AU2008201605A1 - Palatable ductile chewable veterinary composition - Google Patents

Description

Australian Patents Act 1990 Regulation 3.2 ORIGINAL COMPLETE SPECIFICATION STANDARD PATENT Invention Title "Palatable ductile chewable veterinary composition" The following statement is a full description of this invention, including the best method of performing it known to me/us:- Q \OPER\AS\2008\ApriU0S l5637 div filing dmsdoc PI\OPER\ 2\O8(3O55637 div SPcO ArO.doC412/20D0 00 -1- Palatable ductile chewable veterinary composition This is a divisional of Australian Patent Application No. 2004262492, the entire contents of which are incorporated herein by reference.

The present invention relates to an easy-to-use, safe, efficacious, and stable 00 veterinary formulation consisting of a highly palatable ductile chewable veterinary 00 Scomposition comprising an effective amount of one or more ingredients that are active against animal pests, pathogens or animal diseases; of meat flavoring; of partially gelatinized starch; of a softener; and of up to 9% of water. The present invention also relates to a method of controlling said animal pests or pathogens and of curing or preventing said animal diseases by feeding an animal with said highly palatable ductile chewable veterinary composition. Further, the invention relates to a process for producing said highly palatable ductile chewable veterinary composition by cold extrusion. In a preferred embodiment, the highly palatable ductile chewable veterinary composition controls animal pests like endo-parasites, such as worms, and simultaneously ecto-parasites, such as biting insects like fleas, on pets. The pesticidally effective ingredient is dispensed as the animal chews the product.

Field and background of the invention Veterinary products can be administered to warm-blooded animals in very different ways depending on their mode of action and their ability to be taken up either by the treated animal or the target pest. Thus veterinary products can be administered, for example, topically as pour-on or spot-on formulations, in form of shampoos, showers, as a dip, bath or spray, in form of a collar, and in many variants of these application forms. They can also be administered systemically, for example, orally, parenterally and in certain cases even transdermally. Examples of systemic administration forms are: via injection, as a tablet, capsule, bolus, drink, feed additive and the like. Each of these administration forms can have advantages or disadvantages depending on the actual situation and the animal that is in need of such a treatment. Treatment of herd animals, like horses, cattle, sheep or poultry usually requires different administration methods than for the treatment of single animals, such as pets like dogs and cats.

PAOPERMASN2O 30515637 div spec AprOB dOc.411008 00 0 -1A- One very convenient and easy to manage administration form for human patients is the oral uptake of a medicament. This would also be very desirable in the field of veterinary medicine but here the animal holder or veterinarian is confronted with the natural behavior of the animal and oral treatment can be a real challenge.

NO

00 1 WO 2005/013714 PCT/EP2004/008538 -2- 00 N Many attempts have been made to design the ideal oral application form that is really e accepted and voluntarily taken up by the animal but most of these application forms need still to be improved.

The present inventors recognized that in the field.of animal health the dosage form and 1especially the palatability of the dosage form, i.e. the natural acceptance of the drug plays O the decisive role. The underlying problems are outlined hereinafter.

00o While, in humans, medicaments may be administered in a wide variety of application forms, such as tablets, coated tablets, emulsions, injection solutions, suppositories and the like, because the discipline and the desire to recover in human patients can be relied upon, in the case of animals practical problems are soon encountered, since a few application forms, such as the usage of suppositories, either have to be dispensed with all together or other forms, such as injections, must only be carried out by the veterinarian.

In general, humans do not like to visit the doctor. The same is true for animal keepers who would need advice from a veterinarian. In general, the animal keeper prefers to use those treatment methods that he can carry out himself without having involved a veterinarian.

Among the preferred treatment methods, which an animal keeper can carry out himself, e.g.

following the veterinarian's instructions, is the oral administration of medicaments.

Treating humans with medicines is generally not problematic, because the human patient follows the advice of the doctor or reads the directions on the leaflet in the package and complies with them since this is in his own interest, and because the manufacturer usually prepares the tablet, capsule or coated tablet in a form which is appropriate for oral consurnmption -and-has -been tailored for humaR patients-.

However, as soon as a pharmaceutical active ingredient has a taste which is unpleasant to the animal, whether because it is bitter or has some other unpleasant taste or is simply alien to the animal, the animal refuses to take it orally. This inbom behavior occurs to varying degrees among the different species of animals, and essentially depends on their conventional eating habits. Unfortunately, only a few active ingredients have a neutral taste, so that the problem being discussed here is almost always present.

WO 2005/013714 PCT/EP2004/008538 -3- 00 c1 In the case of a human patient, an unpleasant tasting active ingredient can be masked C relatively easily, e.g. by coating it with a neutral-tasting or sweet layer. Everybody has come across gelatin capsules or tablets coated with sugar or lacquer at some time or other. It is easy to instruct the human patient to take the preparation without chewing.

n An animal-must-have a-natural willingness to take a medicinal preparation orally, which means that the medical preparation must taste well and be palatable. Of course, an C) individualanimal o-a few animals can also be forced to take a medicament, by making it 00 swallow or by injecting it. However, such forced methods are not only unacceptable to large animal operations but also to single dogs and cats which tend to bite or scrape if they are not willing to be treated. This is why animal treatment can be very labor-intensive or can require the intervention of a veterinarian and this ultimately leads to increase of costs.

Therefore, for pets but equally for animals that are kept on a large scale, simple and safe oral application forms are required, which can be easily administered by the animal keeper, which lead to reliable results, and which are affordable.

The chewable composition according to the present invention is not only suitable for replacing the treatment with a tablet or capsule. These chewables can also easily be mixed with conventional non-medicated feed pellets if herds of animals have to be treated.

Due to their excellent palatability the chewables according to the present invention are taken up by animals without causing any acceptance problems. Their handling is easy and safe, and can be adapted to the need either of an individual animal like a cat or a dog or to a herd animals like sheep and cows.

When reviewing the administration of capsules and coated tablets to animals, it has been shown that these application forms are rather unsuitable for animal medicine, since in the case of herd animals they can only be used in a controlled manner with considerable effort on a daily basis, and in the case of pets, such as dogs and cats, lead to particular acceptance problems. As already mentioned above, the eating habits of animals generally play a decisive role when using oral application forms. Thus, most important is an attractive taste and the palatability.

WO 2005/013714 PCT/EP2004/008538 -4- 00 C' In the case of dogs, it has been observed that they gnaw at solid food, e.g. on bones, and O- gulp down other food, either in the form of large scraps or wet formulated food, almost unchewed. If a tablet or coated tablet is mixed with the wet formulated feed, varying results are obtained. In a few cases, the tablet is not noticed by the dog at all and is simply gulped down, and in other cases it remains uneaten in the dog bowl. In contrast to dogs, cats are considerably more fastidious in their eating habits. Only in the rarest cases can a tablet or S coated tablet be mixed with the formulated food, without them noticing it immediately and C rejecting it. Although cats also to not exactly chew their food, they generally break it down 00 with a few small bites. They thereby damage the protective coating of a tablet or capsule and Srelease the unpleasant tasting active ingredient. Attempts to mix the active ingredient directly with the feed likewise fail, because either the degree of dilution is insufficient to neutralize the unpleasant taste or the active ingredient breaks down too rapidly when in contact with the feed. For the same reasons, mixtures of feed, active ingredient and excipients, which should stimulate the appetite of dogs and cats, similarly do not have a successful outcome with cats. Whereas the test animals rush eagerly to a placebo which has a corresponding appetite stimulant, i.e. a tablet consisting of feed, flavoring and other excipients, but no active ingredient, the test animals reject the same combination as soon as active ingredient is added. Clearly, a different technical solution must be found to the existing problem with animals.

Of course, any other active ingredient which is suitable for animals can be administered according to the present invention, but especially those active ingredients that have the taste disadvantages mentioned initially and are therefore not willingly taken orally by animals.

Basically, a diversity of individual active ingredients or mixtures of active ingredients may be -considered,-e;g-those-acting-against-external (ecto)-or-intemal-(endo)-parasites-or-activeingredients acting against animal diseases including viral or bacterial infections, behavioral disorders, such as hypo- or hyper-activity, inflammatory diseases, and auto-immune diseases. Thus, the active ingredient can be a pesticide or a medicament or a mixture of both.

It should be kept in mind that the present invention deals with an optimized application form for veterinary compositions rather than with the treatment of animals with a specific class of active ingredients. On the contrary, the present invention provides an easy-to-use, safe, WO 2005/013714 PCT/EP2004/008538 00 Spowerful, and stable veterinary formulation consisting of a highly palatable ductile chewable C- veterinary composition, which allows to administer orally almost each and any active ingredient to a warm-blooded animal, provided that this active ingredient or mixture of active ingredients is at the administered dose physiologically acceptable to the animal, does not display unacceptable side effects and, what is most important, exhibits after oral uptake t3 ;systemic activity. This means-that the main prerequisite for the active ingredient is that after NO oral administration it is taken up by the body fluids, including blood and lymph, and transported to the animal pest, the pathiogen or the diseased organ where it can exhibit its 00 activity. Thus, any active ingredient or class of active ingredients mentioned hereinafter is nothing but a non-limiting example of suitable active ingredients. The application form of the present invention is actually not limited to existing active ingredients but also suitable for each and any active ingredient developed in the future provided that the future active ingredient meets the main characteristics explained hereinbefore.

The highly palatable ductile chewable veterinary composition of the present invention is in principle a medicated food product and everybody working in this area is aware of the technical problems that arise in context with the production of medicated feed. For example, stability of the active ingredient is very crucial. It is a matter of fact that many potent active compounds are somewhat unstable (temperature-sensitive), above all when in contact with feed material, especially close contact to vegetable and animal materials, during conventional extrusion of feed pellets, result in considerable losses of active ingredient.

For example, when feed pellets are prepared via extrusion, the dried organic starting material of animal or vegetable origin is ground, is intimately mixed with the active ingredient, that is to say is substantially homogenized, and then is moistened with water or steam and is compressedinto-pellets-at-elevated-temperatures-and-under-pressures-f-around-1-00-kbar- However, said high pressures and the permanent high temperatures in the range of 100 0 C are disadvantageous and do not only dramatically reduce the viscosity of the pellets but result in a considerable lost of active ingredient.

