Medine.co.uk

Parafend Lv 9.06% W/V Oral Suspension

Revised: 09 June 2010

AN: 00201/2010


SUMMARY OF PRODUCT CHARACTERISTICS


1. Name of the veterinary medicinal product


Parafend LV 9.06% w/v Oral suspension


2. Qualitative and quantitative composition


Active Substance:


Oxfendazole 9.06 % w/v


Excipients:


Sodium methyl parahydroxybenzoate 0.8 % w/v

Sodium metabisulphite 0.15% w/v


For a full list of excipients, see section 6.1.


3. Pharmaceutical form


Oral suspension

A white to off-white suspension


4. Clinical Particulars


Target species


Cattle

Sheep


4.2 Indications for use, specifying the target species

A broad spectrum anthelmintic for the control of mature and developing immature gastrointestinal roundworms and lungworms and also tapeworms in cattle and sheep. Parafend LV is ovicidal for strongyle eggs.


For the treatment of cattle infested with the following species:


GASTROINTESTINAL ROUNDWORMS:

Ostertagia spp, Haemonchusspp, Nematodirusspp, Trichostrongylusspp, Cooperiaspp, Oesophagostomumspp, Chabertiaspp, Capillaria spp and Trichurisspp.


LUNGWORMS:

Dictyocaulusspp.


TAPEWORMS:

Moniezia spp.


For the treatment of sheep infested with benzimidazole susceptible strains of the following species:


GASTROINTESTINAL ROUNDWORMS:

Ostertagiaspp, Haemonchusspp, Nematodirusspp, Trichostrongylus spp, Cooperiaspp, Oesophagostomumspp and Chabertiaspp. Also provides useful control of Trichurisspp.


LUNGWORMS:

Dictyocaulus spp.


TAPEWORMS:

Monieziaspp.


In cattle it is also effective against inhibited larvae of Cooperiaspp, and usually effective against inhibited/arrested larvae of Ostertagiaspp. In sheep it is effective against inhibited/arrested larvae of Nematodirusspp, and benzimidazole susceptible Haemonchus spp and Ostertagiaspp.


Contraindications


None


4.4 Special Warnings for each target species

Care should be taken to avoid the following practices because they increase the risk of development of resistance and could ultimately result in ineffective therapy:



Suspected clinical cases of resistance to anthelmintics should be further investigated using appropriate tests (e.g. Faecal Egg Count Reduction Test). Where the results of the test (s) strongly suggest resistance to a particular anthelmintic, an anthelmintic belonging to another pharmacological class and having a different mode of action should be used.


Resistance to benzimidazoles has been reported in Teladorsagia, Haemonchus, Cooperia and Trichostongylus species in small ruminants. Therefore the use of this product should be based on local (regional, farm) epidemiological information about susceptability of nematode and recommendations on how to limit further selection for resistance to anthelmintics.



4.5 Special precautions for use


i. Special precautions for use in animals


As with any husbandry procedure, care should be taken when handling the animals especially when inserting the dosing gun nozzle into the animal's mouth. Unnecessary force should not be used as this may cause damage to the mouth and pharyngeal region.


Do not exceed the stated dose.


For oral use only


The bodyweight of animals should be assessed as accurately as possible before calculating the dosage.


Veterinary advice should be sought (a) on appropriate dosing programmes and stock management to achieve adequate parasite control, and to reduce the likelihood of anthelmintic resistance developing; (b) if the product does not achieve the desired clinical effect, as other diseases, nutritional disturbances or anthelmintic resistance may be present.


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


Avoid contact with the skin and eyes. Wash any splashes immediately with cold water.

Wear suitable protective clothing including impermeable rubber gloves.

Wash hands after use.


4.6 Adverse reactions (frequency and seriousness)

None recorded.


4.7 Use during pregnancy, lactation or lay

Safe for use during pregnancy and lactation

4.8 Interaction with other medicinal products and other forms of interaction

None known


Amounts to be administered and administration route


To ensure administration of a correct dose, body weight should be determined as accurately as possible; accuracy of the dosing device should be checked.


Shake the container before use

Do not mix with other products


Cattle: 4.5 mg oxfendazole per kg bodyweight.

