RU2129430C1 - Preparation "santomectin" for ecto- and endoparasites control in animals - Google Patents

Abstract

FIELD: veterinary science. SUBSTANCE: invention proposes the preparation "Sandomectin" that can be recommended for prophylaxis and treatment of animals with sicknesses caused by endo- and ectoparasites. Preparation has an avermectin complex and clozantel as active components. Combination of components taken at the definite ratio provides high therapeutic effect at decreased dose of avermectin. EFFECT: enhanced effectiveness. 10 ex

Description

 The invention relates to the field of veterinary medicine and can be used for the prevention and treatment of diseases caused by endo- and ectoparasites of animals.

 Known antiparasitic drug CIDEKTIN, manufactured by the company "Cyanamide" (USA), which contains moxidectin as an active substance.

 The drug is widely used to combat intestinal ticks, lice, scabies mites, lice and other animal parasites (Chirkh G., Veterinary preparations of the company "Cyanamide", Vetinform, N 1, 1992, S. 13-14).

 The disadvantage of the drug is the high content of active substance in the therapeutic dose (20 mg / 100 kg of animal weight).

 A family of compounds - Avermectins - is known, which is a complex of eight chemically similar substances, which, in turn, are a 16-membered macrolide lactone, combined with two residues of omandrose sugar.

Avermectin components are designated: A _1a , A _1b , A _2a , A _2b , B _1a , B _1b , B _2a , B _2b .

 Avermectins are a vital product of the Srt culture. avermitilis.

Avermectins are represented by three drugs:
Abamectin is an avermectin complex containing not less than 80% avermectin B _1a and not more than 20% avermectin B _1b .

Ivermectin is a semisynthetic dihydrogenated derivative of avermectin containing not less than 80% dihydroavermectin B _1a and not more than 20% dihydroavermectin B _1b (Campbell WC, Ivermectyn and Abamectyn. - Springer-Verlag. - New York-Berlin-London-Paris-Tokyo. - 1989 , - 363 p.).

Doramectin - avermetkin B ₁ containing at position C ₂₅ -cyclohexyl (Arkhipov I.A. et al., Veterinary Medicine, 1997. - N 2. p. 34-38).

 These drugs are broad-spectrum antiparasitic drugs, they are used separately, mainly parenterally, less often - orally.

 However, avermectins are not effective against animal cestodoses and trematodoses.

The most deeply and comprehensively studied Ivermectin in various dosage forms (Volkov F.A., Apalkin V.A., Ivermectin in veterinary medicine, Novosibirsk, MSDAGVET, - 33 pp.)
Ivermectin causes the death of arthropod nematodes. The mechanism of action of this substance on various parasites is not the same, but its influence on the transmission of nerve impulses between nerve cells or from a nerve cell to a muscle tissue cell through the neurotransmitter gamma-aminobutyric acid is common.

 This drug is taken as a prototype.

 The aim of the invention is to reduce the content of antiparasitic substances in the therapeutic dose of the drug and the expansion of its spectrum of action.

 This goal is achieved by the fact that closantel is additionally introduced into the composition of the drug.

 Closantel is the active ingredient in antiparasitic drugs such as faskoverm, ronelon and santel.

Closantel - C ₂₂ H ₁₄ Cl ₂ I ₂ N ₂ O ₂ - N- [5-chloro-4 - [- (4 chloro-phenyl) cyanomethy1-2-methylphehy1] -2- hydroxy-3.5 diiodobenzamide - has a wide spectrum of action , active against ecto- and endoparasites, including Fasciola hepatica, Fasciola gigantica, Bunomostum sp., Haemonchus contortus, Haemonchus placei, Oesophagostomum radiatum, etc.

 The mechanism of action of the drug is to change the processes of phosphorylation and electron transfer in the body of the parasite, which leads to disruption of energy metabolism and death of the parasite (Closantel, a new antiparasitic hydrogen ionophore. Van den Bossche, H .; Verhoeven, H .; Vanparus, O. et all; Archives International's de Physiologie et de Biochemie, 1979 Vol. 87 (4) 851-3).

Our proposed preparation contains, wt.%:
Avermectin complex (abamectin or ivermectin or doramectin) - 0.025 - 20.0
Closantel - 0.5 - 25.0
Solvents or fillers, stabilizers, preservatives - Up to 100
The drug is given the name "Santomectin."

 An analysis of the prior art showed the absence of any information on technical solutions that completely coincide in the aggregate of essential features with the claimed means, which allows us to conclude that the proposed technical solution meets the patentability condition of "novelty."

 Only a combination of the claimed components in the claimed ratio allows to achieve the effect indicated in the purpose of the invention, which allows us to conclude that the claimed drug meets the patentability condition "inventive step".

 The drug also meets the condition of patentability "industrial applicability", because can be widely used in veterinary practice.

 Get the drug by mixing and dissolving the components, and then, if necessary, it is filtered, sterilized, packaged in bottles or ampoules.

 As solvents, dimethylacetamide, dimethyl sulfoxide, dimethylformamide, N-methylpyrrolidone, alcohols, polyethylene glycols, propylene glycols, triglycerides, benzoic acid benzyl ester, glycerol formal, oils (sesame, olive, peach, apricot, etc.) are used. As stabilizers, citric acid, ascorbic acid, EDTA, sodium or potassium hydroxide, and as preservatives, benzyl alcohol, methyl paraben, propyl paraben and others.

