Medine.co.uk

Hymatil 300 Mg/Ml Solution For Injection For Cattle And Sheep

Revised: November 2014

AN: 01558/2013


SUMMARY OF PRODUCT CHARACTERISTICS


NAME OF THE VETERINARY MEDICINAL PRODUCT


Hymatil 300 mg/ml solution for injection for cattle and sheep


2. QUALITATIVE AND QUANTITATIVE COMPOSITION


Each ml contains:


Active substance:

Tilmicosin 300 mg


Excipients:

Propylene glycol 250 mg


For the full list of excipients, see section 6.1.


3. PHARMACEUTICAL FORM


Solution for injection.

Clear and yellow solution.


4. CLINICAL PARTICULARS


Target species


Cattle and sheep


4.2. Indications for use, specifying the target species


Cattle:

Treatment of bovine respiratory disease associated with Mannheimia haemolyticaand Pasteurella multocida.

Treatment of interdigital necrobacillosis.


Sheep:

Treatment of respiratory tract infections caused by Mannheimia haemolyticaand Pasteurella multocida.

Treatment of foot rot in sheep caused by Dichelobacter nodosusand Fusobacterium necrophorum.

Treatment of acute ovine mastitis caused by Staphylococcus aureusand Mycoplasma agalactiae.


4.3. Contraindications


Do not administer intravenously.

Do not administer intramuscularly.

Do not administer to lambs weighing less than 15 kg.

Do not administer to primates.

Do not administer to pigs.

Do not administer to horses and donkeys.

Do not administer to goats.

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


Special warnings for each target species


Sheep

The clinical trials did not demonstrate a bacteriological cure in sheep with acute mastitis caused by Staphyloccocus aureusand Mycoplasma agalactiae.

Do not administer to lambs weighing less than 15 kg since there is a risk of overdose toxicity.

Accurate weighing of lambs is important to avoid overdose. The use of a 2 ml or smaller syringe will facilitate accurate dosing.


Special precautions for use


Special precautions for use in animals


Official, national and regional antimicrobial policies should be taken into account when the product is used.

To avoid self-injection do not use automatic injection equipment.

Wherever possible, the use of the product should be based on susceptibility testing.


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

Operator Safety Warnings:


INJECTION OF TILMICOSIN IN HUMANS CAN BE FATAL – EXERCISE EXTREME CAUTION TO AVOID ACCIDENTAL SELF INJECTION AND FOLLOW THE ADMINISTRATION INSTRUCTIONS AND THE GUIDANCE BELOW, PRECISELY

In case of self-injection SEEK IMMEDIATE MEDICAL ATTENTION and take the vial or the package leaflet with you. Apply a cold pack (not ice directly) to the injection site.


Additional operator safety warnings:


NOTE TO THE PHYSICIAN


INJECTION OF TILMICOSIN IN HUMANS HAS BEEN ASSOCIATED WITH FATALITIES.

The cardiovascular system is the target of toxicity, and this toxicity may be due to calcium channel blockade. Administration of intravenous calcium chloride should only be considered if there is positive confirmation of exposure to tilmicosin.

In dog studies, tilmicosin induced a negative inotropic effect with consequent tachycardia, and a reduction in systemic arterial blood pressure and arterial pulse pressure.

DO NOT GIVE ADRENALINOR BETA-ADRENERGIC ANTAGONISTS SUCH AS PROPRANOLOL.

In pigs, tilmicosin-induced lethality is potentiated by adrenalin.

In dogs, treatment with intravenous calcium chloride showed a positive effect on the left ventricular inotropic state and some improvements in vascular blood pressure and tachycardia.

Pre-clinical data and an isolated clinical report suggest that calcium chloride infusion may help to reverse tilmicosin induced changes in blood pressure and heart rate in humans.

Administration ofdobutamine should also be considered due to its positive inotropic effects although it does not influence tachycardia.

As tilmicosin persists in tissues for several days, the cardiovascular system should be closely monitored and supportive treatment provided.

Physicians treating patients exposed to this compound are advised to discuss clinical management with the National Poisons Information Service on: (indicate here the telephone number of the centre).


Adverse reactions (frequency and seriousness)


Occasionally, a soft diffuse swelling may occur at the injection site but this disappears within five to eight days.In rare cases recumbency, incoordination and convulsions have been observed.