Bodyweight

Dose

100 kg (2 cwt)

5 ml

150 kg (3 cwt)

7.5 ml

200 kg (4 cwt)

10 ml

250 kg (5 cwt)

12.5 ml

300 kg (6 cwt)

15 ml

Above 300 kg give a further 2.5 ml for each additional 50 kg bodyweight.


Sheep: 5.0 mg oxfendazole per kg bodyweight.

Bodyweight

Dose

Up to 17 kg (38 lb)

1.0 ml

18 - 25 kg (39 - 55 lb)

1.5 ml

26 - 35 kg (56 - 79 lb)

2.0 ml

36 - 44 kg (80 - 97 lb)

2.5 ml

45 - 60 kg (98 - 132 lb)

3.5 ml

61 - 80 kg (133 - 176 lb)

4.5 ml

Above 80 kg give a further 0.5 ml for each additional 9 kg bodyweight.


For oral administration only. Give the recommended dose by mouth using standard dosing equipment. Dosing may be repeated at required intervals.


Overdose (symptoms, emergency procedures, antidotes), if necessary


Benzimidazoles have a wide safety margin


Withdrawal period


Cattle (Meat): 9 days

Sheep (Meat): 21 days


Not for use in cattle or sheep producing milk for human consumption.


5. pharmacological properties


Pharmacotherapeutic group:Anthelmintic

ATC Vet Code: QP52AC02

Pharmacodynamic properties


Oxfendazole, (methyl [5-phenylsulphinyl-1-H-benzimidazole-2 yl] carbamate), belongs to a class of compounds, the benzimidazoles.


The Benzimidazoles possess anti-mitotic properties, and this action is related to their capacity to bind to tubulin leading to inhibition of formation of microtubules. This, in turn, leads to disruption of cell division. Eventually cell lysis and disintegration occur. Oxfendazole may concentrate preferentially in intestinal cells of parasites to exert its toxic effects initially and principally at this site. Similar effects do not occur in host cells, possibly because of differential binding characteristics. The disruption of parasite metabolic processes, and the effects of oxfendazole on enzymes of helminth parasites, involves inhibition of glucose and sodium uptake, reduced muscle glycogen content, uncoupling of oxidative phosphorylation and inhibition of malate dehydrogenase and fumarate reductase.

A relationship exists between plasma concentrations of active anthelmintic metabolites, the duration of high plasma metabolite concentrations and anthelmintic efficacy.

Oxfendazole is a sulphoxide identical to the sulphoxide metabolite of fenbendazole, both are known to be anthelmintically active and metabolically interconvertible.

Reduction of oxfendazole to fenbendazole occurs in the ruminal fluid while oxidation of fenbendazole to oxfendazole is carried out by hepatic microsomal enzymes in the liver. Much of fenbendazole's anthelmintic activity is attributed to oxfendazole, the latter being much more potent.


6. Pharmaceutical particulars


List of excipients


Sodium methyl Parahydroxybenzoate

Sodium Metabisulphite

Sodium Citrate Dihydrate

Citric Acid Anhydrous

Disodium Edetate

Polysorbate 80

Xanthan gum

Semitcone

Water, Purified


6.2 Incompatibilities


None known


Shelf life


Shelf life of the veterinary medicinal product as packaged for sale: 4 years


Special precautions for storage


Do not store above 25oC.

Protect from frost.

Protect from light.


Nature and composition of immediate packaging


Presented in 0.5 L, 1.0 L, 2.5 L and 5 L white high density polyethylene flexipacks or rigid packs closed with white high density polyethylene screw caps with polyethylene coated plastic washers.

Not all pack sizes may be marketed.


6.6 Special precautions for the disposal of unused veterinary medicinal product or waste materials derived from the use of such products


Do not contaminate ponds, waterways or ditches with the product or used containers.

Any unused product or waste materials should be disposed of in accordance with national requirements.


7. MARKETING AUTHORISATION HOLDER


Norbrook Laboratories Limited

Station Works

Newry

Co. Down, BT35 6JP

Northern Ireland


8. MARKETING AUTHORISATION NUMBER(S)


Vm02000/4121


DATE OF FIRST AUTHORISATION


27thJuly 1994


10. DATE OF REVISION OF THE TEXT


June 2010


Page 6 of 6