Fungiconazol® Tablets for Dogs

NOAH Compendium
Printed from NOAH Compendium (https://www.noahcompendium.co.uk). (c) Copyright NOAH Compendium 2024. All Rights Reserved. Date: Tuesday, May 7, 2024 18:33
Fungiconazol® Tablets for Dogs Dechra Veterinary Products Telephone: 01939 211200 Website: www.dechra.co.uk Email: info.uk@dechra.com Posted by Administrator 7827 views 0 comments Release 2.116 Fungiconazol® Tablets for Dogs Species: Dogs Therapeutic indication: Pharmaceuticals: Antimicrobials: Oral preparations: Tablets, Pharmaceuticals: Antimicrobials: Antifungal products Active ingredient: Ketoconazole Product:Fungiconazol® Tablets for Dogs Product index: Fungiconazol Tablets for Dogs Incorporating: Qualitative and quantitative composition Fungiconazol 200 mg tablets for dogs: Each tablet contains: Active substance: Ketoconazole 200 mg Fungiconazol 400 mg tablets for dogs: Each tablet contains: Active substance: Ketoconazole 400 mg Pharmaceutical form Tablet. Brown spiked, round flavoured tablets, quadrisect. The tablets can be divided into halves and quarters. Clinical particulars Target species Dogs Indications for use Treatment of dermatomycoses due to the following dermatophytes: - Microsporum canis - Microsporum gypseum - Trichophyton mentagrophytes Contraindications Do not administer to animals with liver failure. Do not use in cases of hypersensitivity to the active substance or to any of the excipients. Special warnings for each target species Although rare, repeated use of ketoconazole may induce cross-resistance to other azoles. Special precautions for use in animals Treatment with ketoconazole suppresses testosterone concentrations and increases progesterone concentrations and may affect breeding effectiveness in male dogs during and for some weeks after treatment. Treatment of dermatophytosis should not be limited to treatment of the infected animal(s). It should also include disinfection of the environment, since spores can survive in the environment for long periods of time. Other measures such as frequent vacuuming, disinfection of grooming equipment and removal of all potentially contaminated material that cannot be disinfected will minimize the risk of re-infection or spread of infection. Combination of systemic and topical treatment is recommended. In case of long term treatment administration, liver function should be closely monitored. If clinical signs suggestive of liver dysfunction develop, treatment should be discontinued immediately. As the tablets are flavoured, they should be stored in a safe place out of the reach of animals. Special precautions to be taken by the person administering the veterinary medicinal product to animals Accidental ingestion should be avoided. Keep the blister in the outer carton to prevent access by children. Part (half/quarter) tablets should be stored in the original blister and be used for the next administration. In case of accidental ingestion, seek medical advice immediately and show the package leaflet or the label to the physician. People with known hypersensitivity to ketoconazole should avoid contact with the veterinary medicinal product. Wash hands after use. Other precautions Dermatophytes mentioned in the indication have zoonotic potential with risk of transmission to humans. Maintain good personal hygiene (washing hands after handling the animal, and avoiding direct contact with animal). If signs of skin lesions occur, contact your physician. Adverse reactions In rare cases (more than 1 but less than 10 animals in 10,000 animals treated), neurological symptoms (apathy, ataxia, tremors), hepatic toxicity, vomiting, anorexia and/or diarrhoea may be observed at standard doses. Ketoconazole has transient anti-androgen and anti-glucocorticoid effects; it inhibits the conversion of cholesterol to steroid hormones such as testosterone and cortisol in a dose dependent and time-dependent manner. See also Special precautions for use in animals for effects in male breeding dogs. Use during pregnancy and lactation Studies in laboratory animals have shown evidence of teratogenic and embryotoxic effects. The safety of the product has not been established in pregnant or lactating bitches. Use is not recommended during pregnancy. Interactions Do not administer with antacids and/or H2-receptor antagonists (cimetidine/rantidine) or proton pump inhibitors (e.g. omeprazole) as the absorption of ketoconazole may be modified (absorption requires an acid environment). Ketoconazole is a substrate and potent inhibitor of cytochrome P450 3A4 (CYP3A4). It may decrease the elimination of drugs metabolized by CYP3A4, thereby altering their plasma concentrations. This may result in increased plasma concentrations of e.g. cyclosporine, macrocyclic lactones (ivermectin, selamectin, milbemycin), midazolam, cisapride, calcium-channel blocking agents, fentanyl, digoxin, macrolides, methylprednisolone or coumarine anticoagulants. The increased plasma levels of drugs mentioned above can prolong the duration of effects as well as side effects. On the other hand, inducers of cytochrome P450 may increase the rate of metabolism of ketoconazole, e.g. barbiturates or phenytoin can increase the rate of metabolism of ketoconazole, resulting in a decreased bioavailability, hence a decreased efficacy. Ketoconazole may decrease theophylline serum concentrations. Ketoconazole inhibits the conversion of