Deaths of cattle have been observed following a single intravenous dose of 5 mg/kg body weight, and following the subcutaneous injection of doses of 150 mg/kg body weight at 72 hour intervals. In pigs, intramuscular injection at 20 mg/kg body weight has caused deaths. Sheep have died following a single intravenous injection of 7.5 mg/kg body weight


4.7. Use during pregnancy, lactation or lay


The safety of the veterinary medicinal product has not been established during pregnancy.

Use only according to the benefit/risk assessment by the responsible veterinarian.


4.8. Interaction with other medicinal products and other forms of interaction


Interactions between macrolides and ionophores could be observed in some species.


4.9. Amounts to be administered and administration route


For subcutaneous injection only

Use 10 mg tilmicosin per kg body weight (corresponding to 1 ml Hymatil per 30 kg body weight).


Cattle:

Method of administration:

Withdraw the required dose from the vial and remove the syringe from the needle, leaving the needle in the vial. When a group of animals has to be treated, leave the needle in the vial to remove the subsequent doses. Restrain the animal and insert separate needle subcutaneously at the injection site, preferably in a skinfold over the rib cage behind the shoulder. Attach the syringe to the needle and inject into the base of the skinfold. Do not inject more than 20 ml per injection site.


Sheep:

Method of administration:

Accurate weighing of lambs is important to avoid overdosing. The use of a 2 ml syringe or smaller improves accurate dosing.

Withdraw the required dose from the vial and remove the syringe from the needle, leaving the needle in the vial. Restrain the sheep whilst leaning over the animal and insert a separate needle subcutaneously into the injection site, which should be in a skinfold over the rib cage behind the shoulder. Attach the syringe to the needle and inject into the base of the skin fold. Do not inject more than 2 ml per injection site.

If no improvement is noted within 48 hours, the diagnosis should be confirmed.

Avoid introduction of contamination into vial during use. The vial should be inspected visually for any foreign particulate matter and/or abnormal physical appearance. In the event of either being observed, discard the vial.


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


In cattle, subcutaneous injections of 10, 30 and 50 mg/kg of body weight, repeated three times with a 72 hour intervals did not cause death. As expected, oedema developed at the site of injection. The only lesion observed at autopsy was anecrosis of the myocardium in the group treated with 50 mg/kg body weight.

Doses of 150 mg/kg body weight, administered subcutaneously with an interval of 72 hours caused death. Oedema at the site of injection was observed and at autopsy a light necrosis of the myocardium was the only lesion determined. Other symptoms observed were: difficulty in moving, reduced appetite and tachycardia.

In sheepsingle injections (approximately 30 mg/kg body weight) may cause a slight increase of the rate of respiration. Higher doses (150 mg/kg body weight) caused ataxia, lethargy and the inability to raise the head.

Deaths occurred after one single intravenous injection of 5 mg/kg body weight in cattle and 7.5 mg/kg body weight in sheep.


4.11. Withdrawal period


Cattle:

Meat and offal: 70 days.

Milk: 36 days.

If the product is administered to cows during the dry period or to pregnant dairy heifers (in accordance with section 4.7 above), milk should not be used for human consumption until 36 days after calving.


Sheep:

Meat and offal: 42 days.

Milk: 18 days.

If the product is administered to ewes during the dry period or to pregnant ewes (in accordance with section 4.7 above), milk should not be used for human consumption until 18 days after lambing.


5. PHARMACOLOGICAL PROPERTIES


Pharmacotherapeutic Group: antibacterials for systemic use, macrolides.

ATC Vet code: QJ01FA91.


Pharmacodynamic properties


Tilmicosin is a mainly bactericidal semi-synthetic antibiotic of the macrolide group. It is believed to affect protein synthesis. It has bacteriostatic action but at high concentrations it may be bactericidal. This antibacterial activity is predominantly against Gram-positive microorganism with activity against certain Gram-negative ones and Mycoplasma of a bovine and ovine origin. In particular its activity has been demonstrated against the following micro-organism:


Mannheimia, Pasteurella, Actinomyces (Corynebacterium), Fusobacterium, Dichelobacter, Staphylococcus, and Mycoplasma organisms of bovine and ovine origin.


Minimum inhibition concentration measured in recently (2009-2012) isolated European field strains, derived from respiratory bovine disease.


Bacteria spp

MIC (µg/ml) range

MIC50 (µg/ml)

MIC90 (µg/ml)

P. multocida

0.5- > 64

4

8

M. haemolytica

1 - 64

8

16


The Clinical and Laboratory Standards Institute (CLSI) has set the interpretive criteria for tilmicosin against M. haemolyticaof bovine origin and specifically for bovine respiratory disease, as 8 μg/ml ) = susceptible, 16 μg/ml = intermediate and 32 μg/ml = resistant. The CLSI at the present time have no interpretive criteria for P. multocidaof bovine origin, however they have interpretive criteria for P. multocidaof swine origin, specifically swine respiratory disease, as 16 μg/ml = susceptible and 32 μg/ml = resistant.

