Endogard Plus XL tablets for Dogs

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Printed from NOAH Compendium (https://www.noahcompendium.co.uk). (c) Copyright NOAH Compendium 2024. All Rights Reserved. Date: Monday, April 29, 2024 20:50
Endogard Plus XL tablets for Dogs Virbac Limited Telephone: 01359 243243 Website: www.virbac.co.uk Posted by Administrator 4641 views 0 comments Release 2.53 Endogard Plus XL tablets for Dogs Species: Dogs Therapeutic indication: Pharmaceuticals: Endoparasiticides: Anthelmintics for dogs, Tapeworm products Active ingredient: Febantel, Praziquantel, Pyrantel Embonate Product:Endogard Plus XL Tablets for Dogs Product index: Endogard Plus XL Tablets for Dogs Incorporating: Qualitative and quantitative composition Each tablet contains: Active substances: Praziquantel 175 mg Pyrantel embonate 504 mg Febantel 525 mg Pharmaceutical form Tablets Oval, biconvex tablets with bevelled edges and scored on both sides. Slightly greenish-yellow. The tablets can be divided into equal halves. Clinical particulars Target species Dogs, large and extra large sizes Indications for use For the treatment of mixed infestations with the following roundworms and tapeworms in adult dogs: Nematodes: Ascarids: Toxocara canis, Toxascaris leonina (late immature forms and mature forms) Hookworms: Uncinaria stenocephala, Ancylostoma caninum (adults) Cestodes: Tapeworms: Taenia spp., Dipylidium caninum Contra-indications Do not use simultaneously with piperazine compounds. Do not use in animals with a known hypersensitivity to the active substance or to any of excipients. Do not exceed the stated dosage when treating pregnant bitches. Special warnings for each target species Fleas serve as intermediate hosts for one common type of tapeworm – Dipylidium caninum. Tapeworm infestation is certain to re-occur unless control of intermediate hosts such as fleas, mice etc is undertaken. Special precautions for use Special precautions for use in animals This product is not recommended for use in dogs under 17.5 kg body weight. Any part-used tablets should be discarded. Special precautions to be taken by the person administering the veterinary medicinal product to animals In the interests of good hygiene, persons administering the tablet directly to a dog or by adding it to the dog's food, should wash their hands afterwards. In case of accidental ingestion, seek medical advice and show the package leaflet to the physician. Adverse reactions In very rare cases vomiting, with or without diarrhoea, may occur. Use during pregnancy, lactation or lay Consult a veterinary surgeon before treating pregnant animals for roundworms. The product may be used during lactation. Do not use in bitches during the first two-thirds of pregnancy. Interactions Do not use simultaneously with piperazine as the anthelmintic effects of pyrantel and piperazine (used in many worming products for dogs) may be antagonized. Concurrent use with other cholinergic compounds can lead to toxicity. Amounts to be administered and administration route For oral administration. Dosage The recommended dose rates are: 15 mg/kg bodyweight febantel, 14.4 mg/kg pyrantel and 5 mg/kg praziquantel. This is equivalent to 1 tablet per 35 kg bodyweight. Tablets may be halved to allow accuracy of dosing. Administration and Duration of Treatment No restriction of access to food is required either before or after administration of the product. The tablet(s) can be given directly to the dog or disguised in food. To ensure administration of a correct dose, bodyweight should be determined as accurately as possible. For the control of Toxocara, nursing bitches should be dosed 2 weeks after giving birth and every 2 weeks until weaning. In the event of a heavy roundworm infestation, a repeat dose should be given after 14 days. For routine control adult dogs should be treated every 3 months. Overdose The product is well tolerated in dogs. In safety studies, doses of up to five times the recommended dose gave rise to occasional vomiting. Withdrawal periods Not applicable Pharmacological particulars Pharmacotherapeutic group: Anthelmintics, Benzimidazoles and related substances ATCvet code: QP52AC55 Pharmacodynamic properties The product contains anthelmintics active against roundworms and tapeworms. The product contains three active substances: febantel, pyrantel embonate (pamoate) and praziquantel, a partially hydrogenated pyrazino-isoquinoline derivative used widely as an anthelmintic for both human and veterinary use. Pyrantel acts as a cholinergic agonist. Its mode