Whereas most active ingredients in pure form or in contact with carriers that are routinely used in the production of tablets or capsules withstand such relatively high temperatures per se very well and can be stored in pure form or as tablets or capsules at room temperature for months or years without any measurable loss of active ingredient, they decompose relatively WO 2005/013714 PCT/EP2004/008538 -6- 00 rapidly under pressure and in intimate contact with animal or vegetable fibers in feedstuffs and under the prevailing elevated temperatures. It appears that contact with the fibers actually catalyses the decomposition process. Even when the elevated-pressure and elevated-temperature phase is kept as short as technically possible and the finished pellets are immediately cooled down to room temperature directly after the compression process, a quarter to a third of the active ingredient is nevertheless lost. Even though in the rare cases where the degradation products do not have disadvantageous effects on the animals treated, the unavoida6ble loss of active ingredient inevitably results ina considerable increase 00 in the cost of the final product. Thus extrusion processes can lead to very undesirable effects.

For the reasons mentioned, therefore, much effort has been directed at stabilizing temperature-sensitive active ingredients so that they withstand the elevated temperatures and pressures during pellet preparation without loss of active substance and also, when in the form of the finished pellets, have a long-term storage stability suitable for practical purposes.

Unsuccessful attempts at such stabilization include, for example, reduction of the active ingredient surface area by means of compression into granules, a very great variety of granule sizes having been tried; sealing of the said active ingredient granules in a very great variety of protective layers, for example gelatin or various sugars and coatings; (3) enclosure of the active ingredient within porous materials such as, for example, various celluloses, starches, silicic acids or zeolites, with or without additional protective layers; and chemical modification of the basic macrocyclic structure of the active ingredient. Although in a few cases chemical modification has resulted in improved stability of the compound per se,it-has-simultaneously-resulted-in-loss-of-activity7 However, none of those attempts has resulted in an appreciably smaller loss of active ingredient on compression into feed pellets or in measurably improved storage stability.

Moreover, success has now been achieved, surprisingly, in providing the user with the userfriendly, easy-to-use, safe, powerful, stable, and especially highly palatable chewable veterinary composition of the present invention.

WO 2005/013714 PCT/EP2004/008538 -7- 00 N Astonishingly, it is now possible to provide a product that not only withstands the extrusion CL process undamaged but also survives for a outstanding long storage period.

Therefore, it is highly surprising and was absolutely unpredictable that even so the chewable veterinary composition of the present invention contains a relatively high amount of meat material, this has obviously when combined with the appropriate amount of partially N gelatinized starch, no adverse effect on the stability of the active ingredient. It actually turned out that the chewable eterinary comriposition-of the present invention is a very stable product 00 that can be stored at room temperature over many months without significant loss or S degradation of active ingredient. Tests with stored material demonstrate that the palatability is not decreased and the efficacy of the active ingredient stays at a high level.

Moreover, investigations of the kinetic behavior demonstrate another surprising effect. It could not have been foreseen that the administration of the chewable veterinary composition of the present invention could lead to absolutely the same level of bioavailability as the administration of tablets or capsules. Thus, the present invention provides a safe, easy to use and stable product that is at least as efficacious as conventional oral application forms, like tablets or capsules.

Many biocides and veterinary medicines that may be now be incorporated into the chewable veterinary composition and be used according to the present invention, have been known to skilled specialists for a long time but the conventional oral dosage forms are not satisfactory because they are not attractive for animals and show the disadvantages discussed above.

With the chewable veterinary composition of the present invention one can combat all kinds ofparasites-Eteal-arasites-also-called-etoparasites-are-understood-to-be-parasiteswhich normally live on the animal, i.e. an the animal's skin or in the fur. Enclosed are biting insects, such as mosquitoes, blowfly, fleas or lice, or members of the order Acarina, e.g.

mites or ticks. Suitable products against external parasites include insecticides and acaricides. It does not matter what their mode of action actually is. They can be e.g. chitin synthesis inhibitors, growth regulators; juvenile hormones; adulticides. They can be broadband insecticides, broad-band acaricides. The active ingredient can be a killer or a deterrent or repellent. It can affect e.g. only adult stages or juvenile stages of the parasite or may affect any stage. The only prerequisite is that the active ingredient acts systemically. This WO 2005/013714 WO 205/03714PCT/EP2004/008538 -8- 00 means that it is not decomposed after oral uptake but transported by the body fluids to the skin or organ where the parasite uses to live.

If the active ingredient is an acaricide one can, for example, select a systemically acting acaricide from one of the following well-known classes of acaricides including: antibiotic acaricides such as abamectin, doramectin, eprinomectin, ivermectin, milbemnectin, NO nikkomnycins, selamnectin, tetranactin, and thuringiensin; bridged diphenyl acaricides such as azobenzene, benz*oxirn ate,' benzyl benzoate, bromopro .pylate, chlorbenside, chlo feneth .ol, 00 chlorfenson, chlorfensuiphide, chlorobenzilate, chloropropylate, dicofol, diphenyl sulfone, 0 dofenapyn, fenson, fentrifanil, fluorbenside, proclonol, tetradifon, and tetrasul; carbamnate acaricides such as benomyl, carbanolate, carbaryl, carbofuran, fenothiocarb, methiocarb, metolcarb, promacyl, and propoxur; oxime carbamate acaricides such as aldicarb, butocarboxim, oxamyl, thiocarboxime, and thiofanox; dinitrophenol acaricides such as binapacryl, dinex, dinobuton, dinocap, dinocap-4, dinocap-6, dinocton, dinopenton, dinosulfon, dinoterbon, and DNOC; formamidine acaricides such as amitraz, chlordimeforrn, chloromebuform, formetanate, and formparanate, mite growth regulators such as clofentezine, dofenapyn, fluazuron, flubenzimine, flucycloxuron, flufenoxuron, and hexythiazox; organochlorine acaricides such as bromocyclen, camphechlor, dienochlor, and endosulfan; organotin acaricides such as azocyclotin, cyhexatin, and fenbutatin oxide; pyrazole acaricides such as acetoprole, Fipronil and analogues and derivatives thereof, tebufenpyrad, and vaniliprole; pyrethroid acaricides including: pyrethroid ester acaricides like acrinathrin, bifenthrin, cyhalothrin, cypermethrin, alpha-cypermethrin, fenpropathrin, fenvalerate, flucythrinate, flumethrin, fluvalinate, tau-fluvalinate, and permethrin, and pyrethroid ether acaricides like halfenprox; quinoxaline acaricides such as chinomethionat and thioquinox; sulfite ester acaricides such as propargite; tetronic acid acaricides such as spirodiclofen-and-from-unclassified-acaricidessch-acequinocyl,-amidoflumet--arser~usoxide, chioromethiuron, closantel, crotamiton, diafenthiuron, dichiofluanid, disulfiram, fenazaflor, fenazaquin, fenpyroximate, fluacrypyrim, fluenetil, mesulfen, MNAF, nifluridide, pynidaben, pyrimidifen, sulfiram, sulfiuramid, sulfur and triarathene.

Suitable insecticides acting either as adulticides or insect growth regulators (IGRs) can be chosen from a variety of well-known different chemical classes such as chlorinated hydrocarbons, organophosphates, carbamates, pyrethroids, formamidines, borates, phenylpyrazoles, and macrocyclic lactones (previously known as avermectins). Prominent WO 2005/013714 PCT/EP2004/008538 -9- 00

O

CN representatives of adulticides/insect killers are imidacloprid, fenthion, fipronil, allethrin, resmethrin, fenvalerate, permetrin, malathion and derivatives thereof. Insect adulticides kill the insect in almost any development stage either by contact or as a stomach poison. Widely used representatives of insect growth regulators (IGRs) are, for example benzoylphenylureas such as diflubenzuron, lufenuron, noviflumuron, hexaflumuron, ^V triflumuron, and teflubenzuron or substances like fenoxycarb, pyriproxifen, methoprene, NO kinoprene, hydroprene, cyromazine, buprofezin, pymetrozine and derivatives thereof. Insect 0 growth inhibitors or insect growth regulators (any of which is commonly known as an IGR) 00 are products or materials that interrupt or inhibit the life cycle of a pest.

It goes without saying that the highly palatable ductile chewable veterinary composition according to the present invention is also very suitable for administering active ingredients that combat internal parasites (endo-parasites) such as worms living in the blood or in organs of the animal. Thus, the active ingredient can be an anthelmintic (dewormer).

Anthelmintics (dewormers) are a heterogeneous group of drugs but they are selectively toxic to worms. The drugs can achieve this by either inhibiting the metabolic process vital to the parasite, or by causing the parasite to be exposed to higher concentration of drug than are the hosts cells, which means that one makes use of the existence of an advantageous therapeutic window. Anthelmintics can affect the target parasite during treatment by interfering with the integrity of parasite cells, inhibiting neuromuscular transmission and coordination, or mechanisms which protect against host immunity, that ultimately lead to the starvation, neuromuscular paralysis, death and expulsion of the parasite. Anthelmintics are commonly administered by drench, paste, orally, or by injection. The drugs are absorbed into the blood stream and widely diffused. They are metabolized in the liver and excreted in feces -and-urine:-An-the-animal-health-field-anthelminties-are-used-widely-used-against-roundworms-, lungworms, tapeworms, intestinal worms, whipworms, hookworms, pinworms, trichinella (trichinosis), and other less common organisms, liver flukes and other less common organisms in a broad range of animals such as beef, cattle, swine, goats, horses, and pets like cats and dogs. The activity spectrum of anthelmintics for dogs and cats embraces Trematodes such as Alaria alata and Opisthorchis tenuicollis; Cestodes such as Taenia hydatigena, Taenia pisiformis, Taenia ovis, Hydatigena Taenia taeniaeformis, Echinococcus granulosus, Echinococcus multilocularis, Dipylidium caninum, Diphyliobothrium latum, Multiceps multiceps, Multiceps serialis, Mesocestoides lineatus, and Mesocestoides corti; I 1 WO 2005/013714 PCTIEP2004/008538 00 and Nematodes such as Ancylostoma caninum, Uncinaria stenocephaia, Toxocara canis, SToxocara cati, Toxascaris leonina, Strongyloides stercoralis, Filaroides osieri, Capillaria aerophila, Capillaria plica, Capillaria hepatica, Trichinella spiralis, Angiostrongylus vasorum, Trichuris vulpis, Spirocerca lupi, Dirofilaria immitis, Ancylostoma tubaeforme, and Aelurostrongyius abstrusus.