cholesterol to cortisol and may thus affect trilostane/mitotane dosing in dogs concurrently being treated for hyperadrenocorticism. It is not known to what extent these interactions are relevant for dogs and cats, but in the absence of data, co-administration of the product and these drugs should be avoided. Amounts to be administered and administration route For oral use. Fungiconazol 200 mg tablets for dogs: 10 mg of ketoconazole per kg body weight daily, by oral administration. This corresponds to 1 tablet per 20 kg body weight daily. Fungiconazol 400 mg tablets for dogs: 10 mg of ketoconazole per kg body weight daily, by oral administration. This corresponds to 1 tablet per 40 kg body weight daily. It is recommended to sample the animal once a month during treatment and to stop antifungal administration after two negative cultures. When mycological follow up is not possible, treatment should be continued for an adequate period of time to ensure mycological cure. If lesions persist after 8 weeks of treatment, medication should be re-evaluated by the responsible veterinarian. To be administered preferably together with food, in order to maximise absorption. Tablets can be divided into halves or quarters to ensure accurate dosing. Put the tablet on a flat surface, with its scored side facing up and the convex (rounded) side facing the surface. Halves: With the tip of the thumbs, exert a slight vertical pressure on both sides of the tablet to break it into halves. Quarters: With the tip of a thumb, exert a slight vertical pressure on the middle of the tablet to break it into quarters. Overdose In cases of overdose the following effects may be seen: anorexia, vomiting, pruritus, alopecia and increase of hepatic alanine aminotransferase (ALT) and alkaline phosphatase (ALP). Pharmacological particulars Pharmacotherapeutic group: Systemic antimycotics, imidazole derivatives. ATCvet code: QJ02AB02 Pharmacodynamic properties Ketoconazole is an antifungal agent with a wide spectrum, derived from imidazole-dioxolane, which exerts a fungistatic and sporicidal effect on dermatophytes in dogs. Ketoconazole widely inhibits the cytochrome P450 system. Ketoconazole modifies the permeability of membranes of fungi, and inhibit specifically the synthesis of ergosterole, which is an essential component of the cellular membrane of fungi, principally by inhibiting the enzyme cytochrome P450 14-alpha-demethylase (P45014DM). Ketoconazole has anti-androgen and anti-glucocorticoid effects; it inhibits the conversion of cholesterol to steroid hormones such as testosterone and cortisol. It produces this effect through inhibition of cytochrome P450 enzymes involved in the synthesis. Through inhibition of CYP3A4, metabolism of many drugs is decreased and their in-vivo bioavailability increased. Ketoconazole inhibits p-glycoprotein efflux pumps and may increase the oral absorption and tissue distribution of other medicines, e.g. prednisolone. Pharmacokinetic properties After oral administration, peak plasma levels of 22-49 µg/ml (mean 35 µg/ml) are obtained within 1.5-4.0 hours (mean 2.9 hours). Ketoconazole absorption is enhanced in an acidic environment and drugs that raise gastric pH may lessen absorption. High levels of the drug are found in the liver, adrenals, and pituitary gland, while more moderate levels are found in the kidneys, lungs, bladder, bone marrow, and myocardium. At usual doses (10 mg/kg), drug levels attained are probably inadequate in the brain, testis, and eyes to treat most infections; higher dosages are required. It crosses the placenta (in rats) and is excreted into milk. Ketoconazole is 84-99% bound to the albumin fraction of plasma proteins. Ketoconazole is metabolised by the liver into several inactive metabolites. It is excreted predominantly into bile and to a lesser extent into urine. The terminal elimination half-life ranged between 3 and 9 hours (mean 4.6 hours). Pharmaceutical particulars Shelf life Shelf life of the veterinary medicinal product as packaged for sale: 2 years In-use shelf life subdivided tablets (quarters/halves): 3 days Special precautions for storage This veterinary medicinal product does not require any special storage conditions. Immediate packaging Carton containing 1, 2, 3, 4, 5, 6, 7, 8, 9, 10 Aluminium/PVC/PE/PVDC blisters, containing 10 tablets each. Not all pack sizes may be marketed. Disposal Any unused veterinary medicinal product or waste materials derived from such veterinary medicinal product should be disposed of in accordance with local requirements. Marketing Authorisation Holder (if different from distributor) GB: Dechra Regulatory BV, Handelsweg 25, 5531 AE Bladel, The Netherlands. NI: Le Vet Beheer BV, Wilgenweg 7, 3421 TV Oudewater, The Netherlands. Marketing Authorisation Number GB: Vm 50406/4027: 200 mg NI: Vm 41821/4012: 200 mg GB: Vm 50406/4028: 400 mg NI: Vm 41821/4013: 400 mg Significant changes Date of the first authorisation or date of renewal 200 mg: 4 November 2014 400 mg: 5 November 2014 Date of revision of the text May 2023 Any other information For animal treatment only. To be supplied only on veterinary prescription. Keep out of the sight and reach of children. Legal category Legal category: POM-V GTIN GTIN description:Fungiconazol 200 mg Tablets for Dogs 100 tablets: GTIN:08718469445653 GTIN description:Fungiconazol 400 mg Tablets for Dogs 100 tablets: GTIN:08718469445660