of action is to stimulate nicotinic cholinergic receptors of the parasite, induce spastic paralysis and thereby allow removal from the gastro-intestinal (GI) system by peristalsis. With the mammalian system febantel undergoes ring closure forming fenbendazole and oxfendazole. It is these chemical entities which exert the anthelmintic effect by inhibition of tubulin polymerization. Formation of microtubules is thereby prevented, resulting in disruption to structures vital to the normal functioning of the helminth. Glucose uptake, in particular, is affected, leading to depletion in cell ATP. The parasite dies upon exhaustion of its energy reserves, which occurs 2 – 3 days later. Praziquantel is very rapidly absorbed and distributed throughout the parasite. Both in vitro and in vivo studies have shown that praziquantel causes severe damage to the parasite integument, resulting in contraction and paralysis. There is an almost instantaneous tetanic contraction of the parasite musculature and a rapid vacuolisation of the syncytial tegument. This rapid contraction has been explained by changes in divalent cation fluxes, especially calcium. In this fixed combination product pyrantel and febantel act synergistically against all relevant nematodes in dogs. In particular, the activity spectrum covers Toxocara canis, Toxascaris leonina, Uncinaria stenocephala and Ancylostoma caninum. The spectrum of activity of praziquntel covers also cestode species in dogs, in particular all Taenia spp. and Dipylidium caninum. Praziquantel acts against adult and immature forms of these parasites. Pharmacokinetic properties Perorally administered praziquantel is absorbed almost completely from the intestinal tract. After absorption, the drug is distributed to all organs. Praziquantel is metabolized into inactive forms in the liver and secreted in bile. It is excreted within 24 hours to more than 95% of the administered dosage. Only traces of non-metabolised praziquantel is excreted. The pamoate salt of pyrantel has low aqueous solubility, an attribute that reduces absorption from the gut and allows the drug to reach and be effective against parasites in the large intestine. Because of the low systemic absorption of pyrantel pamoate, there is very little danger of adverse reactions/toxicity in the host. Following absorption, pyrantel pamoate is quickly and almost completely metabolized into inactive metabolites that are excreted rapidly in the urine. Febantel is absorbed relatively rapidly and metabolized to a number of metabolites including fenbendazole and oxfendazole, which have anthelmintic activity. Pharmaceutical particulars Excipients Lactose monohydrate Maize starch Povidone K-30 Sodium laurilsulfate Microcrystalline cellulose (E460) Colloidal anhydrous silica Magnesium stearate (E572) Major incompatibilities None known Shelf life Shelf-life of the veterinary medicinal product as packaged for sale: 3 years. Special precautions for storage This medicinal product does not require any special storage conditions. Immediate packaging Print and perforated Alu-Alu blister: 2 tablets (1 blister with 2 tablets), in a box. Print and perforated Alu-Alu blister: 4 tablets (2 blisters with 2 tablets), in a box. Print and perforated Alu-Alu blister: 10 tablets (1 blister with 10 tablets), in a box. Print and perforated Alu-Alu blister: 12 tablets (2 blisters with 6 tablets), in a box. Print and perforated Alu-Alu blister: 24 tablets (4 blisters with 6 tablets), in a box. Print and perforated Alu-Alu blister: 30 tablets (3 blisters with 10 tablets or 5 blisters with 6 tablets), in a box. Print and perforated Alu-Alu blister: 50 tablets (5 blisters with 10 tablets), in a box. Print and perforated Alu-Alu blister: 60 tablets (10 blisters with 6 tablets or 6 blisters with 10 tablets), in a box. Print and perforated Alu-Alu blister: 100 tablets (10 blisters with 10 tablets), in a box. Print and perforated Alu-Alu blister: 102 tablets (17 blisters with 6 tablets), in a box. Not all pack sizes may be marketed. Disposal Any unused veterinary medicinal product or waste materials derived from such veterinary medicinal products should be disposed of in accordance with local requirements. Marketing Authorisation Holder (if different from distributor) KRKA, d.d., Novo mesto Šmarješka cesta 6 8501 Novo mesto Slovenia Marketing Authorisation Number Vm 01656/4018 Significant changes Date of the first authorisation or date of renewal June 2011 Date of revision of the text April 2018 Any other information Nil Legal category Legal category: NFA-VPS GTIN