NO Internal parasites within the present invention include all species of worm infestation (helminthes) but also 6acteria and viruses causing bacteial[and viral infections,in particular 00 those that infest the organs or parts of the body, such as the lungs, heart, alimentary tract or Sextremities, or which spread through the whole organism.

The anthelmintic can be selected from endo-parasiticides and endecticides including one of the following well-known groups of dewormers such as macrocyclic lactones (sometimes called simply macrolides), benzimidazoles, pro-benzimidazoles, imidazothiazoles, tetrahydropyrimidines, organophosphates and piperazines.

A most preferred group of anthelmintics consists of the more modern natural or chemically modified macrocyclic lactones (macrolides), such as avermectins, milbemycins and derivatives thereof, including prominent representatives such as Ivermectin, Doramectin, Moxidectin, Selamectin, Emamectin, Eprinomectin, Milbemectin, Abamectin, Milbemycin oxime, Nemadectin, and a derivative thereof, in free form or in the form of a physiologically acceptable salt.

The macrocyclic lactones are most preferred because they exhibit a broad spectrum of activity. Most of them exhibit ecto and in parallel endo-parsiticidal activity. Therefore, they -are-also-called-endectocides:- Macrocyclic-actones-bind-to-glutamated-chlorine-channels causing in the first instance paralysis and later on the death of the parasite.

In the context of the invention, a preferred group of macrocyclic lactones is represented by compounds of formula I) WO 2005/013714 WO 205/03714PCT[EP2004/008538 00 22 3 23 CH3

H

RI 0 H C0 0 OH H

(I)

X

CH

3 c-I

H

00 wherein X is or Y is -C(H 2 or C(=N-00H 3 R, is hydrogen or one of radicals H 3 CO H 3 CO H 3

CO

0- HO 0- 0 0 0 H 3 C H 3 C

H

3

C

or CH 3

-O-CH

2 -CO-NH

CO-O-

R

4 is hydroxyl, -NH-CH 3 or -NH-OCH 3

R

2 is hydrogen, -CH 3

-C

2 1- 5

-CH(CH

3

)-CH

3

CH(CH

3

)-C

2

H

5 l, -C(0H 3

)=CH-CH(CH

3 2 or cyclohexyl; and if the bond between atoms 22 and 23 represents a double bond the carbon atom in 23-position is unsubstituted so that Y is if is the bond between atoms 22 and 23 is a single bond the carbon atom in 23position is unsubstituted or substituted by hydroxy or by the group =N-O-CH 3 so that Y is

C(H

2 or -C(=N-OCH 3 in free form or in the form of a physiologically q-cqeptaLe salt Typical and especially preferred representatives of compounds of formula I are: 1) Ivermectin is 22,23-Dihydroabamectin; 22,23-dihydroavermectin B 1; or 22,23-dihydro C- 0768 1, wherein X is Y is -C(H 2 R, is the radical WO 2005/013714 ~VO 205/03714PCT/EP2001/008538 12- 00 c-IH 3 CO H3CO HO 0 0- 0 0

H

3 C H 3

C

R

2 is either -CH(CH 3

)-CH

3 or -CH(CH 3

)-C

2

H

5 and the bond between atoms 22 and 23 represents a single bond. Ivermectin is known from US-4,199,569.

2) Doramectin is 25-Cyclohexyl-5- 0- demethyl-25-de(1 -methylpropyl)avermectin A 1 a, 00 wherein X is Y is R, is the radical

H

3 CO H 3

CO

HO 0 0- 0 0

H

3 C 1- 3

C

R

2 is cyclohexyl and the bond between atoms 22 and 23 represents a double bond.

Doramectin is known from US-5,089,480.

3) Moxidectin, is [6 R ,23 E, 25 S E )J5- 0- Demethyl-28-deoxy-25-(1,3-dimethyl-1butenyl)-6,28-epoxy-23-(methoxy im ino)milbemycin B, wherein X is Y is

C(=N-OCH

3 R, is hydrogen; R 2 is -C(CH 3

)=CH-CH(CH

3 2 and the bond between atoms 22 and 23 represents a single bond. Moxidectin, is known from EP-O,237,339 and US- 4,916,154.

4) Selamnectin is 25-cyclohexyl-25-de( I-methylpropyl)-5-deoxy-22,23-dihydro-5- (hydroxyimino)avermectin B1 monosaccharide and thus a compound of formula (i ),wherein X is Y is -C(H 2 R, is the radical

H

3 C0 HO 0- 0

H

3

C

R

2 is cyclohexyl; and the bond between atoms 22 and 23 represents a single bond.

Selamnectin is known e.g. from: ECTOPARASITE ACTIVITY OF SELAMECTIN; A novel endectocide for dogs and cats. A Pfizer Symposium, held in conjunction with The 17th WO 2005/013714 WO 205/03714PCTIEP2004/008538 -13- 00 c-i international Conference of the World Association for the Advancement of Veterinary Parasitology, 19 August 1999. Copenhagen, Denmark.

Emamnectin is (4primeprime R 0 -demethyl-4primeprimedeoxy-4primeprime- (methlamino) avermectin A Ila and (4primeprime R 0 kn 4primeprime-deoxy-4primeprime-(methylamino)-25-(I -methylethyl)avermectin A 1 a 1), NO wherein X is Y is R, is- H 3 C0 H 3

CO

00

CH

3 -NH 0 0c-i0 0

H

3 C H 3

C

R

2 is -CH(CH 3

)-CH

3 or -CH(CH 3

)-C

2 Hs, and the bond between atoms 22 and 23 represents a double bond. Emamnectin is known from US-4,874,749.

6) Eprinomectin is (4primeprime R )-4primeprime- epi- (acetylamino)-4primeprimedeoxyavermectin B 1, wherein X is Y is R, is the radical

H

3 CO H 3

CO

CH 3 00NH 0 0- 0 0

H

3 C H1 3

C

R

2 is -CH(CH 3

)-CH

3 or -CH(CH 3

)-C

2

H

5 and the bond between atoms 22 and 23 represents a double bond. Eprinomectin is known from US-4,427,663.

7--ibmci-s(.,5R-5Odmty-2=ex-62=pxy2-mtymbm cn wherein X is Y is -C(H 2 R, is hydrogen; R 2 is -CH 3 or -C 2

H

5 and the bond between atoms 22 and 23 represents a single bond. Milbemnectin is known from US-3,950,360.

8) Abamnectin is Avermectin B 1 which is also named 5- 0- demethylavermectin A 1 a and 0- demethyl-25-de(1 -methylpropyl)-25-(1 -methylethyl)avermectin A 1 a wherein X is Y is R, is the radical WO 2005/013714 PCT/EP2004/008538 -14- 00

H

3 CO H 3

CO

HO 0 0- 0 0

H

3 C H 3

C

R

2 is -CH(CH 3

)-CH

3 or -CH(CH 3

)-C

2

H

5 and the bond between atoms 22 and 23 represents a double bond. Abamectin is known from US-4,310,519.

\O

S9) Milbemycin oxim is milbemycin A 4 5-oxime; milbemycin A 3 5-oxime, wherein X is 00 Y is -C(H 2 R, is hydrogen; R 2 is -CH(CH 3

)-CH

3 or -CH(CH 3

)-C

2

H

5 and the N bond between atoms 22 and 23 represents a single bond. Milbemycin oxim is known from US-4,547,520.

The compound of the formula wherein X is Y is -C(H 2

R

1 is the radical

CH

3 -O-CH-CO-NH CO-O-

R

2 is -CH 3 or C 2

H

5 and the bond between atoms 22 and 23 represents a single bond. This compound is known from WO 01/83500.

11) Nemadectin is antibiotic S-541A; also named [6 R, 23 S, 25 0- Demethyl-28deoxy-25-(1,3-dimethyl-1 -butenyl)-6,28-epoxy-23-hydroxymilbemycin B; wherein X is =CH- OH; Y is -C(H 2

R

1 is hydrogen; R 2 is -C(CH 3

)=CH-CH(CH

3 2 and the bond between atoms 22 and 23 represents a single bond. Nemadectin is known from US-4,869,901.

The compounds specifically mentioned under items 1-11 hereinbefore, are preferred embodiments of the present invention and can be used either alone or in combination with another endo-parasiticide, ecto-parasiticide or endecticide.

Benzimidazoles, benzimidazole carbamate and pro-benzimidazoles interfere with energy metabolism by inhibition of polymerization of microtubules and include very potent compounds such as thiabendazole, mebendazole, fenbendazole, oxfendazole, oxibendazole, albendazole, luxabendazole, netobimin, parbendazole, flubendazole, cyclobendazole, febantel, thiophanate and derivatives thereof.

1 WO 2005/013714 PCT/EP2004/008538 00 N Imidazothiazoles are cholinergic agonists and include highly active compounds such as tetramisole, levamisole, and derivatives thereof.

Tetrahydropyrimidines act are also cholinergic agonists and include highly active compounds such as morantel, pyrantel, and derivatives thereof.

Organophosphates are inhibitors of cholinesterase. This class includes potent compounds such as dichlorvos, haloxon, trichlorfon, and derivatives thereof.

O Piperazines exhibit anticholinergic action and block neuromuscular transmission. This class S includes-highly active compounds such as piperazine and derivatives thereof.

00 Salicylanilide selected from closantel, tribromsalan, dibromsalan, oxychlozanide, clioxanide, rafoxanide, brotianide, bromoxanide and derivatives thereof.

Within the present invention the anthelmintic (dewormer) a preferred embodiment consist of a combination of a macrocyclic lactone and an anthelmintic selected from the group consisting of Albendazole, Clorsulon, Cydectin, Diethylcarbamazine, Febantel, Fenbendazole, Haloxon, Levamisole, Mebendazole, Morantel, Oxyclozanide, Oxibendazole, Oxfendazole, Oxfendazole, Oxamniquine, Pyrantel, Piperazine, Praziquantel, Thiabendazole, Tetramisole, Trichlorfon, Thiabendazole, and derivatives thereof. Most preferred is Praziquantel. In order to broaden the activity spectrum towards ecto-parasites said anthelmintic combination can contain in addition to the dewormers a parasiticidally effective amount of an insecticide, acaricide or an insecticide and an acaricide. Of course one could also add an antibiotic for treating bacterial disease.