 The drug can be used in the form of solutions: injectable, oral, skin (in the form of pur on and spot on), suspensions, as well as in the form of powders, boluses, tablets and pastes.

 Fillers for powders can be sugars (lactose, glucose, fructose), zeolites, chalk, flour, aerosil and more.

 The examples below characterize the biological activity of the proposed drug.

Example 1
On 38 heads of gobies aged 2 - 2.5 years spontaneously invaded by gastrointestinal nematodes and fascioli, the dosage form of ivermectin with closantel was tested in doses of 0.1 and 2.5 ml of DV / kg, respectively, in the form of an injection, subcutaneously. Before treatment with coproovoscopic studies, it was found that the bulls are intensively infested with gastrointestinal strongilates and fascioli. On the 32nd day after treatment, post-mortem autopsy showed that against fasciol extensivity (EE) was 91.5%, and intensity efficacy (IE) was 99.4%, against nematodes, respectively, 90.8 and 99.6%.

Example 2
On 215 heads of sheep aged 2 years, affected by psoroptosis and sarcoptosis, as well as gastrointestinal strongilates, a similar injection of closantel and doramectin was tested in doses of DV of 2 and 0.15 mg / kg body weight, respectively, intramuscularly. On day 15 after treatment, live ticks were not found on the body of animals. Efficiency against helminths (EE) was 100%.

Example 3
On 30 heads of cattle spontaneously invaded by gastrointestinal strongilates and fasciols, a powder form of a mixture of closantel with ivermectin was tested. The dose of DV, respectively, 10 and 0.1 mg / kg. EE against nematodes was 99.7% and against fasciol - 98.5%.

Example 4
For cattle hypodermatosis, a solution of closantelum with abamectin was administered subcutaneously in doses of 1.5 and 0.1 mg / kg to 65 cows, respectively. The processing was carried out in October 1996, the effectiveness was taken into account in April 1997. Studies of the skin of cows in the back, croup, and sides showed the absence of hypoderm nodules.

Example 5
In another group of cows (20 animals), puron was tested, containing closantel and ivermectin as a DV. Puron was applied to the skin of the back at the rate of DV of 5 and 0.15 mg / kg, respectively. In this experiment and the next, the animals were affected by dictiocauliasis. By co-prooscopic studies, it was found that EE was 99.8%.

Example 6
A similar group of cows was injected with an oral solution of closantel in combination with ivermectin calculated on the basis of DV, respectively 7 and 0.1 mg / kg in the form of an oral solution. A cooproscopic examination 2 weeks after treatment showed an EE of 98.4%.

Example 7
Production tests of the effectiveness of the control of fasciols and gastrointestinal strongilates were carried out on 70 cows, which were injected intramuscularly with closantelum mixed with abamectin in doses of DV of 2.5 and 0.1 mg / kg, respectively. Post-mortem autopsy showed that against immature fasciol EE = 98.6 and IE = 91.2%, and against mature forms - EE = 98.8 and IE = 99.7%.

Example 8
In the experiment on 45 cows and heifers, the cessation of discharge of dictiocaul larvae and fasciol eggs with feces was noted 3 weeks after treatment. Oral boluses were administered with closantel and ivermectin at doses of DV of 3 and 0.1 mg / kg, respectively.

Example 9
On 3 heads of horses with clinically pronounced signs of onchocerciasis, the dosage form of closantel with ivermectin was tested, respectively, at 2.5 and 0.1 mg of AI / kg in the form of an oral paste. After slaughter of animals, no live onchocercal ligaments were found in the studied samples.

Example 10
Production tests of the effectiveness of the fight against nematodoses, as well as with sarcoptosis and sifunculosis of pigs were carried out on 47 gilts, which were injected intramuscularly with closantelum mixed with abamectin in doses of DV of 2.5 and 0.1 mg / kg, respectively. Post mortem autopsy showed that against nematodes EE = 93.1 and IE = 97.4%. Efficacy against ectoparasites was 100%.

 Thus, the highly effective drug "Santomectin" was obtained, which can be used in animal diseases such as psoroptosis, sarcoptosis, sifunculosis and nematodoses, as well as fascioliasis, dictiocauliasis, hypodermatosis and bovine teliasis; fascioliasis, dictyocaulosis, and small cattle estrosis.

 The high therapeutic effect of the proposed dosage form, in which the avermectin content is halved, is due to the presence of closantel in the preparation and its synergistic interaction with avermectin.

 This is noted for gastrointestinal nematodes, dictiocaul, fasciol, hypodermis, scabies mites and for estrosis.

 The dosage form of the drug in the form of a powder with zeolite or chalk is well eaten by animals, has a high therapeutic effect and is convenient in practical use.

 It is also convenient to treat animals with Santomectin in the form of pur on, as only one veterinarian can carry out such treatment and no additional labor is required to fix the animals.

 The injection form of Santomectin does not have a local irritant effect and does not cause animal anxiety.

Claims (1)

Avermectin-based animal ecto- and endoparasite preparation, characterized in that it additionally contains closantelum, as well as solvents or fillers, stabilizers and preservatives, and avermectin complex as avermectins: abamectin, or ivermectin, or doramectin in the following ratio of components , wt.%:
Avermectin complex (abamectin, or ivermectin, or doramectin) - 0.025 - 20.0
Closantel - 0.5 - 25.0
Solvents or fillers, stabilizers, preservatives - Up to 100