NOAH Compendium

Printed from NOAH Compendium (https://www.noahcompendium.co.uk). (c) Copyright NOAH Compendium 2024. All Rights Reserved.
Date: Tuesday, May 7, 2024 18:33

Dechra Veterinary Products

Telephone: 01939 211200

Website: www.dechra.co.uk

Email: info.uk@dechra.com

Posted by Administrator

7827 views

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Release 2.116

Fungiconazol® Tablets for Dogs

Species: Dogs

Therapeutic indication: Pharmaceuticals: Antimicrobials: Oral preparations: Tablets, Pharmaceuticals: Antimicrobials: Antifungal products

Active ingredient: Ketoconazole

Product:Fungiconazol® Tablets for Dogs

Product index: Fungiconazol Tablets for Dogs

Incorporating:

Qualitative and quantitative composition

Fungiconazol 200 mg tablets for dogs:

Each tablet contains: Active substance: Ketoconazole 200 mg

Fungiconazol 400 mg tablets for dogs:

Each tablet contains: Active substance: Ketoconazole 400 mg

Pharmaceutical form

Tablet. Brown spiked, round flavoured tablets, quadrisect. The tablets can be divided into halves and quarters.

Clinical particulars

Target species

Dogs

Indications for use

Treatment of dermatomycoses due to the following dermatophytes:

- Microsporum canis

- Microsporum gypseum

- Trichophyton mentagrophytes

Contraindications

Do not administer to animals with liver failure.

Do not use in cases of hypersensitivity to the active substance or to any of the excipients.

Special warnings for each target species

Although rare, repeated use of ketoconazole may induce cross-resistance to other azoles.

Special precautions for use in animals

Treatment with ketoconazole suppresses testosterone concentrations and increases progesterone concentrations and may affect breeding effectiveness in male dogs during and for some weeks after treatment.

Treatment of dermatophytosis should not be limited to treatment of the infected animal(s). It should also include disinfection of the environment, since spores can survive in the environment for long periods of time. Other measures such as frequent vacuuming, disinfection of grooming equipment and removal of all potentially contaminated material that cannot be disinfected will minimize the risk of re-infection or spread of infection.

