g per 1 table.):
potato starch 0,308 lactose 0.5405 polyvinylpyrrolidone 0,07 calcium stearate 0.0179