All of the suitable parasiticides mentioned hereinbefore are known. Most of them are described in THE MERCK INDEX 1999 by Merck Co Inc, Whitehouse Station, NJ, USA; published on CD-ROM by Chapman Hill/CRC, 1999, Hampden Data Service Ltd. and in -theJiteatuespecificaly-mentionednT HE-MERCKJNDEX-1.999, Suitable antimicrobial active ingredients are, e.g. various penicillins, tetracyclines, sulfonamides, cephalosporins, cephamycins, aminoglucosids, trimethoprim, dimetridazoles, erythromycin, framycetin, fruazolidone, various pleuromutilins such as thiamulin, valnemulin, various macrolides, streptomycin and substances acting against protozoa, e.g. clopidol, salinomycin, monensin, halofuginone, narasin, robenidine, etc.

WO 2005/013714 PCT/EP2004/008538 -16- 00

O

O

N Behavioral disorders include e.g. separation worry or travel sickness of dogs and cats. A suitable compound acting against behavioral disorders is e.g. clomipramine.

The chewable combination according to the present invention may also contain an active ingredient for the treatment of disfunctions or hypo-activity.

N0 Dysfunction or hypo-activity is understood to include functions like autoimmune disorders, which deviate from the normwhether through inborn or acquired damage to individual 00 organs or tissue. This complex also includes rheumatic diseases, pathological changes to 0 S joints, bones or internal organs, and much more. A prominent representative of compounds that can be used in this complex area is cyclosporine and derivatives thereof. The term "animal disease" even includes different types of cancer and metastasis progression in connective tissues that are common in animals. In this field bisphosphonates like coledronate, clodronate, etidronate, pamidronate and alendronate play an important role.

Said bisphosphonates can also be administered in the treatment or prophylaxis of ulcers, rheumatoid arthritis and other arthitides, and periodontitis. Another suitable class of active ingredients encompasses anti-inflammatory agents such as benzenesulfonamides like Deracoxib, which is extremely suitable for the control of pain and inflammation associated with osteoarthritis. Further anti-inflammatory agents are diclofenac and derivatives thereof.

In the present invention, the administration problems depicted in connection with conventional oral dosage forms, like tablets and capsules, can be very easily resolved and chewable products can be prepared, which are taken orally by the animals without causing any problems. The animals actually take the chewable veterinary composition voluntarily.

Summary-of-the-I nventionr The present invention overcomes the disadvantages and shortcomings of the prior art by providing an easy-to-use, safe, powerful, and stable veterinary formulation consisting of a highly palatable ductile chewable veterinary composition which is produced by an extrusion process wherein the product is extruded at or near room temperature, and where the extruder is cooled down below room temperature, preferably to 5-10 0 C. The palatable ductile chewable composition constitutes a veterinary composition and is administered orally. The composition is capable of killing endo-parasites and ecto-parasites and/or can be used for WO 2005/013714 PCT/EP2004/008538 -17- 00 0 CNl treating prophylactic or curative animal diseases, and it is useful for the treatment of any warm-blooded non-human animal, including herd animals, like horses, cattle, sheep or poultry and preferably pets like dogs and cats.

O

The highly palatable ductile chewable veterinary composition of the invention is composed of in an organic composition which contains an effective amount of one or more active N0 ingredients, preferably an effective amount of a mono, binary or ternary mixture of organic O compounds-capable of controlling ecto-parasites, endo-parasites or bacterial or viral 00 pathogens or a combination of ecto-parasites, endo-parasites, bacterial or viral pathogens.

O Depending on the mode of action the highly palatable ductile chewable veterinary composition of the invention contains a parasiticidally or anti-pathogenically effective amount of one or more active ingredients. The expression "parasiticidally effective amount" refers to that amount of active ingredient in the composition which will fully control the target parasite which means that 95-100%, preferably 98-100% or close to 100% of the parasites are killed and the active ingredient is nevertheless well tolerated. The expression "anti-pathogenically effective amount" refers to that amount of active ingredient in the composition which will efficiently cure a bacterial, viral or behavioral disease or if administered prophylactically will suppress the outbreak of such a disease. The highly palatable ductile chewable veterinary composition of the invention comprises an effective amount of one or more ingredients that are active against animal pests, pathogens or animal diseases; it further comprises meat flavoring and partially gelatinized starch, and it comprises of a softener; and of up to 9 preferably 3-7 most preferred 4-6 of water. It is essential that that during the extrusion process the extruder is cooled down below room temperature. A temperature range of 5-10°C is ideal.

EaGh-of-the-fllowing-pargraphs-defines-a-prefeFred-embedimentof-the-pesent-inventier A highly palatable ductile chewable veterinary composition that comprises an effective amount of one or more ingredients that are active against animal pests, pathogens or animal diseases; meat flavoring; partially gelatinized starch; a softener; and (E) optionally up to 9 water.

A highly palatable ductile chewable veterinary composition as defined above capable of controlling endo-parasites and simultaneously ecto-parasites of non-human animals.

WO 2005/013714 PCT/EP2004/008538 -18- 00

O

Cr A highly palatable ductile chewable veterinary composition as defined above wherein the animal disease comprises bacterial infections, viral infections, behavioral disorders, inflammatory diseases, and auto-immune diseases.

A highly palatable ductile chewable veterinary composition as defined above comprising to 30 of a natural meat flavoring.

NO

O A highly palatable ductile cheviable veterinary composition as defined above wherein the 00 natural meat flavoring comprises 20 to 55 fat.

O

A highly palatable ductile chewable veterinary composition as defined above comprising to 70 of partially gelatinized starch.

A highly palatable ductile chewable veterinary composition as defined above wherein the partially gelatinized starch comprises 12 to 17 of gelatinized starch.

A highly palatable ductile chewable veterinary composition as defined above comprising to 20 preferably about 11-15 of a softener, based upon the weight of the partially gelatinized starch.

A highly palatable ductile chewable veterinary composition as defined above wherein the softener is selected from the group consisting of glycerol, polyethylene glycol and polypropylene glycol.

A highly palatable ductile chewable veterinary composition as defined above comprising up to-9--(wlw)-preferably-3-to7-%-(w/w)-more-preferably-4to-6-%-(w/w-of-water- A highly palatable ductile chewable veterinary composition as defined above comprising 1 to (wlw), preferably 3 to 7 of a sweetener.

A highly palatable ductile chewable veterinary composition as defined above comprising 0 to (wlw), preferably 0.01 to 0.5 of an antioxidant.

WO 2005/013714 PCT/EP2004/008538 -19- 00

O

O

N A highly palatable ductile chewable veterinary composition as defined above comprising 0 to preferably 0.05 to 2 of a coloring agent.

A highly palatable ductile chewable veterinary composition as defined above comprising 0 to 4% of sodium chloride.

N0 A highly palatable ductile chewable veterinary composition as defined above comprising an O parasiticidally effective amount of an ecto-parasiticide, an endo-parasiticide, an endectocide 00 or of a combination of a parasiticide selected from the group consisting of an ecto- 0 0 parasiticide, an endo-parasiticide and an endectocide.

A highly palatable ductile chewable veterinary composition as defined above wherein the ecto-parasiticide is active against insects, members of the order Acarina or insects and members of the order Acarina.

A highly palatable ductile chewable veterinary composition as defined above wherein the ecto-parasiticide is an insecticide which is either an insect adulticides or insect growth regulators.

A highly palatable ductile chewable veterinary composition as defined above comprising an parasiticidally effective amount of an endo-parasiticide or endecticide selected from the group consisting of macrocyclic lactones, benzimidazoles, pro-benzimidazoles, imidazothiazoles, tetrahydropyrimidines, organophosphates and piperazines.

A highly palatable ductile chewable veterinary composition as defined above comprising an effective-amount-of-a-natural-or-chemically-modified-macroGyclic-lactone-Gf-foFmnula-(-I WO 2005/013714 PCT/EP2004/008538 00 R I o 0 SH H 00 H

O

00 H wherein X is or Y is -C(H 2 or

C(=N-OCH

3

R

1 is hydrogen or one of radicals H CO H 3 CO H 3

CO

R4 o0 0 O HO 0- 0 0 0

H

3 C H 3 C H 3

C

or CH 3 -O-CH2-CO-NH- CO-0-

R

4 is hydroxyl, -NH-CH 3 or -NH-OCH 3

R

2 is hydrogen, -CH 3

-C

2 Hs, -CH(CH 3

)-CH

3

CH(CH

3

)-C

2

H

5

-C(CH

3

)=CH-CH(CH

3 2 or cyclohexyl; and if the bond between atoms 22 and 23 represents a double bond the carbon atom in 23-position is unsubstituted so that Y is or if is the bond between atoms 22 and 23 is a single bond the carbon atom in 23position is unsubstituted or substituted by hydroxy or by the group =N-O-CH 3 so that Y is

C(H

2 or -C(=N-OCH 3 in free form or in the form of a physiologically acceptable salt.

A highly palatable ductile chewable veterinary composition as defined above comprising an effective amount of a natural or chemically modified macrocyclic lactone of formula (I wherein X is Y is -C(H 2

R

1 is the radical

CH

3

-O-CH

2 -CO-NH CO-O- WO 2005/013714 PCT/EP2004/008538 -21 00 C

R

2 is -CH 3 or C 2

H

s and the bond between atoms 22 and 23 represents a single bond.

A highly palatable ductile chewable veterinary composition as defined above wherein the animal pests are external animal parasites or internal animal parasites or both.

t A highly palatable ductile chewable veterinary composition as defined above wherein the N macrocyclic lactone is selected from the group consisting of avermectins, milbemycins and derivatives thereof, in free form or in the form of a physiologically acceptable salt.

00 O A highly palatable ductile chewable veterinary composition as defined above wherein the macrocyclic lactone is selected from the group consisting of Ivermectin, Doramectin, Moxidectin, Selamectin, Emamectin, Eprinomectin, Milbemectin, Abamectin, Milbemycin oxime, Nemadectin, and a derivative thereof, in free form or in the form of a physiologically acceptable salt.

A highly palatable ductile chewable veterinary composition as defined above comprising an effective amount of a macrocyclic lactone in combination with an effective amount of an anthelmintic selected from the group consisting of Albendazole, Clorsulon, Cydectin, Diethylcarbamazine, Febantel, Fenbendazole, Haloxon, Levamisole, Mebendazole, Morantel, Oxyclozanide, Oxibendazole, Oxfendazole, Oxfendazole, Oxamniquine, Pyrantel, Piperazine, Praziquantel, Thiabendazole, Tetramisole, Trichlorfon, Thiabendazole, and a derivative thereof.

