DE19741114A1 - Oral veterinary dosage forms - Google Patents

Abstract

Oral veterinary dosage forms (granules, pellets, powders or tablets) that are moisture-stable and resistant to gastric fluid comprise (a) a core that comprises or is coated with an acid-stable material that is soluble, swellable or "retarding" at neutral or basic pH and (b) an outer coating that is acid-labile or "retarding". Also claimed are aqueous suspensions of such dosage forms.

Description

The present invention relates to the development of a moisture stable and at the same time Enteric-coated oral dosage form for animals.

State of the art

The manufacture of moisture-stable and at the same time gastric juice-resistant oral dosage forms is of great importance in the manufacture of veterinary medicinal products. An example of the need for such pharmaceutical forms is the combating of viral and bacterial diseases in fish in pond management, lake and river fishing. However, the development of vaccine formulations against viral diseases has so far been problematic. Due to the high expenditure and the short protective effect, passive fish immunization is practically hopeless [Dresenkamp, dissertation Berlin 1992]. Only active immunization with inactivated or live vaccines is considered promising. The following options are described in the literature.

• 1. Schäperclaus (fish diseases, Akademie Verlag, (1990)) and Smith (Vaccination against vibrosis in fish vaccination (Ellis, A. Ed., Academic press, London, 67-84, (1988)) report on immunization procedures using intrapertonic injections. The ones to be vaccinated Fish are immersed in a narcotic solution, on a table after the effects begin placed and vaccinated with dosing syringes. However, such an application method is in the intensive mass fish farming impractical and associated with very high costs. In addition comes the high stress associated with vaccination for the fish. Also be large amounts of antigen required. The reasons mentioned contribute to the fact that despite good The protective effect of vaccination for fish immunization was only very limited.
• 2. The bath vaccination was successfully tested with inactivated bacterial vaccines (Kölbl, Tierärztliche Umschau 45, 624-629, 1990). To do this, put the vaccine in the fish tank given and the water supply and quantity throttled beforehand. Technical problems (e.g. River maintenance) and stress factors limit this use.
• 3. In a spray process that is also known, the fish are removed from the network and sprayed with an appropriate pressure (Gould et al. in Fish Pathol. 13, 63-68 (1978)). The method represents a high stress load for the fish. It also has the consequence that the Fish receive different amounts of vaccine and are therefore not always sufficient be immunized.
• 4. The oral application proves itself for mass vaccinations of animals of any size and especially suitable for young animals. The daily feeding schedule does not have to change so that the application is not associated with stress for the animals [Kolb, dissertation, Gießen, 1994]. Trying with gastric juice-insoluble coatings a drug form develop that allows immunization, however, was not sufficient because the gastric juice-resistant layer dissolved in the water after a short time and thus one effective immunization was prevented (Assmus and Schubert, dissertation Halle, 1980).

There are currently two options for administering the active ingredient or vaccine orally:

• a) An attempt is made to add the active ingredient to the feed preparation. However, problems arise from the high Antigen content, which must be 100 times greater than with parenteral administration, since it is already in the In advance by mechanical barriers, release or destruction of the antigen in the water or in the  Gastric effects are lost (Horsch, immunoprophylaxis in farm animals, Fischer Verlag, Jena, 1977).
• b) The most important alternative currently is that of Stampniok (dissertation, Halle 1985) developed lipid pearl. An acceptable immunization was thus achieved to reach. The disadvantage of this pharmaceutical form results from the high cost of production.

The object of the present invention is therefore to provide novel and inexpensive substances develop that are superior to the above-mentioned prior art.

A substance will now be described which has the disadvantages of the already known substances overcomes.

Description of the invention

The previous substances and processes have so far been inadequate due to high costs Possibility of transfer to large-scale production, high stress on the animals, limited uses in factory farming and inadequate protection of the Pharmaceutical form labeled in water.

The aim of the new substance is to immunize or give an oral application To achieve drug delivery. According to the invention this object is achieved in that it is the new substance for granules, pellets, powder or tablets for the treatment of animals acts as the outer layer at least one acid-labile or retarding coating have and in addition an acid-stable, but soluble at neutral or basic pH or contain swelling or retarding core or the core with an acid-stable, at neutral or basic pH value but soluble or swelling or retarding Material is covered. The outer layer preferably dissolves at a pH value of less than 5 or swells.