Combination of systemic and topical treatment is recommended.

In case of long term treatment administration, liver function should be closely monitored. If clinical signs suggestive of liver dysfunction develop, treatment should be discontinued immediately. As the tablets are flavoured, they should be stored in a safe place out of the reach of animals.

Special precautions to be taken by the person administering the veterinary medicinal product to animals

Accidental ingestion should be avoided. Keep the blister in the outer carton to prevent access by children. Part (half/quarter) tablets should be stored in the original blister and be used for the next administration. In case of accidental ingestion, seek medical advice immediately and show the package leaflet or the label to the physician.

People with known hypersensitivity to ketoconazole should avoid contact with the veterinary medicinal product. Wash hands after use.

Other precautions

Dermatophytes mentioned in the indication have zoonotic potential with risk of transmission to humans. Maintain good personal hygiene (washing hands after handling the animal, and avoiding direct contact with animal). If signs of skin lesions occur, contact your physician.

Adverse reactions

In rare cases (more than 1 but less than 10 animals in 10,000 animals treated), neurological symptoms (apathy, ataxia, tremors), hepatic toxicity, vomiting, anorexia and/or diarrhoea may be observed at standard doses.

Ketoconazole has transient anti-androgen and anti-glucocorticoid effects; it inhibits the conversion of cholesterol to steroid hormones such as testosterone and cortisol in a dose dependent and time-dependent manner. See also Special precautions for use in animals for effects in male breeding dogs.

Use during pregnancy and lactation

Studies in laboratory animals have shown evidence of teratogenic and embryotoxic effects.

The safety of the product has not been established in pregnant or lactating bitches.

Use is not recommended during pregnancy.

Interactions

Do not administer with antacids and/or H2-receptor antagonists (cimetidine/rantidine) or proton pump inhibitors (e.g. omeprazole) as the absorption of ketoconazole may be modified (absorption requires an acid environment).

Ketoconazole is a substrate and potent inhibitor of cytochrome P450 3A4 (CYP3A4). It may decrease the elimination of drugs metabolized by CYP3A4, thereby altering their plasma concentrations. This may result in increased plasma concentrations of e.g. cyclosporine, macrocyclic lactones (ivermectin, selamectin, milbemycin), midazolam, cisapride, calcium-channel blocking agents, fentanyl, digoxin, macrolides, methylprednisolone or coumarine anticoagulants. The increased plasma levels of drugs mentioned above can prolong the duration of effects as well as side effects.

On the other hand, inducers of cytochrome P450 may increase the rate of metabolism of ketoconazole, e.g. barbiturates or phenytoin can increase the rate of metabolism of ketoconazole, resulting in a decreased bioavailability, hence a decreased efficacy.

Ketoconazole may decrease theophylline serum concentrations.

Ketoconazole inhibits the conversion of cholesterol to cortisol and may thus affect trilostane/mitotane dosing in dogs concurrently being treated for hyperadrenocorticism.

It is not known to what extent these interactions are relevant for dogs and cats, but in the absence of data, co-administration of the product and these drugs should be avoided.

Amounts to be administered and administration route

For oral use.

Fungiconazol 200 mg tablets for dogs: 10 mg of ketoconazole per kg body weight daily, by oral administration. This corresponds to 1 tablet per 20 kg body weight daily.

Fungiconazol 400 mg tablets for dogs: 10 mg of ketoconazole per kg body weight daily, by oral administration. This corresponds to 1 tablet per 40 kg body weight daily.

It is recommended to sample the animal once a month during treatment and to stop antifungal administration after two negative cultures. When mycological follow up is not possible, treatment should be continued for an adequate period of time to ensure mycological cure. If lesions persist after 8 weeks of treatment, medication should be re-evaluated by the responsible veterinarian.

To be administered preferably together with food, in order to maximise absorption.

Tablets can be divided into halves or quarters to ensure accurate dosing. Put the tablet on a flat surface, with its scored side facing up and the convex (rounded) side facing the surface.

Halves: With the tip of the thumbs, exert a slight vertical pressure on both sides of the tablet to break it into halves.