NOAH Compendium

Printed from NOAH Compendium (https://www.noahcompendium.co.uk). (c) Copyright NOAH Compendium 2024. All Rights Reserved.
Date: Monday, April 29, 2024 20:50

Virbac Limited

Telephone: 01359 243243

Website: www.virbac.co.uk

Posted by Administrator

4641 views

0 comments

Release 2.53

Endogard Plus XL tablets for Dogs

Species: Dogs

Therapeutic indication: Pharmaceuticals: Endoparasiticides: Anthelmintics for dogs, Tapeworm products

Active ingredient: Febantel, Praziquantel, Pyrantel Embonate

Product:Endogard Plus XL Tablets for Dogs

Product index: Endogard Plus XL Tablets for Dogs

Incorporating:

Qualitative and quantitative composition

Each tablet contains:

Active substances:

Praziquantel 175 mg

Pyrantel embonate 504 mg

Febantel 525 mg

Pharmaceutical form

Tablets

Oval, biconvex tablets with bevelled edges and scored on both sides. Slightly greenish-yellow.

The tablets can be divided into equal halves.

Clinical particulars

Target species

Dogs, large and extra large sizes

Indications for use

For the treatment of mixed infestations with the following roundworms and tapeworms in adult dogs:

Nematodes:

Ascarids: Toxocara canis, Toxascaris leonina (late immature forms and mature forms)

Hookworms: Uncinaria stenocephala, Ancylostoma caninum (adults)

Cestodes:

Tapeworms: Taenia spp., Dipylidium caninum

Contra-indications

Do not use simultaneously with piperazine compounds.

Do not use in animals with a known hypersensitivity to the active substance or to any of excipients.

Do not exceed the stated dosage when treating pregnant bitches.

Special warnings for each target species

Fleas serve as intermediate hosts for one common type of tapeworm – Dipylidium caninum. Tapeworm infestation is certain to re-occur unless control of intermediate hosts such as fleas, mice etc is undertaken.

Special precautions for use

Special precautions for use in animals

This product is not recommended for use in dogs under 17.5 kg body weight.

Any part-used tablets should be discarded.

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

In the interests of good hygiene, persons administering the tablet directly to a dog or by adding it to the dog's food, should wash their hands afterwards.

In case of accidental ingestion, seek medical advice and show the package leaflet to the physician.

Adverse reactions

In very rare cases vomiting, with or without diarrhoea, may occur.

Use during pregnancy, lactation or lay

Consult a veterinary surgeon before treating pregnant animals for roundworms.

The product may be used during lactation.

Do not use in bitches during the first two-thirds of pregnancy.

Interactions

Do not use simultaneously with piperazine as the anthelmintic effects of pyrantel and piperazine (used in many worming products for dogs) may be antagonized.

Concurrent use with other cholinergic compounds can lead to toxicity.

Amounts to be administered and administration route

For oral administration.

Dosage

The recommended dose rates are: 15 mg/kg bodyweight febantel, 14.4 mg/kg pyrantel and 5 mg/kg praziquantel. This is equivalent to 1 tablet per 35 kg bodyweight.

Tablets may be halved to allow accuracy of dosing.

Administration and Duration of Treatment

No restriction of access to food is required either before or after administration of the product. The tablet(s) can be given directly to the dog or disguised in food.

To ensure administration of a correct dose, bodyweight should be determined as accurately as possible.

For the control of Toxocara, nursing bitches should be dosed 2 weeks after giving birth and every 2 weeks until weaning.

In the event of a heavy roundworm infestation, a repeat dose should be given after 14 days.

For routine control adult dogs should be treated every 3 months.

Overdose

The product is well tolerated in dogs. In safety studies, doses of up to five times the recommended dose gave rise to occasional vomiting.

Withdrawal periods

Not applicable

Pharmacological particulars

Pharmacotherapeutic group: Anthelmintics, Benzimidazoles and related substances

ATCvet code: QP52AC55

Pharmacodynamic properties

The product contains anthelmintics active against roundworms and tapeworms. The product contains three active substances: febantel, pyrantel embonate (pamoate) and praziquantel, a partially hydrogenated pyrazino-isoquinoline derivative used widely as an anthelmintic for both human and veterinary use.