A highly palatable ductile chewable veterinary composition as defined above comprising additionally an effective amount of an insecticide, acaricide or an insecticide and an -aearieide 7 A highly palatable ductile chewable veterinary composition as defined above comprising an effective amount of milbemycin oxime and praziquantel.

A highly palatable ductile chewable veterinary composition as defined above comprising an effective amount of lufenuron, praziquantel and milbemycin oxime.

WO 2005/013714 PCT/EP2004/008538 -22- 00 C A highly palatable ductile chewable veterinary composition as defined above comprising an S effective amount of cyclosporin.

SA highly palatable ductile chewable veterinary composition as defined above comprising an effective amount of an antimicrobial selected from the group consisting of a penicillin, Stetracycline, sulfonamide, cephalosporin, cephamycin, aminoglucosid, trimethoprim, dimetridazole, erythromycin, framycetin, fruazolidone, pleuromutilin, streptomycin and a compound that is active against protozoa.

00 0 O A highly palatable ductile chewable veterinary composition as defined above comprising an effective amount of compound that is active against behavioral including separation worry or travel sickness of dogs and cats.

A highly palatable ductile chewable veterinary composition as defined above wherein the active ingredient or a different chemical class is an insecticide or acaricide.

A highly palatable ductile chewable veterinary composition as defined above wherein the insecticide is selected from the group consisting of insect killers and insect growth regulators.

Another preferred embodiment of the present invention is a method of controlling said animal pests or pathogens and of curing or preventing said animal diseases by feeding an animal with said highly palatable ductile chewable veterinary composition.

Yet another preferred embodiment of the present invention is a method of controlling said *animal-pests-or-pathogens-and-ef-euring-er-preventing-said-animal-diseases-by-feeding-ap animal with said highly palatable ductile chewable veterinary composition.

Yet another preferred embodiment of the present invention is a process for the production of a highly palatable ductile chewable veterinary composition as defined above, comprising (i) feeding the hopper of an extruder with an effective amount of one or more ingredients that are active against animal pests, pathogens or animal diseases; meat flavoring; partially gelatinized starch; a softener; and up to 9% (wlw) of water, (ii) cooling constantly down the mixture of active ingredients and carriers so that the temperature of the extrudate in the WO 2005/013714 PCT/EP2004/008538 -23- 00 C extruder does during the whole extrusion process at no time exceed 400C, (iii) pressing the S extrudate through a die that is decisive for the shape of the chewable product, and (iv) cutting the extrudate that leaves the extruder into equal pieces.

Yet another preferred embodiment of the present invention is a process as defined above wherein the hopper of the extruder is fed continuously and simultaneously with pre-mixture N and pre-mixture wherein pre-mixture consist of a homogenized mixture of one or more'actiVe iigredients and partially gelatinized starch, and pre-mrixture consists of a 00 homogenized mixture of meat flavoring, a softener and optionally of a carrier selected from the group consisting of a sweetener, softener, an antioxidant, a coloring agent and sodium chloride.

Yet another preferred embodiment of the present invention is a process as defined above wherein the extruder is cooled down below room temperature.

A further preferred embodiment of the present invention is a method of controlling nonhuman animal pests or nonhuman animal pathogens or of curing or preventing nronhuman animals diseases comprising feeding an animal with a palatable ductile chewable veterinary composition as defined above.

A further preferred embodiment of the present invention is a method as defined above, wherein the palatable ductile chewable veterinary composition consist of one chewable portion containing an effective amount of a compound or mixture of compounds capable of controlling nonhuman animal pests or nonhuman animal pathogens or of curing or preventing nonhuman animals diseases.

A further preferred embodiment of the present invention is a method as defined above, wherein the amount of active ingredient is adjusted to the bodyweight of the nonhuman animal that is in need of the treatment.

Another preferred embodiment of the present invention is the use of an effective amount of one or more ingredients that are active against animal pests, pathogens or animal diseases; meat flavoring; partially gelatinized starch; a softener; up to 9% WO 2005/013714 PCT/EP2004/008538 -24- 00 t

C

water; and an active ingredient suitable for combating animal pests, pathogens or animal 9^ diseases for the preparation of a highly palatable ductile chewable veterinary composition.

SAnother preferred embodiment of the present invention is the use as defined above, comprising 20 to 30 of a natural meat flavoring.

Another preferred embodiment of the present invention is the use as defined above, wherein N the natural meat flavoring coriprises 20 to 55 fat: 00 SAnother preferred embodiment of the present invention is the use as defined above, comprising 25 to 70 of partially gelatinized starch.

Another preferred embodiment of the present invention is the use as defined above, wherein the partially gelatinized starch comprises 12 to 17 of gelatinized starch.

Another preferred embodiment of the present invention is the use as defined above, comprising 10 to 20 of a softener, based upon the weight of the partially gelatinized starch.

Another preferred embodiment of the present invention is the use as defined above, wherein the softener is selected from the group consisting of glycerol, polyethylene glycol and polypropylene glycol.

Another preferred embodiment of the present invention is the use as defined above, comprising 3 to 7 of water.

Another preferred embodiment of the present invention is the use as defined above, wherein the animal pests are external animal parasites or internal animal parasites or both.

Another preferred embodiment of the present invention is the use as defined above, comprising 1 to 10 of a sweetener.

Another preferred embodiment of the present invention is the use as defined above, comprising 0 to 3.5 of an antioxidant.

WO 2005/013714 PCT/EP2004/008538 00 O0 S Another preferred embodiment of the present invention is the use as defined above, S comprising 0 to 5 of a coloring agent.

Another preferred embodiment of the present invention is the use as defined above, comprising 0 to 4% of sodium chloride.

Another preferred embodiment of the present invention is the use as defined above, 00 comprising an parasiticidally effective amount of an ecto-parasiticide, an endo-parasiticide, 0 an endectocide or of a combination of a parasiticide selected from the group consisting of an ecto-parasiticide, an endo-parasiticide and an endectocide.

Another preferred embodiment of the present invention is the use as defined above, wherein the ecto-parasiticide is active against insects, members of the order Acarina or insects and members of the order Acarina.

Another preferred embodiment of the present invention is the use as defined above, wherein the ecto-parasiticide is an insecticide which is either an insect adulticides or insect growth regulators.

Another preferred embodiment of the present invention is the use as defined above, comprising an parasiticidally effective amount of an endo-parasiticide or endecticide selected from the group consisting of macrocyclic lactones, benzimidazoles, pro-benzimidazoles imidazothiazoles, tetrahydropyrimidines, organophosphates and piperazines.

SAnother-preferFed-embodiment-of-the-present-invention-is-the-use-as-defined-abovecomprising an effective amount of a natural or chemically modified macrocyclic lactone of formula (I) WO 2005/013714 WO 205/017 14PCT/EP200S/008538 26 00 22 2 3 CH 3 OT

R

H 2 CH 3 wherein X is ;or Y is -C(H 2 or

C(=N-OCH

3 R, is hydrogen or one of radicals

H

3 00 H 3

C

HO 0-

R

4 is hydroxyl, -NH-CH 3 or -NH-00H 3

R

2 is hydrogen, -OCH 3

-C

2

H

5

-CH(CH

3

)-CH

3

CH(CH

3

)-C

2 Hs, -C(CH 3

)=CH-CH(CH

3 2 or cyclohexyl; and if the bond between atoms 22 and 23 represents a double bond the carbon atom in 23-position is unsubstituted so that Y is or if is the bond between atoms 22 and 23 is a single bond the carbon atom in 23position is unsubstituted or substituted by hydroxy or by the group =N-0-CH 3 so that Y is

C(H

2 or -C(=N-OCH 3 in free form or in the form of a physiologically acceptable.sait.

Another preferred embodiment of the present invention is the use as defined above, wherein the macrocyclic lactone is a compound of the formula I wherein X is Y is

C(H

2 R, is the radical WO 2005/013714 PCT/EP2004/008538 -27- 00 C R 2 is -CH 3 or C 2

H

5 and the bond between atoms 22 and 23 represents a single bond.

Another preferred embodiment of the present invention is the use as defined above, wherein the endecticide is a macrocyclic lactone is selected from the group consisting of avermectins, milbemycins and derivatives thereof, in free form or in the form of a S physiologically acceptable salt.

NO

O Another preferred embodiment of the-present invention is the use as defined above, wherein 00 the macrocyclic lactone is selected from the group consisting of Ivermectin, Doramectin, 0 Moxidectin, Selamectin, Emamectin, Eprinomectin, Milbemectin, Abamectin, Milbemycin oxime, Nemadectin, and a derivative thereof, in free form or in the form of a physiologically acceptable salt.

Another preferred embodiment of the present invention is the use as defined above, comprising an effective amount of a macrocyclic lactone in combination with an effective amount of an anthelmintic selected from the group consisting of Albendazole, Clorsulon, Cydectin, Diethylcarbamazine, Febantel, Fenbendazole, Haloxon, Levamisole, Mebendazole, Morantel, Oxyclozanide, Oxibendazole, Oxfendazole, Oxfendazole, Oxamniquine, Pyrantel, Piperazine, Praziquantel, Thiabendazole, Tetramisole, Trichlorfon, Thiabendazole, and a derivative thereof.

Another preferred embodiment of the present invention is the use as defined above, comprising in addition to an endo-parasiticide or an endecticide an effective amount of an insecticide, acaricide or an insecticide and an acaricide.

.Another.preferred embodiment of the present invention is the use as defined above, comprising an effective amount of milbemycin oxime and praziquantel.

Another preferred embodiment of the present invention is the use as defined above, comprising an effective amount of lufenuron, praziquantel and milbemycin oxime.

Another preferred embodiment of the present invention is the use as defined above, comprising an effective amount of cyclosporin.

P:\OPERAS\20O8\30515S37 div spec AprO8 dC4f31208 00

O

D -28- Another preferred embodiment of the present invention is the use as defined above, O comprising an effective amount of an antimicrobial selected from the group consisting of a penicillin, tetracycline, sulfonamide, cephalosporin, cephamycin, aminoglucosid, Strimethoprim, dimetridazole, erythromycin, framycetin, fruazolidone, pleuromutilin, streptomycin and a compound that is active against protozoa.

