GR1010072B - Edible veterinary intramammary teat sealant formulations and method for their preparation - Google Patents

Abstract

The present invention refers to novel template intramammary formulations namely Mastin, as well as to a process for their preparation, wherein said formulations comprise oleogels composed of at least 75% vegetable oils and at least 5% of a food grade gelator, oleogels composed of w/o emulsions of vegetable oils, oleogels composed of suspensions of hydrophilic compounds in vegetable oils, oleogels composed of enriched vegetable oils with plant extracts, oleogels composed of vegetable oils with honey and/or its derivatives and biphasic gels composed of mixtures of vegetable oil oleogel mixed with hydrogels.

Description

EDIBLE VETERINARY COMPOSITIONS FOR MAMMAL INTOMAMARY PROTECTION AND METHOD FOR THEIR PREPARATION

Technical field of the invention

The present invention relates to standard intramammary protection formulations, as well as processes for their preparation, wherein said standard intramammary protection formulations include oleogels consisting of vegetable oils and edible food-grade coagulants, oleogels consisting of w/o emulsions of vegetable oils, oleogels consisting of suspensions of hydrophilic compounds in vegetable oils, oleogels consisting of enriched vegetable oils with vegetable extracts, oleogels consisting of vegetable oils with honey and/or its derivatives and biphasic gels consisting of mixtures of oleogels of vegetable oils mixed with hydrogels.

Background of the invention

The application of intramammary preparations is mainly focused on the treatment and treatment of various diseases or disorders related to the mammary gland, such as for example infections. The majority of these formulations focus on the treatment of lactating animals. The standard method of their application is injection, where the preparation is introduced into the mammary gland through the nipple duct. The latter are also characterized as injectable preparations. However, other formulations such as creams, emulsions and ointments are applied topically to the skin of the nipples or breast.

The most serious, common and potentially fatal disease of the mammary gland in dairy animals is mastitis. Mastitis is a major health problem in dairy animals worldwide. The majority of available information on mastitis concerns dairy cattle.

Some types of pathogens are listed here. The inflammation of the mammary gland, regardless of its origin, severity and progression is described as mastitis. Clinically, it can be classified as clinical or subclinical mastitis, depending on the extent of infection in the mammary gland. The main pathogens that cause mastitis are Escherichiacoll (E. Coli), Streptococcusuberis, and Staphylococcusaureus, along with a host of other microorganisms that have been implicated as potential mastitis agents. These microorganisms are described as major pathogens and are generally considered to be frequently associated with clinical mastitis in dairy animals.

Alongside microbiological factors, predisposing factors such as the environment, genetic predisposition, anatomical factors and nutritional factors also play an important role. Usually, mastitis occurs when microorganisms pass through the mammary gland. This can take place either during lactation or during the dry season. During breastfeeding, the infection can start from bacteria present on the outside of the nipple. At the end of the milking process, the teat duct remains dilated for 1-2 hours while strained teats may remain open, leaving the mammary gland exposed to new infections.

The importance of mastitis is mainly economic, such as reduced milk production and the cost of treatment, but also sanitary, especially with regard to dairy products, as well as legal (European directives 46/92 and 71/94 defining the microbiological quality of milk). All these issues can directly affect the dairy industry and the viability of dairy producers, as animals with mastitis are prone to new infections resulting from partial restoration or permanent damage of the mammary gland tissue.

In clinical practice, veterinarians treat cases of mastitis by administering antibiotics directly into the mammary gland using syringes suitable for intramammary infusion. The main disadvantages of antibiotic use are the development of resistant microbial strains, the high cost of treatment and consumer concerns regarding the possibility of antibiotic residues in milk, in cases where the milk produced after treatment has not been disposed of.

Prior art level

There are a number of publications that disclose the development of intramammary protective formulations for the treatment of mastitis in cattle.

Document numbers US7906138 and US8795714 B2 both describe an intramammary protection composition and a corresponding method of forming a natural barrier in the mammary duct of lactating non-human animals to prevent mammary disorders during the animal's dry season. The methods include the steps of injecting a formulation free of bismuth hyponitrate into the mammary duct of the animal. They also prevent the formation of black spots in dairy products, especially cheddar cheese, which is made from the milk of animals to which the formulation has been placed.