Quarters: With the tip of a thumb, exert a slight vertical pressure on the middle of the tablet to break it into quarters.

Overdose

In cases of overdose the following effects may be seen: anorexia, vomiting, pruritus, alopecia and increase of hepatic alanine aminotransferase (ALT) and alkaline phosphatase (ALP).

Pharmacological particulars

Pharmacotherapeutic group: Systemic antimycotics, imidazole derivatives.

ATCvet code: QJ02AB02

Pharmacodynamic properties

Ketoconazole is an antifungal agent with a wide spectrum, derived from imidazole-dioxolane, which exerts a fungistatic and sporicidal effect on dermatophytes in dogs.

Ketoconazole widely inhibits the cytochrome P450 system. Ketoconazole modifies the permeability of membranes of fungi, and inhibit specifically the synthesis of ergosterole, which is an essential component of the cellular membrane of fungi, principally by inhibiting the enzyme cytochrome P450 14-alpha-demethylase (P45014DM).

Ketoconazole has anti-androgen and anti-glucocorticoid effects; it inhibits the conversion of cholesterol to steroid hormones such as testosterone and cortisol. It produces this effect through inhibition of cytochrome P450 enzymes involved in the synthesis.

Through inhibition of CYP3A4, metabolism of many drugs is decreased and their in-vivo bioavailability increased.

Ketoconazole inhibits p-glycoprotein efflux pumps and may increase the oral absorption and tissue distribution of other medicines, e.g. prednisolone.

Pharmacokinetic properties

After oral administration, peak plasma levels of 22-49 µg/ml (mean 35 µg/ml) are obtained within 1.5-4.0 hours (mean 2.9 hours).

Ketoconazole absorption is enhanced in an acidic environment and drugs that raise gastric pH may lessen absorption. High levels of the drug are found in the liver, adrenals, and pituitary gland, while more moderate levels are found in the kidneys, lungs, bladder, bone marrow, and myocardium. At usual doses (10 mg/kg), drug levels attained are probably inadequate in the brain, testis, and eyes to treat most infections; higher dosages are required. It crosses the placenta (in rats) and is excreted into milk.

Ketoconazole is 84-99% bound to the albumin fraction of plasma proteins. Ketoconazole is metabolised by the liver into several inactive metabolites. It is excreted predominantly into bile and to a lesser extent into urine. The terminal elimination half-life ranged between 3 and 9 hours (mean 4.6 hours).

Pharmaceutical particulars

Shelf life

Shelf life of the veterinary medicinal product as packaged for sale: 2 years

In-use shelf life subdivided tablets (quarters/halves): 3 days

Special precautions for storage

This veterinary medicinal product does not require any special storage conditions.

Immediate packaging

Carton containing 1, 2, 3, 4, 5, 6, 7, 8, 9, 10 Aluminium/PVC/PE/PVDC blisters, containing 10 tablets each.

Not all pack sizes may be marketed.

Disposal

Any unused veterinary medicinal product or waste materials derived from such veterinary medicinal product should be disposed of in accordance with local requirements.

Marketing Authorisation Holder (if different from distributor)

GB: Dechra Regulatory BV, Handelsweg 25, 5531 AE Bladel, The Netherlands.

NI: Le Vet Beheer BV, Wilgenweg 7, 3421 TV Oudewater, The Netherlands.

Marketing Authorisation Number

GB: Vm 50406/4027: 200 mg

NI: Vm 41821/4012: 200 mg

GB: Vm 50406/4028: 400 mg

NI: Vm 41821/4013: 400 mg

Significant changes

Date of the first authorisation or date of renewal

200 mg: 4 November 2014

400 mg: 5 November 2014

Date of revision of the text

May 2023

Any other information

For animal treatment only. To be supplied only on veterinary prescription. Keep out of the sight and reach of children.

Legal category

Legal category: POM-V

GTIN

GTIN description:Fungiconazol 200 mg Tablets for Dogs 100 tablets:

GTIN:08718469445653

GTIN description:Fungiconazol 400 mg Tablets for Dogs 100 tablets:

GTIN:08718469445660