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Anthelmintic Drugs
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Helmintic infections
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Human is the primary host for most helminthic infections. Most worms produce eggs and larva These pass out of human body and infect secondary host Immature forms invade humans via skin or GIT
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Types of worms Worms live in host, s alimentary canal Worms or larvae live in muscles, viscera, menninges, lungs. Subcutaneous tissues
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Intestinal Worms A) Round worms ( Nematodes ) Ascaris lmubricods ( common ) Enterobius vermicularis ( pin worm) Trichris trichuria ( whip worm) Strongyloids stercoralis ( thread Ankylostoma dudenale ( hook worm
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B) Tape worms ( cestodes ) Taenia saginata ( Beef) Taenia solium ( pork) Humans become infected by eating raw or unde cooked meat containing larvae of infected cattle or pig
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Continue ( cestodes ) In some cases the larva gets encysted in muscles, viscera, brain, eye resulting in cysticercosis
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Tissue worms Filariae ( bancrofti, loa loa ) Adult filariae live in the lymphatics, causing lymphadenitis, swelling of limb. Microfilariae goes to blood stream to be ingested by mosquitoes Trichnella spiralis : larva migrats from intestine to tissues of leg or foot producing ulcer
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Anthelminthic Drugs May act by causing : paralysis of the worm. damaging the worm leading to partial digestion or rejection by immune mechanisms. interfere with the metabolism of the worm.
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Ascaris lumbricoids ( common round worm)
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filariasis
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Hookworm
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Pinworm male,female
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Tapeworm
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whipworm
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Dircrocoelium dendriticum
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Fasiola hepatica
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Tricuris tricura
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Trichinela spiralis
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elephantiasis
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Hydateid cyct
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cysticercosis
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ANTHELMINTIC DRUGS ALBENDAZOLE Broad spectrum Drug of choice for treatment of hydatid disease and cysticercosis. Used for the treatment of ( intestinal nematodes ) e.g. ascariasis, tricurasis and strongyloidiasis, pinworm, hookworm
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Mechanism Of Action Inhibits microtubule synthesis that irreversibly impairs glucose uptake, intestinal parasites are immobilized and die slowly. larvicidal in : hydatid,cysticercosis, ascariasis and hook worm infections. Ovicidal in ascariasis,hookworm, trichuriasis
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Pharmacokinetics Benzimidazole carbamate Administered orally, absorption increased with a fatty meal Metabolized in the liver to the active metabolite albendazole sulfoxide
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Pharmacokinetics Plasma half life 8-12 hours sulfoxide is mostly protein bound distributes well to tissues and enters bile, CSF & hydatid cysts. Metabolites are excreted in urine
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Clinical uses Used on empty stomach when used against intraluminal parasites but with a fatty meal when used against tissue parasites. In ascariasis,trichuriasis,hookworm, pin worm infections : children over 2 years & adults (single dose 400mg, repeated for 2-3 day in heavy ascaris infection. For 2 wks for pin worm infection 2. Hydatid diseases
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Albendazole (con’) 3.Neurocysticercosis: Used with corticosteroid to decrease the inflammation caused by dying organism and it also reduces the duration of course for 21 days 4. Other infections: Drug of choice in cutaneous and visceral larva migrans, intestinal capillariasis & others
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Adverse Effects In short term(1-3 days): No significant adverse effects In long term use : abdominal pain, headache,fever,fatigue, alopecia, increased liver enzymes, pancytopenia. Not given during pregnancy, hypersensitive peoples & children under 2 years.
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MEBENDAZOLE (Vermox) Synthetic benzimidazole Wide spectrum and safer than albendazole Mechanism of action: As albendazole It kills hookworm, pin worm, ascariasis and trichuris eggs.
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Pharmacokinetics less than 10% of orally administered drug is absorbed Absorption increases with fatty meal. Absorbed drug is 90 % protein bound Converted to inactive metabolites. Half- life of 2-6 hours Excreted in urine.
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Clinical Uses Tablets should be chewed before swallowing. Pinworm, trichuriasis, hookworm & ascaris infections. in adults and children over 2 years cure rate is 90-100 % except hookworm it is less.
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Adverse Effects & Precautions Short term therapy.Mild GI disturbance. High dose : hypersensitivity reactions, agranulocytosis, alopecia,elevation of liver enzymes. Used with caution under 2ys of age may cause convulsion. Contraindicated in pregnancy..