Patent number US6340469 describes an anti-infective formulation for the prevention of dry season bovine mastitis consisting of about 65% by weight bismuth hyponitrate in an aluminum stearate gel base. The sealant is prepared by adding the bismuth hyponitrate to the gel base, following at least two separate steps.

The patent number EP 2369937 B1 describes an intramammary protection composition comprising vegetable oils in the broad sense of oil without being limited to oil extracts, bismuth hyponitrate, liquid paraffin, aluminum stearate and silicon dioxide, as an intramammary sealant for the prevention or treatment of mastitis in animals.

Patent number EP 0971690 B2 describes the use of an intramammary protection pharmaceutical preparation which forms a natural teat duct barrier, particularly for the prevention of mastitis in cattle, without the use of antibiotics.

Patent number US6106838 describes various forms of veterinary medicinal products for veterinary and therapeutic applications, where they include essential oils as active ingredients, able to replace antibiotics due to the significant action they show against microorganisms that cause inflammation, infections and diarrhea in humans and animals . Essential oils high in thymol and carvacrol from the extract of thyme, oregano and others are reported to be effective antibiotics for the treatment of mastitis when used in vaseline-based intramammary preparations.

However, none of the above preparations can be considered edible as the raw materials used for their preparation and consequently the final product are not edible. Therefore, all of the above preparations must be removed from the mammary duct before the initiation of lactation since they are not suitable for immediate consumption, e.g. from newborn animals.

Thus, one of the major concerns with existing commercial intramammary formulations is that they must be removed before lactation begins and the milk must be discarded, as they are not safe for direct consumption by young animals or human consumers.

Purpose of the invention

The present invention provides an alternative and viable solution to the aforementioned problems. The formulations described here consist exclusively of edible raw materials and are therefore absolutely safe to be consumed directly, either by the young animals, or by the final consumers of the dairy products.

The final product is edible and does not require removal from the breast, fundamentally differentiating it from any existing product.

The technical objective of the product of the invention is to provide an intramammary protection formulation, an alternative to the already existing products consisting of bismuth hyponitrate and vegetable essential oils with antimicrobial properties.

Accordingly, bovine mastitis will be used as a working example in the context of the presentation of the invention. However, the applications of the present invention are not limited to bovine mastitis but may cover the entire range of mammary gland diseases.

Summary of the invention

According to the invention, preparations are proposed as defined in claim 1, as an intramammary protection preparation specifically for animals, specifically for dairy animals, which consists of at least one vegetable oil, at least one coagulating agent, at least one surfactant, at least one stabilizer, at least a hydrogel and at least one w/o emulsion or suspension, which is notable in that these formulations are in the form of structured oils or pastes or gels or biphasic oleogel-hydrogel systems, referred to as beijels, where the above vegetable oil includes all the oils that can form oil gels, where the above coagulation factor includes all the components that can form oil gels, where the above hydrogel includes all the known hydrogels in pharmaceutical technology.

According to a typical embodiment according to the invention, the formulations which are based on oil gels and consist of at least 75% vegetable oils and at least 5% of edible coagulating agents, have the form of a gel or paste.

According to another preferred embodiment of the invention, the formulations contain edible natural oils and edible coagulating agents, and are therefore edible and safe for use in intramammary applications. These preparations are intended for the prevention or treatment of diseases related to the mammary gland, such as, for example, mastitis, without being limited to it.

According to another further embodiment of the invention, veterinary or pharmaceutical preparations containing one or more edible vegetable oils and edible coagulating agents, their preparation methods and their applications are proposed. The formulations are used as intramammary infusions to prevent or treat infections of the mammary gland of non-human dairy animals.

According to a characteristic embodiment of the invention, the formulations proposed herein advantageously create a physical barrier which prevents the migration of bacteria from the outside of the nipple, into the nipple duct and finally into the breast, preventing possible infections by such bacteria.

The present invention further relates to a method of preventing or treating mammary tissue damage in non-human dairy animals. Accordingly, according to the invention, a method of preparing preparations applied to the mammary tissue for the prevention or treatment of diseases such as mastitis, without being limited to it, is proposed.

According to a further embodiment of the invention, methods of preparing formulations are also provided. The formulations proposed herein can be prepared by a method and suitable equipment for mixing the ingredients of the formulation to form a gel or paste or biphasic gel system, referred to as beijels, including all known.