00 Another preferred embodiment of the present invention is the use as defined above, comprising an effective amount of compound that is active against behavioral including separation worry or travel sickness of dogs and cats.

An additional preferred embodiment of the present invention is the use of a highly palatable ductile chewable veterinary composition as defined above in a process of controlling nonhuman animal pests or nonhuman animal pathogens or of curing or preventing nonhuman animals diseases.

In one aspect the present invention provides a highly palatable ductile chewable veterinary composition comprising an effective amount of one or more ingredients that are active against animal pests, pathogens or animal diseases; meat flavoring; partially gelatinized starch; a softener; and up to 9% water, whenever produced by process comprising feeding the hopper of an extruder with an effective amount of one or more ingredients that are active against animal pests, pathogens or animal diseases; meat flavoring; partially gelatinized starch; a softener; and up to 9% of water, (ii) constantly cooling down the mixture of active ingredients and carriers so that at no time during the whole extrusion process does the temperature of the extrudate that leaves the tip of the extruder exceed 40°C, (iii) pressing the extrudate through a die that is decisive for the shape of the chewable product, and (iv) cutting the extrudate that leaves the extruder into equal pieces.

Detailed Description of the Invention Even so meat flavoring is actually not the main component of the highly palatable ductile chewable veterinary composition it plays the major role for the present invention. It has surprisingly been recognized that the desired high palatability that is PAOPER1AS\2008X30515637 dv sped AprO8 doc-4J/V208 00 -28Anecessary for achieving reliable and well-reproducible results strictly depends on the amount of meat flavoring in the final composition. The meat flavoring is either a natural product consisting of dried powdered meat derived, for example, from domestic animals and productive livestock, e. g. pigs, horses, cattle, sheep, goats and poultry including chicken, duck, goose and turkey. It further surprisingly turned out that the natural content of fat in said natural meat powder of 20-55% is very 00 important not only for achieving the desired high palatability and excellent taste for the 00 Sanimal but also for achieving the desired softness of the final chewable product. In N1 context with the present invention, a "meat flavoring" shall refer to natural dried and powdered meat as well as to artificial meat flavorings, which are well-know from the food industry. It has however be recognized that artificial meat flavorings are only suitable for the present invention if they already contain 20-55% fat or if this amount of fat is added to the artificial flavoring. Fat that can be added to artificial meat flavorings can be chosen either from animal fats or preferably from plant fats including vegetable oils. However, if vegetable oils are used it is advantageous to use hardened/saturated oils. Unsaturated oils are usually WO 2005/013714 PCT/EP2004/008538 -29- 00 ri liquid at room temperature and result in products that do not show the desired ductility/softness. They are usually too soft. Preferred is the use of saturated/hardened S oils/fats that are generally solid at room temperature and lead to chewable compositions showing the desired ductility.

Fats and oils contain many different fatty acids which affect the body in varying ways. Most simply, they are classified as saturated or unsaturated. Saturated fats sometimes are also N called hardened fats. It is the saturated fat found in many animal products. Saturated fats are generally solid at room-temperature. They are mairily of animal origin but can also be 00 isolated from plants. Typical examples stemming from plants are cocoa butter and coconut 0 and palm oils. These products are often used in store-bought baked goods, non-dairy whipped toppings, cream substitutes, most peanut butter and some margarines. Typical sources of saturated fat are: Animal Fat; Coconut Oil; Meat Fat; Bacon Fat; Cream; Palm Kernel Oil; Beef Fat; Palm Oil; Butter; Ham Fat; Pork Fat; Chicken Fat and Skin; Hardened Fat or Oil; Turkey Fat and Skin; Hydrogenated Vegetable Oil; Cocoa Butter; Lamb Fat; and Coconut.

Natural and artificial meat flavoring is commercially obtainable from various producers.

Natural meat flavoring is, for example, obtainable from: IDF (International Dehydrated Food) INTERNATIONAL DEHYDRATED FOODS, INC.

P.O. Box 10347 Springfield, Missouri 65808, USA 800/641-6509 or 417/881-7820 ADF (American Dehydrated Food), American Dehydrated Foods, Inc., P.O. Box 4087 3801 East Sunshine, Springfield, Missouri 65809 IFF (International Flavour and Fragrance), IFF Global Headquarters, 521 West 57th Street, New York, NY 10019, United States Proliant, Proliant Inc. U.S. Office, 2325 North Loop Drive Ames, IA 50010 USA Some-examples-of-sourees-of-artifieial-mneat-flavoring-a e- Kemin, Worldwide Headquarters 2100 Maury Street, Box 70 Des Moines, Iowa 50301- 0070 USA.

McCormick, 226 Schilling Circle Hunt Valley, MD 21031 Givaudan, Givaudan Flavors Corp.

(Flavours creation, sales production) 1199 Edison Drive Cincinnati, Ohio 45216 Haarman und Reimer 00

O

Within the present invention the expression "soft" is used to characterize a product that is S not as hard and crunchy as, for example, a cornflake and on the other hand is not as ductile as, for example, a marshmallow. The desired ductility/hardness lies somewhere in between.

If measured with a commercially available TEXTURE ANALYSER that is commercially available from Stable Micro Systems(TA-XT2 iHR/25), the texture (softness/hardness) of the chewables lies ideally between 6 12 N.

NO

Hard and crunchy products are especially disadvantageous if one intends to treat older dogs 0 0 and cats because most of these old animals suffer from periodontal disease (Pyorrhea). This disease involves the inflammation and degeneration of tissues that surround and support the teeth. These include the gingiva, alveolar bone, periodontal ligament, and cementum.

Periodontitis or the loss of supporting bone is the latest stage of this progressive disorder and is the major cause of tooth loss in old dogs and cats. Animals suffering from periodontitis avoid eating hard and crunchy products because they cause them pain.

The second important feature of the present invention is the use or partially gelatinized starch. This starch contains 10-20% preferably about 13-17% most preferably 13-17% pre-gelatinized starch. This is important as non-gelatinized and completely pre-gelatinized starch do not result in the desired ductility of the final product.

Starches exhibit thermal stability to about 121 C. Starches are carbohydrates of a general formula (C 6

H

0 0Os)n and are derived from corn, wheat, oats, rice, potatoes, yucca and similar plants and vegetables. They consist of about 27% linear polymer (amylose) and about 73% branched polymer (amylopectin). The two polymers are intertwined within starch granules.

Granules are insoluble in cold water, but soaking in hot water or under steam pressure ruptures-their-covering-and-the-polymers-hydrate-int-a-Gollidal-suspensioR--This-preduGtisa pregelatinized starch and has been used in muds for many years. Thus, pregelatinized starch is water-soluble starch that has undergone irreversible changes by heating in water or steam. Many suitable pregelatinized starches are commercially available. For example, Naster® Instant which is a pregelatinized Pea Starch with a high gel strength. Due to its high amylose level, it has some remarkable properties. It shows an excellent stability to high temperatures, shearing and to variations in pH and is ideal for use in cold processes.

WO 2005/013714 PCT/EP2004/008538 -31 00 A further important component is the softener, which keeps the moisture within the CL composition and allows to store the final product for weeks and months. It does not become hard and does not dry out.

If the mentioned meat flavoring, partially gelatinized starch and the basic component V% containing the active ingredient does not contain moisture one should add water during the NO extrusion process. This has an impact on the flexibility on the chewable veterinary O composition of the present invention. It turned out that it is advantageous to adjust the- 00 moisture content of the product so that the final product contains water at a concentration Sequal to or lower than 9 preferably about 3 to 7 more preferably 4 to 6 For the present invention not only the proportion of meat flavoring and partially pregelatinized starch is extremely important but also the production process as such has an influence on the final product. The highly palatable ductile chewable veterinary composition of the present invention is the outcome of a special extrusion process. As such, extrusion is a very common thermoforming process widely used in the food industry for the production of customary feed pellets. However, in order to achieve the chewables according to the present invention, i.e. a highly palatable ductile product one has to modify the process and secure that the extrudate is not heated during the whole extrusion process because this leads to hard and crunchy products, to losses of active ingredient, and especially to a decrease of the palatability. Actually, production in the desired manner can easily be achieved. The highly palatable ductile chewable veterinary composition of the present invention is conveniently carried out in an injection molding machine or extruder. A mixture comprising an effective amount of one or more ingredients that are active against animal pests, pathogens or animal -disea-sesi-feat-flavering,-partially-gelatinized-star-ehT-a-seftenef-and-up-te-9%-(w)-of-wateris fed through the hopper onto a rotating, reciprocating screw. The material moves along the screw towards the tip. During this process, its temperature is cooled down constantly by means of external coolers around the outside of the barrel and by the shearing action of the screw. The cooling process is controlled so that the temperature of the extrudate during the whole extrusion process does not exceed peak temperature of 40 0 C. Starting in the feeding zone and continuing in the compression zone, the extrudate should not reach temperatures higher than said 40 0 C. It has been found that ideally the product is extruded at or near room temperature, and the extruder is cooled down below room temperature, preferably to 5-10°C.

WO 2005/013714 PCT/EP2004/008538 -32- 00

O

C1 It is then conveyed through the metering zone, where homogenization occurs, to the end of C- the screw. The homogenized material at the tip is then pressed through a form-determining die to obtain shaped articles of the desired size. The simplest way is cutting the extrudate that leaves the extruder into equal pieces of the desired size. 'Desired' means that each piece contains the appropriate amount of active ingredient. Thus, for example, for big dogs S one would produce bigger pieces than for young cats. The amount of active ingredient has to NO be adapted to the bodyweight of the animal that has to be treated.

00 This cooling during the extrusion process is extremely important because extruding this kind 0 of a material without cooling can easily lead to temperatures inside the extruder in the range of 100-200°C. High extrusion temperatures however transform the matrix of the extrudate in an undesirable manner. The reason for this being that the starch is heated above the melting and glass transition temperatures of its components so that they undergo endothermic transitions. As a consequence a melting and disordering of the molecular structure of the starch granules takes place, so that an essentially destructurized starch is obtained. Instead of a ductile and rather soft product one obtains a hard or crunchy product which is not only refused by the animals but does not contain a reproducible amount of active ingredient.

Many active ingredients are not even stable enough at these relatively high temperatures and are at least partially degraded. As a result the biological activity of the product is reduced, and undesired degradation products can be formed that can cause undesired side effects or lead to allergic reactions. Cooling the extruder to temperatures near room temperature, preferably to 5-10 0 C, suppresses all these undesired effects and leads to a perfect product that is not only highly palatable but can surprisingly be stored for months without being degraded.

