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lariam cambodia |
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lariam cambodia Manufacturer: Roche Laboratories DESCRIPTION Mefloquine hydrochloride is a 4-quinolinemethanol derivative with the specificchemical name of (R*, S*)-(±)-(alpha)-2-piperidinyl-2,8-bis (trifluoromethyl)-4-quinolinemethanolhydrochloride lariam cambodia. It is a 2-aryl substituted chemical structural analog of quinine lariam cambodia. The drug is a white to almost white crystalline compound, slightly soluble inwater lariam cambodia. Mefloquine hydrochloride has a calculated molecular weight of 414.78 lariam cambodia. The inactive ingredients are ammonium-calcium alginate, corn starch, crospovidone,lactose, magnesium stearate, microcrystalline cellulose, poloxamer #331, andtalc lariam cambodia. CLINICAL PHARMACOLOGY Distribution Mefloquine crosses the placenta lariam cambodia. Excretion into breast milk appears to be minimal(see PRECAUTIONS : Nursing Mothers ) lariam cambodia. Metabolism Elimination Pharmacokinetics in Special Clinical Situations No relevant age-related changes have been observed in the pharmacokineticsof mefloquine lariam cambodia. Therefore, the dosage for children has been extrapolated fromthe recommended adult dose lariam cambodia. No pharmacokinetic studies have been performed in patients with renal insufficiencysince only a small proportion of the drug is eliminated renally lariam cambodia. Mefloquineand its main metabolite are not appreciably removed by hemodialysis lariam cambodia. No specialchemoprophylactic dosage adjustments are indicated for dialysis patients toachieve concentrations in plasma similar to those in healthy persons lariam cambodia. Although clearance of mefloquine may increase in late pregnancy, in general,pregnancy has no clinically relevant effect on the pharmacokinetics of mefloquine lariam cambodia. The pharmacokinetics of mefloquine may be altered in acute malaria lariam cambodia. Pharmacokinetic differences have been observed between various ethnic populations lariam cambodia. In practice, however, these are of minor importance compared with host immunestatus and sensitivity of the parasite lariam cambodia. During long-term prophylaxis (>2 years), the trough concentrations and theelimination half-life of mefloquine were similar to those obtained in the samepopulation after 6 months of drug use, which is when they reached steady state lariam cambodia. In vitro and in vivo studies showed no hemolysis associated with glucose-6-phosphatedehydrogenase deficiency (see ANIMAL TOXICOLOGY ) lariam cambodia. Microbiology Activity In Vitro and In Vivo Drug Resistance Cross-Resistance
Note: Patients with acute P lariam cambodia. vivax malaria, treated with Lariam, are at highrisk of relapse because Lariam does not eliminate exoerythrocytic (hepatic phase)parasites lariam cambodia. To avoid relapse, after initial treatment of the acute infectionwith Lariam, patients should subsequently be treated with an 8-aminoquinolinederivative (eg, primaquine) lariam cambodia. Prevention of Malaria
Data on the use of halofantrine subsequent to administration of Lariam suggesta significant, potentially fatal prolongation of the QTc interval of the ECG lariam cambodia. Therefore, halofantrine must not be given simultaneously with or subsequentto Lariam lariam cambodia. No data are available on the use of Lariam after halofantrine (seePRECAUTIONS : Drug Interactions ) lariam cambodia. Mefloquine may cause psychiatric symptoms in a number of patients, rangingfrom anxiety, paranoia, and depression to hallucinations and psychotic behavior lariam cambodia. On occasions, these symptoms have been reported to continue long after mefloquinehas been stopped lariam cambodia. Rare cases of suicidal ideation and suicide have been reportedthough no relationship to drug administration has been confirmed lariam cambodia. To minimizethe chances of these adverse events, mefloquine should not be taken for prophylaxisin patients with active depression or with a recent history of depression, generalizedanxiety disorder, psychosis, or schizophrenia or other major psychiatric disorders lariam cambodia. Lariam should be used with caution in patients with a previous history of depression lariam cambodia. During prophylactic use, if psychiatric symptoms such as acute anxiety, depression,restlessness or confusion occur, these may be considered prodromal to a moreserious event lariam cambodia. In these cases, the drug must be discontinued and an alternativemedication should be substituted lariam cambodia. Concomitant administration of Lariam and quinine or quinidine may produce electrocardiographicabnormalities lariam cambodia. Concomitant administration of Lariam and quinine or chloroquine may increasethe risk of convulsions lariam cambodia.
In patients with epilepsy, Lariam may increase the risk of convulsions lariam cambodia. Thedrug should therefore be prescribed only for curative treatment in such patientsand only if there are compelling medical reasons for its use (see PRECAUTIONS: Drug Interactions ) lariam cambodia. Caution should be exercised with regard to activities requiring alertness andfine motor coordination such as driving, piloting aircraft, operating machinery,and deep-sea diving, as dizziness, a loss of balance, or other disorders ofthe central or peripheral nervous system have been reported during and followingthe use of Lariam lariam cambodia. These effects may occur after therapy is discontinued dueto the long half-life of the drug lariam cambodia. Lariam should be used with caution in patientswith psychiatric disturbances because mefloquine use has been associated withemotional disturbances (see ADVERSE REACTIONS ) lariam cambodia. In patients with impaired liver function the elimination of mefloquine maybe prolonged, leading to higher plasma levels lariam cambodia. This drug has been administered for longer than 1 year lariam cambodia. If the drug is to beadministered for a prolonged period, periodic evaluations including liver functiontests should be performed lariam cambodia. Although retinal abnormalities seen in humans withlong-term chloroquine use have not been observed with mefloquine use, long-termfeeding of mefloquine to rats resulted in dose-related ocular lesions (retinaldegeneration, retinal edema and lenticular opacity at 12.5 mg/kg/day and higher)(see ANIMAL TOXICOLOGY ) lariam cambodia. Therefore, periodic ophthalmic examinations are recommended lariam cambodia. Parenteral studies in animals show that mefloquine, a myocardial depressant,possesses 20% of the antifibrillatory action of quinidine and produces 50% ofthe increase in the PR interval reported with quinine lariam cambodia. The effect of mefloquineon the compromised cardiovascular system has not been evaluated lariam cambodia. However, transitoryand clinically silent ECG alterations have been reported during the use of mefloquine lariam cambodia. Alterations included sinus bradycardia, sinus arrhythmia, first degree AV-block,prolongation of the QTc interval and abnormal T waves (see also cardiovasculareffects under PRECAUTIONS : Drug Interactions and ADVERSE REACTIONS ) lariam cambodia. The benefitsof Lariam therapy should be weighed against the possibility of adverse effectsin patients with cardiac disease lariam cambodia. |
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Copyright 2005 D-S LTD. |