A characteristic advantage of the above incorporation according to the invention, is the fact that the preparations described here promote the healing of ulcers and wounds as they promote the restoration of the intramammary environment by restoring the balance of fatty acids of the breast, in cases of infected tissues.

Another advantage of the above incorporation according to the invention is that the ingredients provided in the proposed formulations can have antimicrobial and/or antiviral properties. Thus according to yet another advantageous feature of the above embodiments of the invention, the proposed formulations act as an antimicrobial and/or antiviral agent in non-human animals.

The present invention thus also concerns specific uses of the above preparations prepared according to the invention for the prevention or treatment of diseases of the mammary tissue in non-human animals, where in particular the above diseases include mastitis.

A further use of the above compositions according to the invention is in the preparation of an intramammary infusion composition for the prevention or treatment of mammary gland TOU diseases of non-human animals.

A still further use of the above formulations according to the invention is in the preparation of a formulation for the prevention or treatment of diseases according to the preceding claim by applying it to mammary tissue to promote the healing of ulcers and wounds and to restore the balance of fatty acids of the udder in the case of an infected udder of a non-human animal.

According to a still further advantageously characteristic way of carrying out the invention, the formulations described here are edible and of food quality, therefore it is not necessary to remove them from the teat before milking the animal and there is no concern about possible residues of harmful substances or antibiotics in the milk produced, which greatly simplifies the whole milking process.

Additional advantages of the present invention are disclosed below from the further dependent claims and/or from the description of certain embodiments or formulations as described below according to the invention with preferred examples of preparation of formulations.

Brief description of the plans

Figure 1 shows oleogels of extra virgin olive oil with beeswax concentration of 5, 10, 15, 20 and 25% wax.

Figure 2 is a graphical representation of the texture analysis of the oleogels.

Figure 3 shows oleogels of extra virgin olive oil with candelillame wax concentration of 5, 10, 15, 20 and 25% in wax.

Figure 4 shows the phase separation of oleogels of extra virgin olive oil with cannellilla wax with a concentration of 5, 7.5, 10, 12.5 and 15 % wax.

Description of the invention

Unless otherwise indicated, all technical and scientific terms used herein are as understood by one of ordinary skill in the art to which this invention pertains. Similarly, when the terms "one, one, one" and "the, the, the" are used they may refer to the plural unless the text clearly states otherwise. Similarly, the term "or" is intended to include the term "and" unless the text clearly states otherwise.

The term "animal" as used herein refers to all mammals (including humans), birds and fish, including all vertebrates. This term also includes all animals at all stages of development, including embryos. The term "livestock" describes all populations and breeding of animals, used by humans as pets or productive animals for commercial purposes. Examples include, but are not limited to, animals such as cattle, lambs, pigs, birds, and the like. The term cattle as used herein generally refers to animals such as cow, bull, calf, etc. of all ages. The same applies to the terms pork, pig, pig, etc.

It is also noted that in the description of the invention and in particular in the claims, terms such as "includes" and the like, may have the meaning of "is included" according to the American terminology, while the terms "consists of" or "consists of" have the meaning of being it is possible to allow other characteristic elements that are not precisely mentioned, but in any case they do not include elements that may impinge on the novelty of the invention.

The present invention relates to veterinary or pharmaceutical preparations containing one or more edible vegetable oils and edible coagulating agents.

The present invention includes edible coagulants, which form oleogels when used in combination with vegetable oils. The term oleogel includes all types of gels consisting of an organic liquid phase within a three-dimensional network and/or all structured oils which have, for example, been solidified in the presence of a coagulating agent. The term coagulating agent includes all components that can form oleogels with vegetable oils, such as natural or synthetic waxes, waxes of plant origin, waxes of animal origin, natural and/or synthetic polymers, nanoparticles.

All oleogels are solid systems by definition. More specifically, oleogels prepared by mixing vegetable oils and edible coagulating agents are non-fluid hard waxy solids. Contrary to the fact that they are non-fluid hard waxy solids, it was here surprisingly observed that, when subjected to low shear stress mixing processes, the systems start to behave like viscous pastes, whose viscosity decreases with each mixing cycle. This remarkable behavior is attributed to the partial degradation of the three-dimensional lattice of the gel, which leads to the partial phase separation of the system. Gels made using beeswax tend to be more cohesive and compact, allowing for more cohesive and more stable pastes to be created. Oil gels made with carnauba and/or candelilla wax tend to undergo more intense phase separation, releasing free oil from the gel that is used as a nipple cleanser.