The basis of the new substance is a powder mixture, which is preferably made from potato starch and Lactose exists. However, they are also powder mixtures made from other substances such as starches or possible from feed bases. A solid active ingredient (e.g. Antibiotic or serum lyophilisate) added. Should this be unfavorable, then there is Possibility to add or dissolve the active ingredient or the serum in the binder. In addition, the serum can also be added directly to the powder and then by the Binders are solidified. They are used as binders in food chemistry and known pharmaceutical technology compounds such. B. PVP or gelatin Available.

With the aid of the binder, the powder mixture is thus solidified, whereby the particle size can be controlled by choosing the amount of liquid binder. Especially particles between 0.1 and 10 mm are favorable. The particle size can be changed that it comes closest to the food of the animals depending on their age and size. The Manufactured advantageously by granulators such. B. by a Fluid bed granulator or by a screen press granulator.

To realize the moisture and water stability as well as the acid stability According to the invention, various principles are available:

1. The outer shell is insoluble in the neutral and basic range, but swelling and acid-labile. The inner shell is acid-stable, but soluble in the neutral and basic area (see Fig. 1). In the case of active substances which are sensitive to solvents or live vaccines, the inner shell is advantageously coated as an aqueous dispersion.

The following materials are suitable for the outer shell:
Copolymers of acrylic acid (e.g. copolymers with a cationic character based on dimethylaminoethyl methacrylate and neutral methacrylic acid esters, copolymers with an anionic character based on methacrylic acid and methyl methacrylate, copolymers of acrylic acid and methyl methacrylate with a low content of ammonium groups).

Isopropanol, acetone and methylene chloride are preferred as solvents, or aqueous Dispersions used.

The following materials can be used for the inner shell:

• a) Shellac
  Alcohol is used as the solvent.
• b) cellulose derivatives (e.g. hydroxyethyl cellulose, cellulose acetate phthalate, cellulose acetate succinate)
  Isopropanol, acetone and methylene chloride are used as solvents.
• c) methacrylic acid derivatives (e.g. polymers with anionic character based on Methacrylic acid and methyl methacrylate, anionic copolymers based on Methacrylic acid and ethyl acrylate, copolymers based on methacrylic acid and Ethyl acrylate, copolymers of methacrylic acid and methyl methacrylate and methyl acrylate). These dispersions are in aqueous form and can be used for solvent-sensitive Fabrics are used.
• d) copolymers of acrylic acid
  (e.g. copolymer with a cationic character based on dimethylaminoethyl methacrylate and neutral methacrylic acid esters, copolymer with an anionic character based on methacrylic acid and methacrylic acid methyl ester).
  Isopropanol, acetone and methylene chloride or mixtures thereof are preferred as solvents.

2. The outer shell (see Fig. 2) is retarding in the neutral and basic area (delayed release) but swelling (see material under 1.). The inner shell is acid-stable, but soluble in the neutral and basic area (material see 2.). The following materials are used as the material for the outer shell:

• a) Copolymers of acrylic acid
  (e.g. copolymers of acrylic acid and methacrylic acid methyl esters with a low content of ammonium groups). Isopropanol, acetone and methylene chloride are used as solvents.

3. The outer shell (see Fig. 3) is insoluble in the neutral and basic area, but swelling. Inside there is a matrix that ensures a delay or protection against the acid. Macromolecular substances such as starch, carboxymethyl starch, cellulose ether, alginates, galactomanan are used as the matrix material. There is also the option of incorporating acrylic acid derivatives (see 2.a and b) as scaffolding agents.

4. The outer shell is insoluble in the neutral and basic range, but swelling. Inside, in addition to the powder mixture and the active ingredient, there is a basic ion exchanger (resinate) that prevents premature release in an acidic environment ( Fig. 4).
The following substances are available as basic ion exchangers: Pemutit ESB, Varion Ad, Anionit AW17, Dowex1, Nalcite SBW, Duolite A42, Amberlite IR400 or CG50, Lewatit MN, Permutit E or CCG, Lewatit MIH, Amberlite IR45, Duolite A6 , A7.