Pyrantel acts as a cholinergic agonist. Its mode of action is to stimulate nicotinic cholinergic receptors of the parasite, induce spastic paralysis and thereby allow removal from the gastro-intestinal (GI) system by peristalsis.

With the mammalian system febantel undergoes ring closure forming fenbendazole and oxfendazole. It is these chemical entities which exert the anthelmintic effect by inhibition of tubulin polymerization. Formation of microtubules is thereby prevented, resulting in disruption to structures vital to the normal functioning of the helminth. Glucose uptake, in particular, is affected, leading to depletion in cell ATP. The parasite dies upon exhaustion of its energy reserves, which occurs 2 – 3 days later.

Praziquantel is very rapidly absorbed and distributed throughout the parasite. Both in vitro and in vivo studies have shown that praziquantel causes severe damage to the parasite integument, resulting in contraction and paralysis. There is an almost instantaneous tetanic contraction of the parasite musculature and a rapid vacuolisation of the syncytial tegument. This rapid contraction has been explained by changes in divalent cation fluxes, especially calcium.

In this fixed combination product pyrantel and febantel act synergistically against all relevant nematodes in dogs. In particular, the activity spectrum covers Toxocara canis, Toxascaris leonina, Uncinaria stenocephala and Ancylostoma caninum. The spectrum of activity of praziquntel covers also cestode species in dogs, in particular all Taenia spp. and Dipylidium caninum. Praziquantel acts against adult and immature forms of these parasites.

Pharmacokinetic properties

Perorally administered praziquantel is absorbed almost completely from the intestinal tract. After absorption, the drug is distributed to all organs. Praziquantel is metabolized into inactive forms in the liver and secreted in bile. It is excreted within 24 hours to more than 95% of the administered dosage. Only traces of non-metabolised praziquantel is excreted.

The pamoate salt of pyrantel has low aqueous solubility, an attribute that reduces absorption from the gut and allows the drug to reach and be effective against parasites in the large intestine. Because of the low systemic absorption of pyrantel pamoate, there is very little danger of adverse reactions/toxicity in the host. Following absorption, pyrantel pamoate is quickly and almost completely metabolized into inactive metabolites that are excreted rapidly in the urine.

Febantel is absorbed relatively rapidly and metabolized to a number of metabolites including fenbendazole and oxfendazole, which have anthelmintic activity.

Pharmaceutical particulars

Excipients

Lactose monohydrate

Maize starch

Povidone K-30

Sodium laurilsulfate

Microcrystalline cellulose (E460)

Colloidal anhydrous silica

Magnesium stearate (E572)

Major incompatibilities

None known

Shelf life

Shelf-life of the veterinary medicinal product as packaged for sale: 3 years.

Special precautions for storage

This medicinal product does not require any special storage conditions.

Immediate packaging

Print and perforated Alu-Alu blister: 2 tablets (1 blister with 2 tablets), in a box.

Print and perforated Alu-Alu blister: 4 tablets (2 blisters with 2 tablets), in a box.

Print and perforated Alu-Alu blister: 10 tablets (1 blister with 10 tablets), in a box.

Print and perforated Alu-Alu blister: 12 tablets (2 blisters with 6 tablets), in a box.

Print and perforated Alu-Alu blister: 24 tablets (4 blisters with 6 tablets), in a box.

Print and perforated Alu-Alu blister: 30 tablets (3 blisters with 10 tablets or 5 blisters with 6 tablets), in a box.

Print and perforated Alu-Alu blister: 50 tablets (5 blisters with 10 tablets), in a box.

Print and perforated Alu-Alu blister: 60 tablets (10 blisters with 6 tablets or 6 blisters with 10 tablets), in a box.

Print and perforated Alu-Alu blister: 100 tablets (10 blisters with 10 tablets), in a box.

Print and perforated Alu-Alu blister: 102 tablets (17 blisters with 6 tablets), in a box.

Not all pack sizes may be marketed.

Disposal

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

Marketing Authorisation Holder (if different from distributor)

KRKA, d.d., Novo mesto

Šmarješka cesta 6

8501 Novo mesto

Slovenia

Marketing Authorisation Number

Vm 01656/4018

Significant changes

Date of the first authorisation or date of renewal

June 2011

Date of revision of the text

April 2018

Any other information

Nil

Legal category

Legal category: NFA-VPS

GTIN