Additionally, the fact that the viscosity of the system decreases with each cycle of applied stress makes removal of material from the breast easier with each successive massage of the breast.

The present invention will be better understood by the description which will be carried out with preferred examples of formulations, where below such refer to the use of edible vegetable oils and edible coagulants of natural origin. The present invention is not limited to the examples described below but may cover all known ingredients in pharmaceutical science, which can be used in a similar manner to those described according to the present invention.

Example 1

To evaluate the ability of edible vegetable oils and edible coagulants to function in the desired manner, a base formulation was prepared. Edible extra virgin olive oil was used as a standard vegetable oil, while beeswax was used as a standard edible coagulant of natural origin. The formulation was as follows:

Table 1 shows the composition of the base formulation.

Material % By Weight

Extra Virgin Olive Oil 75 - 95

Beeswax 5 - 25

Table 1

The formulation was prepared following the following process:

1. Loading the extra virgin olive oil into a suitable heated vessel equipped with a low shear stirrer, to avoid air entrapment that can promote the oxidation of the oil and starting the heating, under an inert atmosphere, to avoid oxidation reactions. 2. Gradually add the beeswax in the form of flakes and increase the temperature of the system to 70<º>C, temperature 5<º>C above the melting point of the wax and maintain a constant stirring rate until the wax is completely dissolved. After the wax has dissolved the mixture should be clear with no visible solid residue. The system must not be heated above 80<º>C to avoid discoloration of the wax.

3. Stop stirring and gradually cool the system. Abrupt cooling is avoided as it may cause inhomogeneity in the final oleogel, 4. The final oleogel is in the form of a solid waxy material which does not flow.

Oil gels with a wax content of less than 5% collapse under their own weight and are therefore not preferred, as shown in Figure 1.

5. The solid oleogels are then subjected to low shear agitation to convert them into viscous, non-free-flowing pastes. Agitation may be accomplished using suitable low shear mixing devices, or a static mixer or any device capable of producing a similar effect. The rheological behavior of the products directly depends on the number of mixing cycles that will be carried out. The specific dependence is shown in Figure 2, where the texture analysis is presented where for each cycle of applied stress to the material, the material's resistance to pressure decreases and the resistance is due to the drag flow around the cantilever of the device. Oil gels with a cream consistency greater than 25% show great hardness and are difficult to process and are not preferred.

6. Filling 5 mL syringes with the oleogel paste and sterilizing them with radiation c. The material can exit the syringe by applying a maximum pressure of 10 kPa. The term syringe refers to the standard syringes used for infusions in veterinary intramammary applications.

Example 2

The formulation was as follows:

Table 2 shows the composition of the base formulation which also contains a fraction of free oil.

_ Material _ % By Weight _ Extra Virgin Olive Oil 75 - 95

_ Candelilla candle _ 5 - 25 _

The formulation was prepared following the following process:

1. Loading the extra virgin olive oil into a suitable heated vessel equipped with a low shear stirrer, to avoid air entrapment that can promote oxidation of the oil, and starting heating, under an inert atmosphere, to avoid oxidation reactions. 2. Gradual addition of candelilla wax flake form and increase the temperature of the system to 75 ° C, temperature 5<º>C above the melting point of the wax and maintaining a constant stirring rate until the wax is completely dissolved. After the wax has dissolved the mixture should be clear with no visible solid residue. The system must not be heated above 80 °C to avoid discoloration of the wax.

3. Stop stirring and gradually cool the system. Abrupt cooling is avoided as it may cause inhomogeneity in the final material.

4. The final oleogel is in the form of a solid waxy material which does not flow.

Oil gels with a wax content below 5% collapse under their own weight and for this reason are not preferred, as can be seen from Figure 3.

5. The solid oleogels are then subjected to low shear agitation and converted into viscous, non-free-flowing pastes. Agitation may be accomplished using suitable low voltage mixing devices, or a static mixer, or any device capable of producing a similar effect. The rheological behavior of the products is similar to the behavior of oleogels prepared with extra virgin olive oil and beeswax. Oil gels with a cream consistency greater than 25% show great hardness and are difficult to process and are not preferred.