Scientific evidence suggests that macrolides act synergistically with the host immune system. Macrolides appear to enhance phagocyte killing of bacteria.

Following oral or parenteral administration of tilmicosin the main target organ for toxicity is the heart. The primary cardiac effects are increased heart rate (tachycardia) and decreased contractility (negative inotrophy). Cardiovascular toxicity may be due to calcium channel blockade.

In dogs, CaCl2treatment showed a positive effect on the left ventricular inotrophic state after tilmicosin administration and some changes in vascular blood pressure and heart rate.

Dobutamine partially offset the negative inotropic effects induced by tilmicosin in dogs. Beta adrenergic antagonists such as propranolol exacerbated the negative inotrophy of tilmicosin in dogs.

In pigs, intramuscular injection of 10 mg tilmicosin/kg body weight caused increased respiration, emesis and convulsions; 20 mg/kg body weight resulted in mortality in 3 of 4 pigs, and 30 mg/kg body weight caused the death of all 4 pigs tested. Intravenous injection of 4.5 to 5.6 mg tilmicosin/kg body weight followed by intravenous injection of 1 ml epinephrine (1/1000) 2 to 6 times resulted in death of all 6 injected pigs. Pigs given 4.5 to 5.6 mg tilmicosin/kg body weight intravenously with no epinephrine all survived. These results suggest that intravenous epinephrine may be contraindicated.

Cross resistance between tilmicosin and other macrolides and lincomycin has been observed.



Pharmacokinetic particulars


Absorption: Several studies have been conducted. The results show that, when administered as recommended to calves and sheep by subcutaneous injection over the dorso-lateral chest, the main parameters are:


Dose Rate

Tmax

Cmax

Cattle:




Neonatal calves

10 mg/kg body weight

1 hour

1.55 μg/ml

Feedlot cattle

10 mg/kg body weight

1 hour

0.97 μg/ml

Sheep




40 kg animals

10 mg/kg body weight

8 hours

0.44 μg/ml

28-50 kg animals

10 mg/kg body weight

8 hours

1.18 μg/ml


Distribution: Following subcutaneous injection, tilmicosin is distributed throughout the body, but especially high levels are found in the lung.


Biotransformation: Several metabolites are formed, the predominant one being identified as T1 (N-demethyl tilmicosin). However the bulk of the tilmicosin is excreted unchanged.


Elimination: Following subcutaneous injection, tilmicosin is excreted mainly via the bile into the faeces, but a small proportion is excreted via the urine. The half-life following subcutaneous injection in cattle is 2-3 days.


6. PHARMACEUTICAL PARTICULARS


6.1. List of excipients


Propylene glycol.

Phosphoric acid, concentrated (for pH adjustment).

Water for injection.


6.2. Incompatibilities


In the absence of compatibility studies, this veterinary medicinal product must not be mixed with other veterinary medicinal products.


6.3. Shelf life


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

Shelf life after first opening the immediate packaging: 28 days.


6.4. Special precautions for storage


Do not store above 30 C.

Keep the vial in the outer carton in order to protect from light.

Do not freeze.

After withdrawal of the first dose, the product should not be stored above 25 ºC.


6.5. Nature and composition of immediate packaging


Clear, amber glass type II vials containing 50 ml, 100 ml and 250 ml of solution in boxes of 1, 6, 10 or 12 vials.

50 ml and 100 ml vials are closed with grey bromobutyl rubber stoppers and aluminium overseals.

250 ml vials are closed with pink bromobutyl rubber stoppers and aluminium overseals.

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


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

Veterinary medicinal product must not be disposed of via waste water or the drainage systems.


7. MARKETING AUTHORIZATION HOLDER


Industrial Veterinaria, S.A.

Esmeralda 19

E-08950 Esplugues de Llobregat

Barcelona

Spain


8. MARKETING AUTHORISATION NUMBER


Vm: 36547/4000


9. DATE OF FIRST AUTHORISATION


Date:14 December 2010


DATE OF REVISION OF THE TEXT


Date:November 2014


PROHIBITION OF SALE, SUPPLY AND/OR USE

To be supplied only on veterinary prescription.

Administration only by a veterinary surgeon.


Approved: 26/11/2014

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