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CLOSANTEL PLUS

CLOSANTEL PLUS

CLOSANTEL PLUS

closantel-plus
CLOSANTEL AND ABAMECTIN ORAL SUSPENSION
COMPOSITION
Closantel Sodium Dihydrate BP
Eq. To Closantel 5.0% w/v
Abamectin 0.1% w/v
Aqueous Base Q.S.
DRUG DESCRIPTION
For the treatment and control of mature and developing immature gastrointestinal roundworms, lungworms and fluke over 6 weeks in sheep and lambs.

It is ovicidal against nematode eggs and delays egg laying in trematodes (fluke).
PHARMACOLOGY
Mechanism of action of Closantel Sodium The molecular mode of action of salicylanilides, including closantel, is not completely elucidated. They all are uncouplers of the oxidative phosphorylation in the cell mitochondria, which disturbs the production of ATP, the cellular “fuel”. This seems to occur through suppression of the activity of succinate dehydrogenase and fumarate reductase, two enzymes involved in this process. This impairs the parasites motility and probably other processes as well. It seems that closantel also disturbs the liquid and ion transport mechanisms in the parasites membranes. Recently it has been discovered that closantel also inhibits chitinase in Onchocerca volvulus. Chitinase is an enzyme involved in larval molting. Its inhibition interrupts their development to adult worms.
Mechanism of action of Abamectin
As all macrocyclic lactones, abamectin acts as agonist of the GABA (gamma-aminobutyric acid) neurotransmitter in nerve cells and also binds to glutamate-gated chloride channels in nerve and muscle cells of invertebrates. In both cases it blocks the transmission of neuronal signals of the parasites, which are paralyzed and expelled out of the body, or they starve. It also affects the reproduction of some parasites by diminishing oviposition or inducing an abnormal oogenesis.

In mammals the GABA receptors occur only in the central nervous system (CNS), i.e. in the brain and the spinal chord. But mammals have a so-called blood-brain barrier that prevents microscopic objects and large molecules to get into the brain. Consequently macrocyclic lactones are much less toxic to mammals than to parasites without such a barrier, which allows quite high safety margins for use on livestock and pets.
PHARMACOKINETICS
Absorption
After oral administration closantel is readily absorbed into the bloodstream. Four days after treatment up to 60% of the injected and 30% of the drenched closantel is absorbed to blood. In the blood, unchanged closantel binds strongly and almost completely (>99%) to plasma albumins.

After oral administration of Abamectin to sheep, peak plasma levels were observed 12 to 36 hours after treatment.
Distribution
Peak plasma levels are reached 10 to 48 hours after administration, both after oral or intramuscular administration. Half-life in plasma is 3 to 4 weeks.

Due to the strong binding to plasma albumins, closantel residues in the tissues are rather low; the highest ones were found in the lungs and the kidneys. Half-life plasma elimination of Abamectin was 50 to 90 hours.
Biotransformation
Closantel is poorly metabolized. About 80% of the administered dose is excreted through the feces, >98% in the form of the parent molecule.
Elimination
CONTRAINDICATIONS
WARNINGS & PRECAUTIONS
Special precautions for use in animals
Special precautions to be taken by the person administering the veterinary medicinal product to animals
Dosing recommendations for CLOSANTEL PLUS
CATTLE
Delivery Parasites Dose (against closantel, abamectin-susceptible parasites)
Oral Gastrointestinal roundworms 5-10 mg/kg + 0.2 mg/kg
Oral Hypoderma spp 10 mg/kg+ 0.5 mg/kg
SHEEP
Delivery Parasites Dose (against closantel, abamectin-susceptible parasites)
Oral Gastrointestinal roundworms 5-10 mg/kg+ 0.2 mg/kg
Oral Oestrus ovis 5 mg/kg+ 0.2 mg/kg
Oral Fasciola hepatica 10 mg/kg+ 0.5 mg/kg
GOATS
Delivery Parasites Dose (against closantel, abamectin-susceptible parasites)
Oral Gastrointestinal roundworms 10 mg/kg+ 0.5 mg/kg
SOUTHAMERICAN CAMELIDS
Delivery Parasites Dose (against closantel, abamectin-susceptible parasites)
Oral Gastrointestinal roundworms 5 mg/kg+ 0.2 mg/kg
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