Thehighly-palatable-duGtile-Ghewable-veterinary-eompositien-f-the-present-invention-mayalso contain a sweetener for further improving the palatability. Any natural sugar can be used including confectioners sugar, maltitol, xylitol, sorbitol, mannitol, lactose, dextrose, saccharose, glucose or fructose, or any mixture thereof. In addition, artificial sweeteners known in the art, including saccharin, aspartame and Acesulfame-K, may also be used. The sweetener is preferably present in an amount of from 1 to 10 preferably between from about 3 to about 7 based on the sweetening power of sucrose. The sweetener serves as a palatability enhancer due to its organoleptic properties. Enhancement of the WO 2005/013714 PCT/EP2004/008538 -33- 00

C

palatability can be especially achieved in those cases where the active ingredient is S extremely bitter or exhibits a taste that is absolutely not accepted by the animal.

SThe veterinary composition of the present invention may also contain an antioxidant even so it turned out that in most of the cases this is not necessary. However, in certain cases the antioxidant serves as a preservative which increases the stability of ingredients that are not N stable if exposed for a longer period of time to oxygen. The term "antioxidant" represents the three groups of antioxidarits, true antioxidants, such as Tenox 2, Tenox PG, Tenox s-1 BHA 00 (2-t-butyl-4-methoxyphenol), and BHT (2,6-di-t-butyl-4-methylphenol), sodium metabisulfite reducing agents and antoxidant synergists, such as tocopherols (alpha, beta, or deltatocopherol, tocopherol esters, alpha-tocopherol acetate), alkyl gallates, butylated hydroxyanisole, butylated hydroxytoluene, citric acid, edetic acid and its salts, lecithin and tartaric acid. Further suitable antioxidants are resveratrol, quercetin, benzoic acid, Trolox (Nacetylcysteine, 6-hydroxy-2,5,7,8-tetramethylchroman-2-carboxylic acid), dimethyl thiourea (DMTU), hesperetin, tetrahydrocurcumin, tetrahydrodemethoxycurcumin, and monothioglycerol. Said antioxidant being added in concentrations ranging from 0 to 3.5 preferably 0.01 to 0.5 Preferred antioxidant are Tenox 2 and BHA (2-t-butyl- 4-methoxyphenol).

Sodium chloride may also be added, up to about 4% to further improve the palatability of the product and to bind moisture. For certain animals sodium chloride serves like a palatability enhancer.

The highly palatable ductile chewable veterinary composition of the present invention further may contain a softener. The softener for use in the invention serves as a humectant which enhanees-the-flexibility-of-the-pet-ehew-and-retains-moisture-e-sthat-the-texture-of-the-petchew is maintained at ambient temperatures. Typically, the softener is present in the highly palatable ductile chewable veterinary composition of the present invention at concentrations from about 10-20 and preferably about 11-15% based upon the weight of the partially gelatinized starch. Suitable softeners include alcohols such as sorbitol, mannitol, hexanol, pentanol and polyols (such as glycerine, propylene glycol, polyethylene glycol, and polypropylene glycol).

WO 2005/013714 PCT/EP2004/008538 -34- 00 C The highly palatable ductile chewable veterinary composition of the present invention may S further contain a coloring agent that lead to a better-looking product. The coloring agent can be selected from the group of azo dyes, organic or inorganic pigments, or coloring agents of natural origin, preferably from oxides of iron of titanium. Said coloring agent being added in concentrations ranging from 0 to 5 preferably 0.05 to 2 A preferred coloring agent is ferric oxide, that is normally used in an amount around 0.1

NO

Technical Equipment 00 The extruder used for the production of the chewables according to the present invention is a co-rotating twin screw extruder type BCTG-62/28D with a screw diameter of 62 mm and a screw length of L/D ratio of 28D with a pelleting device from BOhler AG; Industriestrasse; CH-9240 Uzwil; Switzerland. The feeder (delivering the dry blend into the extruder) is obtainable from K-Tron, Switzerland. It is a loss in weight feeder: type K2-ML-T 35 twin screw feeder equipped with a AC (twin auger) screw. In addition two pumps are use to deliver glycerin and water separately. In addition, two chillers are used to maintain an extruder temperature below Measurement of the softness/hardness of the chewables The texture (softness/hardness) of the chewy is measured by using a TEXTURE ANALYSER type: TA-XT2 iHR/25 that is commercially available from Stable Micro Systems Ltd. (Headquater: Stable Micro Systems Ltd., Vienna Court, Lammas Road; UK). One measures the peak force (in N) necessary to push a sphere with a velocity of 1 mm/sec to penetrate 2mm into the chewable. The sphere has a diameter of 8 mm. The texture of the chewablesis-measured-to-determine-when-the-chewables-are-hard-enoughrto-be-packagedinto bins, before they are packaged into blisters. Texture after 24 hours: Typical values lay between 8 and 20 N.

WO 2005/013714 PCT/EP2004/008538 Examples Example 1: 2-Way-formulation containing Milbemycin oxime and Praziquantel Ingredients Active ingredient No.1 Milbemycin oxime Active ingredient No. 2 Praziquantel Excipients Pre-gelatinized starch Natural chicken flavor Sugar Sodium chloride powder Ferric oxide Total solids Amount Percentage [w/w] 1.975 kg 19.000 kg 205.025 kg 150.000 kg 25.000 kg 7.500 kg 0.500 kg 409.000 kg 20.000 kg 70.000 kg 1.000 kg 91.000 kg 500.000 kg 0.395% 3.800% 41.005% 30.000% 5.000% 1.500% 0.100% 81.800% 4.000 14.000% 0.200% 18.200% 100.000% Water Glycerin Tenox 2 Total liquids Total batch size The 2-Way-formulation containing Milbemycin oxime and Praziquantel is produced as follows: -Pre=blend-Milbemycine-oxime-(l-975-kg)-ard-iron-oxide-(0500 kg)-with-t 3-kg-ofpregelatinized Starch using a V-blender for 5 min.

2. Vacuum transfer through a 10 mesh screen into a bin blender 3. Vacuum transfer praziquantel, confectionery sugar, sodium chloride, chicken flavor and the rest of pregelatinized starch through a 10 mesh screen into a bin blender and blend for 20 min 4. Weigh water into the water tank and weigh glycerin into the glycerin tank and mix with tenox.

Start extruder: WO 2005/013714 PCT/EP2004/008538 00

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0 -36- 6. Cooling unit temperature is set at 7. Dry blend (mixture of step 3) is fed into BCTG extruder through K-tron feeding device.

8. Glycerin/Tenox 2 mixture is pumped into the extruder 9. Water is pumped into the extruder Extruder velocity (rpm) is adjusted according feeding velocity of the dry blend 11. Cutting device of the extruder is adjusted to get the appropriate weights of the chewables 12. After extrusion the chewables are transported via conveyer to a hopping conveyer andfinally 13. Filled into boxes of not more than 3 inches 14. Curing of the chewables for approx. 24 hours at ambient temperature and relative humidity After curing chewables are packaged into blister packages Extruder settings for the different chewy sizes of 0.6 g, 1.5 g, 3.0 g and 6.0 g Weights dry blend glycerin water Extruder cutting feed rate addition addition speed [kg/h] [kg/h] [kg/h] [rpm] 0.6 120 20.52 5.76 85 2200 140 23.94 6.72 100 2000 170 29.07 8.16 120 1250 6 200 34.2 9.6 140 700 Example 2: 3-Way-formulation containing Milbemycin oxime, Praziquantel and Lufenuron Ingredients Active ingredient No. 1 Milbemycin oxime Active ingredient No. 2 Praziquantel Active ingredient No. 3 Lufenuron Excipients Pre-gelatinized starch -Ammont 1.975 kg 19.000 kg 38.340 kg Percent0age [/w 0.395% 3.800% 7.667 159.690 kg 31.938% WO 2005/013714 PCT/EP2004/008538 -37- 00

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o Powdered Cooked Beef Stock Aid Bacon Flavour Sugar Sodium chloride powder Ferric oxide Total solids 142.000 kg 25.000 kg 25.000 kg 7.500 kg 0.500 kg 419.000 kg 20.000 kg 60.000 kg 1.000 kg 81.000 kg 500.000 kg 30.000% 5.000% 5.000% 1.500% 0.100% 83.800% 4.000% 12.000% 0.200% 16.200% 100.000% Water Glycerin Tenox 2 Total liquids Total batch size The 3-Way-formulation containing Milbemycin oxime, Praziquantel and Lufenuron is produced along the same lines as described for the 2-Way-formulation in Example 1.

Example 3: 1-Way-formulation containing Cyclosporin Ingredients Active ingredient Cyclosporin Pre-gelatinized starch Natural chicken flavor Sugar Ferric oxide Total-solids Water Glycerin Total liquids Total batch size Amount 43.40 g 183.60 g 150.00 g 25.0 g 0.50 g -410;00-g 20.00 g 70.00 g 90.00 g 500.00 g Percentage [wlw] 8.7% 36.7% 30.0% 5.0 0.1% -82-0%- 4.0 14.0 18.0% 100.00% The 1-Way-formulation containing Cyclosporn is produced along the same lines as described for the 2-Way-formulation in Example 1.

WO 2005/013714 PCTIEP2004/008538 00 O O 0

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0' -38- Example 4: Palatability (acceptance) test for different flavored chewables of a 3-way formulation with 100 doqs and 100 cats 100 male and female dogs of different breeds and age are tested. The dogs are divided in 4 groups of 25 dogs of the same bodyweight. The testing person offers once a day to each dog one test-chewable which is adapted to the bodyweight of the dog. In a first instance the chewable is offered by hand for 60 seconds. If the dog does not take the formulation it is offered the dog in his empty bowl. The dog has again 60 seconds to take the forniulation, if not, it is paced in his/her mouth. If the dog/cat spits it out it is reported as not accepted. In general not more than 5 to 6 different formulations are tested on consecutive days. Each formulation is packaged separately and labeled so that they can be clearly identified. An analogous test is carried out with 100 cats.