6. Filling 5 mL syringes with the oleogel paste and sterilizing them with radiation c. The material can exit the syringe by applying a maximum pressure of 10 kPa. The term syringe refers to the standard syringes used for infusions in veterinary intramammary applications.

7. Oleogels prepared using extra virgin olive oil and candelilla wax show a mild phase separation (in the presence of free oil) which is proportional to the oil concentration of the gel, as shown in Figure 3. A controlled phase separation, as in the example of 15% in a waxy consistency, is desirable as the free oil can be used as a mammary duct cleanser of foreign bodies.

Example 3

The following example refers to the use of edible vegetable oils and edible waxes of natural origin, in combination with edible hydrogels. The specific example is not limited only to those mentioned, but covers all vegetable oils, coagulating agents, hydrogels and/or other natural ingredients, as understood by the expert in the technique to which the invention relates, that can be used with a corresponding way as described in the present example..

For the purposes of this example, the preparation of a formulation consisting of edible extra virgin olive oil, beeswax and aloe hydrogel is described. The composition of the preparation is as follows:

Table 3 shows the composition of a biphasic intramammary formulation system, combining oleogel with hydrogel.

Material_ % By Weight Oleogel

Extra Virgin Olive Oil 64 - 80

Beeswax 16 - 20

Hydrogel

Aloe Gel _ 0-20

Table 3

The formulation was prepared following the following process:

1. Loading the extra virgin olive oil into a suitable heated vessel equipped with a low shear stirrer, to avoid air entrapment that can promote oxidation of the oil, and starting heating, under an inert atmosphere, to avoid oxidation reactions. 2. Gradually add the beeswax in the form of flakes and increase the temperature of the system to 70<o>C, temperature 5<o>C above the melting point of the wax and maintain a constant stirring rate until the wax is completely dissolved. After the wax has dissolved the mixture should be clear with no visible solid residue. The system must not be heated above 80 °C to avoid discoloration of the wax.

3. Stop stirring and gradually cool the system. Abrupt cooling is avoided as it may cause inhomogeneity in the final oleogel.

4. The final oleogel is in the form of a solid waxy material which does not flow.

The solid oleogels are then subjected to low shear agitation and conversion into viscous pastes, which do not flow freely. Agitation may be accomplished using suitable low shear mixing devices, or a static mixer or any device capable of producing a similar effect.

5. The final oil gel is stirred until it is completely homogenized and transformed into a homogeneous paste without visible defects such as aggregates and clots, and then the aloe gel is added gradually. Mixing is continued until the system is completely homogenized with no distinct areas of oil gel or hydrogel.

6. Filling 5 mL syringes with the oleogel paste and sterilizing them with radiation c. The material can exit the syringe by applying a maximum pressure of 7kPa. The term syringe refers to the standard syringes used for infusions in veterinary intramammary applications.

The final biphasic system, characterized as beijel, combines the characteristics of both gels. For a composition of up to 20% in hydrogel, the system presents rheological characteristics similar to those of oil gel. For a composition greater than 20% in hydrogel the system loses its cohesion and flows freely.

Example 4

The following example refers to the use of edible vegetable oils and edible waxes of natural origin, in combination with edible hydrophilic systems. The specific example is not limited only to those mentioned but covers all vegetable oils, coagulants and/or other natural ingredients, as understood by the expert in the technique to which the invention relates, which can be used in a corresponding manner as described in the present example.

For the purposes of this example, the preparation of a formulation consisting of edible coconut oil, beeswax and edible medicated manuka honey (hydrophilic system) is described. The composition of the preparation is as follows:

Table 4 shows the composition of a biphasic intramammary formulation system, combining oleogel with medicated manuka honey.

_ Material _ % By Weight _

Oil gel

Coconut oil 60 - 80

Beeswax 15 - 20

Hydrogel

_ Medicinal Manuka Honey _ 0-20 _

Table 4

The formulation was prepared following the following process:

1. Loading the coconut oil into a suitable heated vessel equipped with a low shear stirrer, to avoid air entrapment that can promote oxidation of the oil, and starting heating, under an inert atmosphere, to avoid oxidation reactions.