It is possible to color the outer protective cover as desired. This makes it possible to adapt the color to the usual feed for the animals. Flavors can also be used additionally be placed on the protective cover so that the animal species is not between the dosage form and Can distinguish feeding.

The principles presented prove to be particularly advantageous for encapsulation gastric juice sensitive or acid labile drugs and vaccines. First of all, protection is guaranteed before moisture or water, there is no premature release such as for example with the pure feed-vaccine mixtures. It also prevents Live vaccines such as in the direct mixing of vaccines, in feed and thus can get directly into the environment. The production of the new oral dosage form is easily possible on an industrial scale. The fabrics are readily available. The application of the substances is also easily possible in factory farming.

The new dosage form can be added to water like feed, but does not dissolve in it immediately. The composition can ensure that the substance can be fed according to the habits of the animals, for example, it is easily possible for animals that eat their food from the water surface (e.g. trout), in water to produce floating substances. Likewise, for animals that eat their food from the bottom, substances that sediment in water are easy to manufacture. The thickness of the water-insoluble The layer on the dosage form can be adapted to the necessary length of stay in the water. The Animals eat the particles that get into the stomach. The enteric coating, the matrix or the ion exchanger provides protection against the acid. The oral dosage form gets into the intestine. At a neutral pH, the layer, the active ingredients or, dissolves the vaccine will be released.

The present invention opens up various possibilities for administration a wide variety of medicines, including vaccines, high quality Feeds such as B. vitamins and minerals to a wide variety of animals. Especially it is suitable for use on fish.

The substances according to the invention are particularly suitable for animals as bait, for all types of feed admixtures or substances to be fed that are high in moisture are exposed or fed in a moistened or suspended state.

If the substance is exposed as bait in the forest, for example, it will rain or Moisture for no loss of active ingredient. The dosage form is eaten by the animal and after passing through the stomach without loss of active ingredient or titer (live vaccine) in the Gut where it releases the active ingredient at a neutral pH.

The following examples illustrate the invention without restricting it.

example 1 (Granules for oral application of viral hemorrhagic septicemia (VHS) vaccine)

A first powder mixture is made from 175 g potato starch and 75 g lactose by trituration in a mortar. 35 g of polyvinylpyrrolidone (Kollidon, BASF) and 700 mg of a 2% VHS serum are dissolved in 35 g of distilled water. According to the effectiveness studies, the virus titer in the VHS oral vaccine is 10 ⁴ KID ₅₀ / g.

The granulation is carried out with an AR 400 perforated disc granulator from Erweka (Frankfurt / M). The granules are air dried. Then the granules overdrawn.

The coating is carried out using the fluidized bed process (Wurster attachment). For this we use a Uni-Glatt fluidized bed granulator from Glatt Ingenieurtechnik GmbH (Weimar) utilized. A copolymer of acrylates is used as the inner coating (preparation 4110 D, Röhm Pharma, Darmstadt). It is an aqueous dispersion, so none Destruction of the live vaccine occurs. The coating amount is 200 ml. The coating time is 60 min. The supply air temperature is 22 ° C so as not to kill the viruses. The Dosing pump works with an average of 0.8 ml / min. As a perforated disc on the granulator size B is used to achieve optimal swirling.

A mixture of 30 g Eudragit S to 200 g is used for the outer coating Isopropanol / acetone (ratio 1: 1) used. The coating time is 100 min. Here too lies the supply and exhaust air temperature at 22 ° C. The dosing pump works with an average of 0.8-2 ml / min. The color of the granules is blue to make a clear distinction from the To reach fish excrement. The granules are 20 cm in size in the basin Trout eaten and the vaccine gets into the stomach (without early release) Intestine. There the vaccine is released.

Example 2 (Granules for oral application of oxytetracycline (OTC))

A first powder mixture of 350 g potato starch and 150 g lactose is obtained by trituration made in a mortar. 15 g of polyvinylpyrrolidone are added to 75 ml of distilled water (Kollidon, BASF) and 25 g OTC incorporated.

