ubcutaneous nodules which are infrequently palpable. surgical excision of these nodules (nodulectomy) may be considered in the management of patients with onchocerciasis, since this procedure will eliminate the microfilariae-producing adult parasites.

everity (e.g., somnolence/drowsiness, stupor, and coma), confusion, disorientation and death, has been reported in patients without onchocerciasis or in patients with onchocerciasis in the absence of loa loa infection. these reactions have generally resolved with supportive care and the discontinuation of ivermectin.

nd careful post-treatment follow-up should be implemented.

ents should take tablets on an empty stomach with water. (see clinical pharmacology, pharmacokinetics .) in mass distribution campaigns in international treatment programs, the most commonly used dose interval is 12 months. for the treatment of individual patients, retreatment may be considered at intervals as short as 3 months. table 2: dosage guidelines for stromectol for onchocerciasis body weight (kg) single oral dose number of 3-mg tablets 15-25 1 tablet 26-44 2 tablets 45-64 3 tablets 65-84 4 tablets ≥85 150 mcg/kg

t be expected to occur in strongyloidiasis patients treated with stromectol. (see adverse reactions, onchocerciasis .) laboratory test findings in clinical trials involving 109 patients given either one or two doses of 170 to 200 mcg/kg stromectol, the following laboratory abnormalities were seen regardless of drug relationship: elevation in alt and/or ast (2%), decrease in leukocyte count (3%). leukopenia and anemia were seen in one patient. onchocerciasis in clinical trials involving 963 adult patients treated with 100 to 200 mcg/kg stromectol, worsening of the following mazzotti reactions during the first 4 days post-treatment were reported: arthralgia/synovitis (9.3%), axillary lymph node enlargement and tenderness (11.0% and 4.4%, respectively), cervical lymph node enlargement and tenderness (5.3% and 1.2%, respectively), inguinal lymph node enlargement and tenderness (12.6% and 13.9%, respectively), other lymph node enlargement and tenderness (3.0% and 1.9%, respectively), pruritus (27.5%), skin involvement including edema, papular and pustular or frank urticarial rash (22.7%), and fever (22.6%). (see warnings .) in clinical trials, ophthalmological conditions were examined in 963 adult patients before treatment, at day 3, and months 3 and 6 after treatment with 100 to 200 mcg/kg stromectol. changes observed were primarily deterioration from baseline 3 days post-treatment. most changes either returned to baseline condition or improved over baseline severity at the month 3 and 6 visits. the percentages of patients with worsening of the following conditions at day 3, month 3 and 6, respectively, were: limbitis: 5.5%, 4.8%, and 3.5% and punctate opacity: 1.8%, 1.8%, and 1.4%. the corresponding percentages for patients treated with placebo were: limbitis: 6.2%, 9.9%, and 9.4% and punctate opacity: 2.0%, 6.4%, and 7.2%. (see warnings .) in clinical trials involving 963 adult patients who received 100 to 200 mcg/kg stromectol, the following clinical adverse reactions were reported as possibly, probably, or definitely related to the drug in ≥1% of the patients: facial edema (1.2%), peripheral edema (3.2%), orthostatic hypotension (1.1%), and tachycardia (3.5%). drug-related headache and myalgia occurred in <1% of patients (0.2% and 0.4%, respectively). however, these were the most common adverse experiences reported overall during these trials regardless of causality (22.3% and 19.7%, respectively). a similar safety profile was observed in an open study in pediatric patients ages 6 to 13. the following ophthalmological side effects do occur due to the disease itself but have also been reported after treatment with stromectol: abnormal sensation in the eyes, eyelid edema, anterior uveitis, conjunctivitis, limbitis, keratitis, and chorioretinitis or choroiditis. these have rarely been severe or associated with loss of vision and have generally resolved without corticosteroid treatment. laboratory test findings in controlled clinical trials, the following laboratory adverse experiences were reported as possibly, probably, or definitely related to the drug in ≥1% of the patients: eosinophilia (3%) and hemoglobin increase (1%). post-marketing experience the following adverse reactions have been reported since the drug was registered overseas: onchocerciasis conjunctival hemorrhage all indications hypotension (mainly orthostatic hypotension), worsening of bronchial asthma, toxic epidermal necrolysis, stevens-johnson syndrome, seizures, hepatitis, elevation of liver enzymes, and elevation of bilirubin. neurotoxicity including alteration of consciousness of variable severity (e.g., somnolence/drowsiness, stupor, and coma), confusion, disorientation, and death (see warnings ).