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Thiabendazole Mechanism as other benzimidazole Chelating agent and form stable complexes with metals including iron, but does not bind with calcium. Rapidly absorbed Half- life of 1-2 hrs Completely metabolized in liver and 90% is excreted in urine Can also absorbed through skin
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Clinical uses Should be given after meals.and tablets should be chewed Strongyloidal infections In cutaneous larva migrans.Thiabendazole cream is applied topically or drug can be given orally for 2 days.
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Adverse Effects & Contraindications More toxic than other benzamidazoles GI disturbances Pruritus,headache, drowsiness, psychoneurotic symptoms. Irreversible liver failure. Fatal Stevens –Johnson syndrome Not used in young children, pregnancy, hepatic and renal diseases.
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PYRANTEL PAMOATE Broad spectrum Pharmacokinetics : Poorly absorbed orally Half of the drug is excreted unchanged in the feces. Mechanism of action : Neuromuscular blocking drug leads to paralizes of worms Effective against luminal organisms( mature or immature forms). Not effective against migratory stages in the tissues or against ova
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Clinical uses Pin worm given orally with or without food. Ascariasis Hookworm
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Adverse Effects Infrequent mild GI disturbance drowsiness, headache,insomnia. Rash,fever Contraindications Pregnancy Children under 2 years of age
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PIPERAZINE Only recommended for the treatment of ascariasis cure rate 90% for 2 days treatment. Readily absorbed orally and excreted mostly unchanged in urine Mechanism of action: Causes paralysis of ascaris by blocking acetylcholine at myoneural junction, the live worms expelled by normal peristalsis.
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Treatment is continued for 3-4 days or repeated after one week in case of heavy infections.
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Adverse Effects GI disturbance Neurotoxicity, allergic reactions. Contraindications Epilepsy Impaired liver or kidney functions pregnancy
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NICLOSAMIDE Second-line drug for treatment of tape worm infections. Mechanism of action: Adult worm is rapidly killed by inhibition of oxidative phosphorylation. Pharmacokinetics: Poorly absorbed from gut & excreted in urine.
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Clinical Uses Treatment of most forms of tapeworms. Not effective against cysticercosis or hydatic disease. Given in the morning on empty stomach. Purgative is necessary to purge all dead segments& prevent liberation of ova.
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Adverse effects Mild,infrequent and transitory GI disturbance Alcohol consumption should be avoided Not indicated in children under 2 years of age or in pregnancy.
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DIETHYL CARBAMAZINE Drug of choice for the treatment of filariasis and tropical eosinophilia. Pharmacokinetics: Rapidly absorbed from gut Half- life is 2-3 hours The drug should be given after meals It is excreted in urine as unchanged or metabolite. Dosage is reduced in urinary alkalosis and renal impairment.
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Mechanism Of Action Immobilizes microfilariae and alters their surface structure,displacing them from tissues & making them susceptible to destruction by host defense mechanism
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Adverse Effects Fever, malaise, papular rash, headache, GI disturbance,cough. Chest,muscle,joint pain Leucocytosis Retinal hemorrhage Encephalopathy lymphangitis and lymphadenopathy. *It is not teratogenic
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Contraindications & Cautions * Hypertension * Renal disease *patient with lymphangitis Patients suspected of malaria
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IVERMECTIN Drug of choice for treatment of filaria & strongyloidiasis It is a macrocyclic lactone ring Given only orally Rapidly absorbed Does not cross BBB. Half- life is 16 hrs Excretion in urine & feces.
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Mechanism Of Action Paralyze nematodes by intensifying GABA- mediated transmission of signals in peripheral nerves.
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Clinical uses Drug of choice for cutaneous larva migrans & strongyloidiasis. Onchocerciasis It is also used for scabies, lice. Filariasis ( it is microfilaricidal ).
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Adverse Effects Fatigue,dizziness, GI disturbance Killing of microfilaria result in a Mazotti reaction ( fever, headache, dizziness, somnolence, hypotension, tachycardia, peripheral edema……). Corneal opacities & other eye lesions.
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Contraindications & Cautions Concomitant use with other drugs that enhance GABA e.g Barbiturates, bnzodiazepines, valproic acid. pregnancy Meningitis Children under 5 years of age.
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BITHIONOL Drug of choice for the treatment of fascioliasis ( sheep liver fluke) Pharmacokinetics: It is orally administered and excreted in urine.
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Adverse Effects GI disturbance Dizziness, headache Skin rashes, urticaria, Leucopenia Contraindications and precautions: Hepatitis, leucopenia Used with caution in children under 8 years of age.
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