2. Gradually add the beeswax in the form of flakes and increase the temperature of the system to 70 °C, temperature 5 °C above the melting point of the wax, and maintain a constant stirring rate until the wax is completely dissolved. After the wax has dissolved the mixture should be clear with no visible solid residue. The system should not be heated above 80°C to avoid discoloration of the wax.

3. Stop stirring and gradually cool the system. Abrupt cooling is avoided as it may cause inhomogeneity in the final material.

4. The final oleogel is in the form of a solid waxy material which does not flow.

The solid oleogels are then subjected to low shear agitation and conversion into viscous pastes, which do not flow freely. Agitation may be accomplished using suitable low shear mixing devices, or a static mixer or any device capable of producing a similar effect.

5. The final oil gel is stirred until it is completely homogenized and transformed into a homogeneous paste without visible defects such as aggregates and clots, and then the medicated manuka honey is added gradually. Mixing is continued until the system is completely homogenized with no distinct areas of oil gel or hydrogel.

6. Filling 5 mL syringes with the oleogel paste and sterilizing them with radiation c. The material can exit the syringe by applying a maximum pressure of 15 kPa. The term syringe refers to the standard syringes used for infusions in veterinary intramammary applications.

The final two-phase system combines the characteristics of both systems. For a composition of up to 20% medicated manuka honey, the system becomes exceptionally sticky due to the excess of honey.

Example 5

The following example refers to the use of edible w/o emulsions (or suspensions of hydrophilic particles) and edible waxes of natural origin. The specific example is not limited only to those mentioned but covers all vegetable oils, coagulants and/or other natural ingredients, as understood by the person skilled in the art to whom the invention relates, that can be used in a corresponding manner as described in the present example.

For the purposes of this example, the preparation of a formulation consisting of edible extra virgin olive oil, beeswax, edible medicated manuka honey (hydrophilic system) and a nonionic surfactant is described. The composition of the preparation is as follows:

Table 5 shows the composition of a biphasic intramammary formulation system, combining w/o emulsions (or suspensions of hydrophilic particles in edible vegetable oils) and edible waxes of natural origin.

Material_ % By Weight Oleogel

Extra Virgin Olive Oil 60 - 80

Beeswax 15 - 20

Span 85 0-1

Medicinal Manuka Honey_ 0-20

Table 5

The formulation was prepared following the following process:

1. Loading the extra virgin olive oil into a suitable heated vessel equipped with a low shear stirrer, to avoid air entrapment that can promote oxidation of the oil, and starting heating, under an inert atmosphere, to avoid oxidation reactions. 2. Add the surfactant and heat the system to 45°C. 3. Transfer of the mixture to a container equipped with a homogenizer (high shear stress process). The process of homogenization includes all kinds of homogenizers that could give the same result as that described in the invention.

4. The honey is preheated to 45<o>C, in order to reduce its viscosity and is gradually added to the oil under continuous homogenization.

5. The w/o emulsion prepared is transferred to a suitable heated vessel equipped with a low shear stirrer, to avoid air entrapment that can promote oil oxidation and start heating, under an inert atmosphere, to avoid oxidation reactions. 6. Gradually add the wax in the form of flakes and increase the temperature of the system to 70<o>C, temperature 5<o>C above the melting point of the wax and maintain a constant stirring rate until the wax is completely dissolved. After the wax has dissolved the mixture should be clear with no visible solid residue. The system should not be heated above 80°C to avoid discoloration of the wax.

7. Stop stirring and gradually cool the system. Abrupt cooling is avoided as it may cause inhomogeneity in the final material.

8. The final oleogel is in the form of a solid waxy material which does not flow.

9. The solid oleogels are then subjected to low shear agitation and converted into viscous, non-free-flowing pastes. Agitation may be accomplished using suitable low shear devices, or a static mixer or any device capable of producing a similar effect.

10. Filling 5 mL syringes with the oleogel paste and sterilizing them with radiation c. The material can exit the syringe by applying a maximum pressure of 10 kPa. The term syringe refers to the standard syringes used for infusions in veterinary intramammary applications.

Example 6

The following example refers to the use of edible vegetable oils enriched with edible vegetable infusions and edible waxes of natural origin. The specific example is not limited only to those mentioned, but covers all vegetable oils, coagulating agents and/or other natural ingredients, as perceived by the expert in the technique to which the invention relates, which can be used in a corresponding manner as describes the example. The composition of the preparation is as follows:

Table 6 shows the composition of the formulation of enriched edible vegetable oil with edible plant extracts and edible waxes of vegetable origin.