The granulation is carried out with a perforated disc granulator from Erweka. The granules is air dried. The granulate is then coated. The cover comes with Using the fluidized bed process (Wurster attachment). We do this Fluid bed granulator Uni-Glatt from Glatt is used. As an inner coating is a Mixture of 20 g triacetin, 0.5 g Tween 80 and 3 parts defoamer in 200 ml water stirred in. The above suspension is stirred into 500 g of Eudragit RS30 D. The Coating time is 60 minutes. The supply air temperature is 45 ° C to ensure the fastest possible To achieve drying. The dosing pump works with an average of 0.8 ml / min. For the outer coating is a mixture of 60 g Eudragit S on 400 g isoprop./acetone (ratio 1: 1) used. The coating time is 100 min. The supply and exhaust air temperature is also here at 45 ° C. The dosing pump works with an average of 0.8-2 ml / min. As a perforated disc Size B used to achieve optimal swirling. The granules are eaten by both fish and mammals and the active ingredient gets through the Stomach (without early release) in the intestine. The active ingredient is released there.  

Example 3 (Granules for oral application of chloramphenicol)

A first powder mixture of 350 g potato starch and 150 g lactose is obtained by trituration made in a mortar. 15 g of polyvinylpyrrolidone are added to 75 ml of distilled water (Kollidon, BASF) and 25 g chloramphenicol incorporated.

The granulation is carried out with a perforated disc granulator from Erweka AR 400 (Frankfurt / M, FRG). The granules are air dried. Then the granules overdrawn. The coating is made using the fluidized bed process (Wurster attachment) carried out. We use a Uni-Glatt fluidized bed granulator from Glatt (Weimar, Germany) used. A mixture of 20 g triacetin, 0.5 g Tween 80 and 3 is used as the inner coating Proportion of defoamer stirred into 200 ml of water. The above suspension is in 500 g Eudragit RS30 D (Röhm Pharma, Darmstadt, Germany) stirred in. The coating time is 60 minutes. The supply air temperature is 45 ° C in order to achieve the fastest possible drying. The Dosing pump works on average with 0.8 ml / min. For the outer coating is a Mixture of 60 g Eudragit S on 400 g isoprop./acetone (ratio 1: 1) was used. The Coating time is 100 min. Here, too, the supply and exhaust air temperature is 45 ° C. The Dosing pump works with an average of 0.8-2 ml / min. The size B used to achieve optimal swirling. The granules are both from Fish as well as eaten by mammals and the active ingredient reaches the stomach (without premature release) in the intestine. The active ingredient is released there.

Example 4 (Granules for oral application of against transmissible gastroenteritis (TGE) vaccine)

A first powder mixture is made from 175 g potato starch and 75 g lactose by trituration in a mortar. 45 g of polyvinylpyrrolidone (Kollidon, BASF) and 700 mg of a 2% TGE virus suspension are dissolved in 45 g of distilled water. According to the studies on efficacy, the virus titer in the TGE oral vaccine is 10 ⁴ - 10 ⁵ (KID ₅₀ ). The granulation is carried out with a perforated disc granulator from Erweka AR 400 . The granules are air dried. The granulate is then coated.

The coating is carried out using the fluidized bed process (Wurster attachment). A fluidized bed granulator from Glatt is used for this. A copolymer of acrylates is used as the inner coating (preparation 4110 D, Röhm Pharma, Darmstadt). It is an aqueous dispersion so that there is no destruction of the live vaccine. The coating amount is 200 ml. The coating time is 60 minutes. The supply air temperature is 22 ° C so as not to kill the viruses. The dosing pump works with an average of 0.8 ml / min. Size B is used as a perforated disc in order to achieve optimal swirling. A mixture of 60 g Eudragit S on 200 g isoprop./acetone (ratio 1: 1) is used for the outer coating. The coating time is 100 min. The supply and exhaust air temperature is also 22 ° C here. The dosing pump works with an average of 0.8-2 ml / min. Size B is used as a perforated disc in order to achieve optimal swirling. The granules are added to the drinking water of pigs. These take up the vaccine while drinking.

List of figures

Fig. 1 Dosage form consisting of an outer shell, which is insoluble in the neutral and basic range, but swelling and acid-labile. The inner shell is acid-stable, but soluble in the neutral and basic area.