20 mg (333 to 2000 mcg/kg) ivermectin in a fasted state or 30 mg (333 to 600 mcg/kg) ivermectin following a standard high-fat (48.6 g of fat) meal. administration of 30 mg ivermectin following a high-fat meal resulted in an approximate 2.5-fold increase in bioavailability relative to administration of 30 mg ivermectin in the fasted state. in vitro studies using human liver microsomes and recombinant cyp450 enzymes have shown that ivermectin is primarily metabolized by cyp3a4. depending on the in vitro method used, cyp2d6 and cyp2e1 were also shown to be involved in the metabolism of ivermectin but to a significantly lower extent compared to cyp3a4. the findings of in vitro studies using human liver microsomes suggest that clinically relevant concentrations of ivermectin do not significantly inhibit the metabolizing activities of cyp3a4, cyp2d6, cyp2c9, cyp1a2, and cyp2e1. microbiology ivermectin is a member of the avermectin class of broad-spectrum antiparasitic agents which have a unique mode of action. compounds of the class bind selectively and with high affinity to glutamate-gated chloride ion channels which occur in invertebrate nerve and muscle cells. this leads to an increase in the permeability of the cell membrane to chloride ions with hyperpolarization of the nerve or muscle cell, resulting in paralysis and death of the parasite. compounds of this class may also interact with other ligand-gated chloride channels, such as those gated by the neurotransmitter gamma-aminobutyric acid (gaba). the selective activity of compounds of this class is attributable to the facts that some mammals do not have glutamate-gated chloride channels and that the avermectins have a low affinity for mammalian ligand-gated chloride channels. in addition, ivermectin does not readily cross the blood-brain barrier in humans. ivermectin is active against various life-cycle stages of many but not all nematodes. it is active against the tissue microfilariae of onchocerca volvulus but not against the adult form. its activity against strongyloides stercoralis is limited to the intestinal stages. clinical studies strongyloidiasis two controlled clinical studies using albendazole as the comparative agent were carried out in international sites where albendazole is approved for the treatment of strongyloidiasis of the gastrointestinal tract, and three controlled studies were carried out in the u.s. and internationally using thiabendazole as the comparative agent. efficacy, as measured by cure rate, was defined as the absence of larvae in at least two follow-up stool examinations 3 to 4 weeks post-therapy. based on this criterion, efficacy was significantly greater for stromectol (a single dose of 170 to 200 mcg/kg) than for albendazole (200 mg b.i.d. for 3 days). stromectol administered as a single dose of 200 mcg/kg for 1 day was as efficacious as thiabendazole administered at 25 mg/kg b.i.d. for 3 days. summary of cure rates for ivermectin versus comparative agents in the treatment of strongyloidiasis cure rate number and % of evaluable patients (%) ivermectin 170-200 mcg/kg comparative agent albendazole 200 mg b.i.d. for 3 days comparative international study who study 24/26 (92) 126/152 (83) 12/22 (55) 67/149 (45) thiabendazole 25 mg/kg b.i.d. for 3 days comparative international study us studies 9/14 (64) 14/14 (100) 13/15 (87) 16/17 (94) in one study conducted in france, a non-endemic area where there was no possibility of reinfection, several patients were observed to have recrudescence of strongyloides larvae in their stool as long as 106 days following ivermectin therapy. therefore, at least three stool examinations should be conducted over the three months following treatment to ensure eradication. if recrudescence of larvae is observed, retreatment with ivermectin is indicated. concentration techniques (such as using a baermann apparatus) should be employed when performing these stool examinations, as the number of strongyloides larvae per gram of feces may be very low. onchocerciasis the evaluation of stromectol in the treatment of onchocerciasis is based on the results of clinical studies involving 1278 patients. in a double-blind, placebo-controlled study involving adult patients with moderate to severe onchocercal infection, patients who received a single dose of 150 mcg/kg stromectol experienced an 83.2% and 99.5% decrease in skin microfilariae count (geometric mean) 3 days and 3 months after the dose, respectively. a marked reduction of >90% was maintained for up to 12 months after the single dose. as with other microfilaricidal drugs, there was an increase in the microfilariae count in the anterior chamber of the eye at day 3 after treatment in some patients. however, at 3 and 6 months after the dose, a significantly greater percentage of patients treated with stromectol had decreases in microfilariae count in the anterior chamber than patients treated with placebo. in a separate open study involving pediatric patients ages 6 to 13 (n=103; weight range: 17-41 kg), similar decreases in skin microfilariae counts were observed for up to 12 months after dosing.