_ Material _ % By Weight _ Extra Virgin Olive Oil with

75 - 95 Sword Grass Extract

(, Hypericum Perforatum )

Candelilla wax _ _ 5 - 25 _ _

Table 6

The formulation was prepared following the following process:

1. Loading the enriched extra virgin olive oil with sword grass extract into a suitable heated vessel equipped with a low shear stirrer, to avoid air entrapment that can promote oxidation of the oil and starting heating, under an inert atmosphere, to avoid oxidation reactions.

2. Gradually add the flake wax and increase the temperature of the system to 75<o>C (temperature maintained 5<o>C above the melting point of the wax) and maintain a constant stirring rate until the wax is completely dissolved. After the wax has dissolved the mixture should be clear with no visible solid residue. The system should not be heated above 80<o>C to avoid discoloration of the wax.

3. Stop stirring and gradually cool the system. Abrupt cooling is avoided as it may cause inhomogeneity in the final material.

4. The final oleogel is in the form of a solid waxy material which does not flow.

Oil gels with a wax content below 5% collapse under their own weight and for this reason are not preferred, as shown in Figure 2.

5. The solid oleogels are then subjected to low shear agitation and converted into viscous, non-free-flowing pastes. Agitation may be accomplished using suitable low shear mixing devices, or a static mixer or any device capable of producing a similar effect.

6. Filling 5 mL syringes with the paste of the elapiket and sterilizing them with radiation c. The material can exit the syringe by applying a maximum pressure of 10 kPa. The term syringe refers to the standard syringes used for infusions in veterinary intramammary applications.

7. Oleogels prepared using enriched extra virgin olive oil with sedum extract and candelilla wax show a mild phase separation (in the presence of free oil) which is proportional to the oil concentration of the gel, as shown in Figure 3. A controlled phase separation, as in the example of 15% in a waxy consistency, is desirable as the free oil can be used as a mammary duct cleaner of foreign bodies.

Claims (16)