Fig. 2 Dosage form consisting of an outer shell, which is retarding (delayed release) in the neutral and basic area, but swelling. The inner shell is acid-stable, but soluble in the neutral and basic area.

Fig. 3 Dosage form consisting of the outer shell, which is insoluble in the neutral and basic area, but swelling. Inside there is a matrix that ensures a delay or protection against the acid.

Fig. 4 Dosage form consisting of the outer shell, which is insoluble in the neutral and basic area, but swelling. Inside, in addition to the powder mixture and the active ingredient, there is a basic ion exchanger (resinate), which prevents premature release in an acidic environment.

Claims (15)

1. Moisture-stable and enteric-coated granules, pellets, powders or tablets for the oral treatment of animals, characterized in that they have at least one acid-labile or retarding coating as the outer layer and additionally an acid-stable, but soluble or swelling or retarding core at neutral or basic pH contain or the core is coated with an acid-stable material which is soluble or swelling or retarding at a neutral or basic pH value. 2. Moisture-stable and enteric-coated granules, pellets, powder or tablets for oral treatment of animals according to claim 1, characterized in that the outer polymer dissolves or swells at a pH of 5. 3. Moisture-stable and enteric-coated granules, pellets, powder or tablets for oral treatment of animals according to claims 1 to 2, characterized in that the acid-labile material is compounds from the Substance classes of the copolymers of acrylic acid. 4. Moisture-stable and enteric-coated granules, pellets, powder or tablets for oral treatment of animals according to claim 3, characterized in that as copolymers of acrylic acid copolymers with cationi cal character based on dimethylaminoethyl methacrylate and neutral Methacrylic acid esters and / or copolymers with an anionic character based on Methacrylic acid and methyl methacrylate and / or copolymers of acrylic acid and Methacrylic acid methyl esters with a low content of ammonium groups used become. 5. Moisture-stable and enteric-coated granules, pellets, powder or tablets for oral treatment of animals according to claims 1 to 4, characterized in that it is the acid-stable or swelling or retarding material around compounds from the substance classes of the polymers and Copolymers of methacrylic acid. 6. Moisture-stable and enteric-coated granules, pellets, powder or tablets for oral treatment of animals according to claim 5, characterized in that as polymers and copolymers of methacrylic acid poly merisates with anionic character based on methacrylic acid and methacrylic acid methyl esters, anionic copolymers based on methacrylic acid and ethyl acrylate, Copolymers based on methacrylic acid and ethyl acrylate, copolymers with cationic character based on dimethylaminoethyl methacrylate and neutral Methacrylic acid esters, copolymer with anionic character based on Methacrylic acid and methyl methacrylate, copolymers of methacrylic acid and Methyl methacrylate and methyl acrylate can be used.   7. Moisture-stable and enteric-coated granules, pellets, powder or tablets for oral treatment of animals according to claims 1 to 4, characterized in that as an acid-stable or swelling or retarding material Shellac or cellulose derivatives can be used. 8. Moisture-stable and enteric-coated granules, pellets, powder or tablets for oral treatment of animals according to claim 7, characterized in that as cellulose derivatives hydroxyethyl cellulose, Cellulose acetate phthalate or cellulose acetate succinate can be used. 9. Moisture-stable and enteric-coated granules, pellets, powder or tablets for oral treatment of animals according to claims 1 to 4, characterized in that an ion exchanger is used as the retarding material. 10. Moisture-stable and enteric-coated granules, pellets, powder or tablets for oral treatment of animals according to claims 1 to 9, characterized in that as matrix formers for the core starch, carboxymethyl starch, cellulose ether, alginates, Galktomanan, or polymers of acrylic acid can be used. 11. Aqueous suspensions of the moisture-stable and gastric juice-resistant granules, pellets, Powders or tablets for the oral treatment of animals according to claims 1 to 10. 12. Use of oral dosage forms according to claims 1 to 11 as Medicated feedingstuffs or medicated baits for animals. 13. Use of oral dosage forms according to claims 1 to 11 as Medicated feed for fish. 14. Use of oral dosage forms according to claims 1 to 11 as feedable Vaccine preparation for animals. 15. Use of oral dosage forms according to claims 1 to 11 as feedable Vaccine preparation for fish.