Chewable to be tested Flavor Total acceptance (dogs) 2-Way-formulation containing Natural bacon 96 Milbemycin oxime and Praziquantel 3-Way-formulation containing Natural bacon 93 Milbemycin oxime, Praziquantel and Lufenuron 3-Way-formulation containing Natural beef 94 Milbemycin oxime, Praziquantel and Lufenuron 3-Way-formulation containing Natural chicken Milbemycin oxime, -Praziquantel-and-I.-fentrorrn- 3-Way-formulation containing Artificial bacon 94 Milbemycin oxime, Praziquantel and Lufenuron 3-Way-formulation containing Artificial beef Milbemycin oxime, Praziquantel and Lufenuron The analogues test in cats shows results in absolutely the same range.

PIOPERAS\2OO8UOX JI 07 M SPec ApO1aOC.4If22O08 00 -39- Example 5: Stability tests Samples of the highly palatable ductile chewable veterinary composition of the present invention are tested for stability under stressing conditions in order to stimulate different temperatures and humidity conditions. The samples are tested at 25°C/60 rh, 30°C 60% rh and 40°C 75% rh. They are kept in incubators and are C analysed after 3, 6, 9 and 12 months with regard to active ingredient content. The Sanalyse of the content of active ingredient of all samples tested at 25°C/60 rh and NC 30"C 60% rh for 12 months show no difference in comparison with identical samples kept in the refrigerator at 25"C for the same period of time. Chewables kept 12 months at 40°C/75% rh show also good stability results which indicate that they would lead to a shelf life for at least 12 months if stored under normal conditions, i.e. 25°C pr and 40-70% rh. No significant difference is seen with regard to the stability of 2way-formulations containing Milbemycin oxime and Praziquantel and 3-wayformulation containing Milbemycin oxime, Praziquantel and Lufenuron.

Throughout this specification and the claims which follow, unless the context requires otherwise, the word "comprise", and variations such as "comprises" and "comprising", will be understood to imply the inclusion of a stated integer or step or group of integers or steps but not the exclusion of any other integer or step or group of integers or steps.

The reference in this specification to any prior publication (or information derived from it), or to any matter which is known, is not, and should not be taken as an acknowledgment or admission or any form of suggestion that that prior publication (or information derived from it) or known matter forms part of the common general knowledge in the field of endeavour to which this specification relates.

Claims (22)

1. A highly palatable ductile chewable veterinary composition comprising an In effective amount of one or more ingredients that are active against animal pests, \Opathogens or animal diseases; meat flavoring; partially gelatinized starch; a softener; and up to 9% water, whenever produced by process 00 comprising feeding the hopper of an extruder with an effective amount of one 00 Sor more ingredients that are active against animal pests, pathogens or animal diseases; meat flavoring; partially gelatinized starch; a softener; and up to 9% of water, (ii) constantly cooling down the mixture of active ingredients and carriers so that at no time during the whole extrusion process does the temperature of the extrudate that leaves the tip of the extruder exceed 40'C, (iii) pressing the extrudate through a die that is decisive for the shape of the chewable product, and (iv) cutting the extrudate that leaves the extruder into equal pieces.

2. A highly palatable ductile chewable veterinary composition produced according to claim 1, wherein during the production process the hopper of the extruder is fed continuously and simultaneously with pre-mixture and pre-mixture wherein pre-mixture consists of an homogenized mixture of one or more active ingredients and partially gelatinized starch, and pre-mixture consists of an homogenized mixture of meat flavoring, a softener and optionally of a carrier selected from the group consisting of a sweetener, softener, an antioxidant, a coloring agent and sodium chloride.

3. A highly palatable ductile chewable veterinary composition produced according to claim 1 or claim 2, wherein the extruder is cooled down below room temperature.

4. A chewable veterinary composition produced according to any one of claims 1 to 3, wherein the animal disease comprises viral or bacterial infections, behavioral disorders, inflammatory diseases, and auto-immune diseases. PA\OPEMASVOO2515637 div spec AO8 doc402/O8 00 -41- A chewable veterinary composition produced according to any one of claims 1 to 3, comprising 20 to 30 of a natural meat flavoring.

6. A chewable veterinary composition produced according to any one of claims 1 to wherein the meat flavoring comprises 20 to 55 (wlw) fat. 0 7. A chewable veterinary composition produced according to any one of claims 1 to 00 S3, comprising 25 to 70 of partially gelatinized starch.

8. A chewable veterinary composition produced according to any one of claims 1 to 3, wherein the partially gelatinized starch comprises 12 to 17 of gelatinized starch.

9. A chewable veterinary composition produced according to any one of claims 1 to 3, comprising 10 to 20 of a softener, based upon the weight of the partially gelatinized starch. A chewable veterinary composition produced according to any one of claims 1 to 3, wherein the softener is selected from the group consisting of glycerol, polyethylene glycol and polypropylene glycol.

11. A chewable veterinary composition produced according to any one of claims 1 to 3, comprising 4 to 6 of water.

12. A chewable veterinary composition produced according to any one of claims 1 to 3, wherein the animal pests are external animal parasites or internal animal parasites or both.

13. A chewable veterinary composition produced according to any one of claims 1 to 3, comprising 1 to 10 of a sweetener.

14. A chewable veterinary composition produced according to any one of claims 1 to 3, comprising 0 to 3.5 of an antioxidant. PAOPER\AS2OOM051S837 div spOC Ap,8dOC-.4)2J2(8 00 O 0D -42- A chewable veterinary composition produced according to any one of claims 1 to 3, comprising 0 to 5 of a coloring agent. S16. A chewable veterinary composition produced according to any one of claims 1 to 3, comprising 0 to 4% of sodium chloride. 00 0 17. A chewable veterinary composition produced according to any one of claims 1 to 1 3, comprising a parasiticidally effective amount of an ecto-parasiticide, an endo- parasiticide, an endectocide or of a combination of a parasiticide selected from the group consisting of an ecto-parasiticide, an endo-parasiticide and an endectocide.

18. A chewable veterinary composition according to claim 17 wherein the ecto- parasiticide is active against insects, members of the order Acarina or insects and members of the order Acarina.

19. A chewable veterinary composition according to claim 18 wherein the ecto- parasiticide is an insecticide which s either an insect adulticides or insect growth regulators. A chewable veterinary composition according to claim 17 comprising a parasiticidally effective amount of an endo-parasiticide or endecticide selected from the group consisting of macrocyclic lactones, benzimidazoles, pro- benzimidazoles, imidazothiazoles, tetrahydropyrimidines, organophosphates and piperazines.

21. A chewable veterinary composition according to claim 20 comprising an effective amount of a natural or chemically modified macrocyclic lactone of formula I PAOPERS\S2OO8N3G5i5637 d. 1Sed ApM OC-A/20O8 00 0 -43- CH 3 Y CH, H 22 2R R O OH R, HC 0 X CH 3 O H (N wherein X is Y is -C(H 2 or -C(=N-OCH 3 R 1 is hydrogen or one of radicals H 3 CO H 3 CO H 3 CO R4 0 0- HO 0- 0 0 0 H 3 C H3C H3C or CH-O-CH2-CO-NH CO-O- R 4 is hydroxyl, -NH-CH 3 or -NH-OCH 3 R 2 is hydrogen, -CH 3 -C 2 H 5 -CH(CH 3 )-CH 3 CH(CH 3 )-C 2 H 5 -C(CH 3 )=CH-CH(CH 3 2 or cyclohexyl; and if the bond between atoms 22 and 23 represents a double bond the carbon atom in 23-position is unsubstituted so that Y is or if the bond between atoms 22 and 23 is a single bond the carbon atom in 23-position is unsubstituted or substituted by hydroxy or by the group =N-O-CH 3 so that Y is -C(H 2 or OCH 3 in free form or in the form of a physiologically acceptable salt.

22. A chewable veterinary composition according to claim 21 wherein the macrocyclic lactone is a compound of the formula I wherein X is Y is -C(H 2 R 1 is the radical CH 3 -O-CH-CO-NH- CO-O- P:NOPERkAS\208%3OS1563 drv spc ApV doe.4r=005 00 O -44- R 2 is -CH 3 or C 2 H 5 and the bond between atoms 22 and 23 represents a single bond.

23. A chewable veterinary composition according to claim 20 wherein the Smacrocyclic lactone is selected from the group consisting of avermectins, C milbemycins and derivatives thereof, in free form or in the form of a physiologically acceptable salt. 00 0 24. A chewable veterinary composition according to claim 23 wherein the macrocyclic lactone is selected from the group consisting of Ivermectin, Doramectin, Moxidectin, Selamectin, Emamectin, Eprinomectin, Milbemectin, Abamectin, Milbemycin oxime, Nemadectin, and a derivative thereof, in free form or in the form of a physiologically acceptable salt. A chewable veterinary composition according to claim 20 comprising an effective amount of a macrocyclic lactone in combination with an effective amount of an anthelmintic selected from the group consisting of Albendazole, Clorsulon, Cydectin, Diethylcarbamazine, Febantel, Fenbendazole, Haloxon, Levamisole, Mebendazole, Morantel, Oxyclozanide, Oxibendazole, Oxfendazole, Oxamniquine, Pyrantel, Piperazine, Praziquantel, Thiabendazole, Tetramisole, Trichlorfon, Thiabendazole, and derivatives thereof.

26. A chewable veterinary composition according to claim 20 additionally comprising an effective amount of an insecticide, acaricide or an insecticide and an acaricide.

27. A chewable veterinary composition produced according to any one of claims 1 to 3, comprising an effective amount of milbemycin oxime and praziquantel.

28. A chewable veterinary composition produced according to any one of claims 1 to 3, comprising an effective amount of lufenuron, praziquantel and milbemycin oxime. P IOPERMASOOM830515637 div speo AprOB doC-412D08 00 0

29. A chewable veterinary composition produced according to any one of claims 1 to 3, comprising an effective amount of cyclosporin. A chewable veterinary composition according to claim 1 comprising an effective Samount of an antimicrobial selected from the group consisting of a penicillin, tetracycline, sulfonamide, cephalosporin, cephamycin, aminoglucosid, C N trimethoprim, dimetridazole, erythromycin, framycetin, fruazolidone, 00 Spleuromutilin, streptomycin and a compound that is active against protozoa.

31. A chewable veterinary composition produced according to any one of claims 1 to 3, comprising an effective amount of a compound that is active against behavioral conditions including separation anxiety or travel sickness of dogs and cats.

32. A chewable veterinary composition according to claim 1 substantially as hereinbefore described with reference to any one of the examples.