Claims 1. Intramammary protection preparation for animals, especially dairy animals, consisting of a) at least one vegetable oil, b) at least one coagulating agent, Y) at least one surfactant, d) at least one stabilizer, e) at least one hydrogel, f) at least one w /o emulsion or suspension, which is characterized by being a structured vegetable oil or paste or biphasic system of oleogel and hydrogel that forms the so-called beijel, where the oleogels are formed from the above vegetable oil, respectively from components such as the above coagulation factors, where the above hydrogels are those known in pharmaceutical technology. 2. Intramammary protection composition according to claim 1, characterized in that it is a structured-solid vegetable oil. 3. Intramammary protection preparation according to claims 1 or 2, characterized in that it is a combination of the above structured vegetable oils, specifically in the form of a solid and/or paste and/or gel and/or a biphasic system called bejel. 4. Intramammary protection preparation, according to one of claims 1 to 3, characterized in that the preparation includes oil gels consisting of at least 75% vegetable oils and at least 5% of edible coagulating agents, and is mainly in the form of a gel or paste, oleogels consisting of w/o emulsions of vegetable oils, oleogels consisting of suspensions of hydrophilic components in vegetable oils, oleogels consisting of enriched vegetable oils with vegetable extracts and oleogels consisting of vegetable oils respectively. 5. Intramammary protection formulation according to claim 4 is characterized in that it consists of natural edible vegetable oils and edible coagulating agents, with the result that they form a safe veterinary or pharmaceutical formulation for intramammary applications and is therefore edible and/or includes vegetable oils with honey and/or its derivatives and biphasic gels consisting of mixtures of vegetable oil gels with hydrogels. 6. Formulation according to one of the preceding claims, characterized in that a physical barrier is composed of the above formulation, wherein the above physical barrier prevents the migration of bacteria from the external environment of the udder to the interior of the animal. 7. A method of preparing formulations as defined according to claims 1 to 6, which is characterized in that the above formulations are prepared by mixing or contacting the components of the formulation to form a gel or paste or biphasic system with suitable mixing or contacting equipment. 8. Method for preparing the preparation as defined according to the previous claim, which is characterized in that the above preparation is prepared with the following steps: a) Loading the vegetable oil into a suitable heated container equipped with a low shear stress stirrer, to avoid air entrapment that can promote the oxidation of the oil and starting the heating, under an inert atmosphere, to avoid oxidation reactions. b) Gradually adding the wax in the form of flakes and increasing the temperature of the system to 70<o>C, temperature 5<o>C above the melting point of the wax and maintaining a constant stirring rate until the complete dissolution of the wax, where after the dissolution of the wax the mixture should be clear with no visible solid residue and the system should not be heated above 80<o>C to avoid discoloration of the wax. c) Cessation of stirring and gradual cooling of the system, where sudden cooling is avoided as it may cause inhomogeneity in the final material and the final oleogel is in the form of a solid waxy material which does not flow and ideally has a wax composition between 5% and 25 %. d) The solid oleogels are then subjected to low shear agitation and conversion into viscous, non-free-flowing pastes, where agitation may be effected using suitable low shear devices, or a static mixer or any device capable of similar result. e) Filling 5 mL syringes with the oleogel paste and sterilizing them with γ radiation, where the material can exit the syringe by applying limited pressure, namely a maximum pressure of 10 kPa, in particular where, step b consists in the gradual addition of the candelilla wax in flake form and heated to a temperature above the melting point of the wax, namely between 75 °C and 80 °C maintaining the stirring of the mixture until the complete dissolution of the wax, where still in particular the wax formulation is 15% candelilla, which allows controlled phase separation in which the free oil is used as a determinant of the mammary duct from foreign bodies. 9. Method of preparing the preparation according to claim 8, which is characterized in that the oil gel is stirred to form a homogeneous paste without visible defects such as aggregates or clots, where aloe gel is gradually added, allowing the above stirring until the formation of a homogeneous paste without distinct areas consisting of the two phases, the oleogel or the hydrogel, and where the above step g consists of filling the syringes, namely a volume of 5 mL with the oleogel paste, allowing flow through the mouth of the syringe applying a maximum pressure of 7 kPa . 10. A method of preparing the formulation according to claim 9, which is characterized in that in the above step a of the process, coconut oil is gradually loaded into the upper container, where the final oil gel is in the form of a white waxy solid material that does not flow, where the oleogel is stirred until a homogeneous paste without visible defects such as aggregates or clots is left and then honey, specifically manuka honey, is gradually added, where the stirring is continued until a homogeneous paste is formed without distinct areas consisting of the two phases, the oleogel or honey , where the oleogel paste can flow through the mouth of the syringe by applying a maximum pressure of 15 kPa. 11. A method of preparing the formulation according to claim 9, which is characterized in that in the above step b, a product defined as Span 85 is added and the mixture is preheated to 45<o>C under constant stirring, where the mixture is transferred to container equipped with a high shear homogenizer, the honey is preheated to 45°C to reduce its viscosity, it is gradually added to the mixture with the extra virgin olive oil under continuous homogenization, where the above syringe is also filled with the oil gel paste where the material can flows from the nozzle of the syringe applying a maximum pressure of 10 kPa. 12. Method of preparation of the formulation according to claim 9, which is characterized by the fact that in the above step a, the virgin olive oil with sedum extract is loaded into the above container, where candelilla wax in the form of flakes is gradually added, where the material can flow from the nozzle of the syringe applying a maximum pressure of lOkPa, where even the oleogels prepared from candelilla wax and extra virgin olive oil with sedum extract show a mild phase separation proportional to the concentration of the oil, with a controlled phase separation, specifically for a candelilla wax concentration of 15 %, achieving the creation of free oil used as a determinant of the mammary duct from foreign bodies. 13. Use of the composition as defined according to one of claims 1 to 6 in the preparation of a composition for the prevention or treatment of mammary tissue diseases in non-human animals, wherein in particular the above diseases include mastitis. Use of the composition as defined according to one of claims 1 to 6 in the preparation of an intramammary infusion composition for the prevention or treatment of diseases of the mammary gland of non-human animals. Use of the formulation as defined according to one of claims 1 to 6 in the preparation of a formulation which acts as an antimicrobial and/or antiviral agent in non-human animals. 16. Use of the above composition in the preparation of a composition for the prevention or treatment of diseases according to the preceding claim, by applying it to breast tissue to promote the healing of ulcers and wounds and to restore the fatty acid balance of the breast in the case of an infected breast non-human animal.