/kg) ivermectin in a fasted state or 30 mg (333 to 600 mcg/kg) ivermectin following a standard high-fat (48.6 g of fat) meal. administration of 30 mg ivermectin following a high-fat meal resulted in an approximate 2.5-fold increase in bioavailability relative to administration of 30 mg ivermectin in the fasted state. in vitro studies using human liver microsomes and recombinant cyp450 enzymes have shown that ivermectin is primarily metabolized by cyp3a4. depending on the in vitro method used, cyp2d6 and cyp2e1 were also shown to be involved in the metabolism of ivermectin but to a significantly lower extent compared to cyp3a4. the findings of in vitro studies using human liver microsomes suggest that clinically relevant concentrations of ivermectin do not significantly inhibit the metabolizing activities of cyp3a4, cyp2d6, cyp2c9, cyp1a2, and cyp2e1.

mparative agent albendazole 200 mg b.i.d. for 3 days comparative international study who study 24/26 (92) 126/152 (83) 12/22 (55) 67/149 (45) thiabendazole 25 mg/kg b.i.d. for 3 days comparative international study us studies 9/14 (64) 14/14 (100) 13/15 (87) 16/17 (94) in one study conducted in france, a non-endemic area where there was no possibility of reinfection, several patients were observed to have recrudescence of strongyloides larvae in their stool as long as 106 days following ivermectin therapy. therefore, at least three stool examinations should be conducted over the three months following treatment to ensure eradication. if recrudescence of larvae is observed, retreatment with ivermectin is indicated. concentration techniques (such as using a baermann apparatus) should be employed when performing these stool examinations, as the number of strongyloides larvae per gram of feces may be very low. onchocerciasis the evaluation of stromectol in the treatment of onchocerciasis is based on the results of clinical studies involving 1278 patients. in a double-blind, placebo-controlled study involving adult patients with moderate to severe onchocercal infection, patients who received a single dose of 150 mcg/kg stromectol experienced an 83.2% and 99.5% decrease in skin microfilariae count (geometric mean) 3 days and 3 months after the dose, respectively. a marked reduction of >90% was maintained for up to 12 months after the single dose. as with other microfilaricidal drugs, there was an increase in the microfilariae count in the anterior chamber of the eye at day 3 after treatment in some patients. however, at 3 and 6 months after the dose, a significantly greater percentage of patients treated with stromectol had decreases in microfilariae count in the anterior chamber than patients treated with placebo. in a separate open study involving pediatric patients ages 6 to 13 (n=103; weight range: 17-41 kg), similar decreases in skin microfilariae counts were observed for up to 12 months after dosing.