increasing its cellular uptake and/or impairing its renal excretion. imidazoles (e.g., ketoconazole, miconazole, clotrimazole, fluconazole, etc.): in vitro and animal studies with the combination of amphotericin b and imidazoles suggest that imidazoles may induce fungal resistance to amphotericin b. combination therapy should be administered with caution, especially in immunocompromised patients. other nephrotoxic medications: agents such as aminoglycosides, cyclosporine, and pentamidine may enhance the potential for drug-induced renal toxicity, and should be used concomitantly only with great caution. intensive monitoring of renal function is recommended in patients requiring any combination of nephrotoxic medications (see precautions: laboratory tests ). skeletal muscle relaxants: amphotericin b-induced hypokalemia may enhance the curariform effect of skeletal muscle relaxants (e.g., tubocurarine). serum potassium levels should be monitored and deficiencies corrected. leukocyte transfusions: acute pulmonary toxicity has been reported in patients receiving intravenous amphotericin b and leukocyte transfusions (see precautions: general ).

ium repletion prior to amphotericin b administration may reduce the risk of developing nephrotoxicity. supplemental alkali medication may decrease renal tubular acidosis complications. since acute pulmonary reactions have been reported in patients given amphotericin b during or shortly after leukocyte transfusions, it is advisable to temporarily separate these infusions as far as possible and to monitor pulmonary function (see precautions: drug interactions ). leukoencephalopathy has been reported following use of amphotericin b. literature reports have suggested that total body irradiation may be a predisposition. whenever medication is interrupted for a period longer than 7 days, therapy should be resumed by starting with the lowest dosage level, e.g., 0.25 mg/kg of body weight, and increased gradually as outlined under dosage and administration .

ture, pulse, respiration, and blood pressure should be recorded every 30 minutes for 2 to 4 hours. in patients with good cardio-renal function and a well tolerated test dose , therapy is usually initiated with a daily dose of 0.25 mg/kg of body weight. however, in those patients having severe and rapidly progressive fungal infection , therapy may be initiated with a daily dose of 0.3 mg/kg of body weight. in patients with impaired cardio-renal function or a severe reaction to the test dose , therapy should be initiated with smaller daily doses (i.e., 5 to 10 mg). depending on the patient's cardio-renal status (see precautions: laboratory tests ), doses may gradually be increased by 5 to 10 mg per day to final daily dosage of 0.5 to 0.7 mg/kg. there are insufficient data presently available to define total dosage requirements and duration of treatment necessary for eradication of specific mycoses. the optimal dose is unknown. total daily dosage may range up to 1.0 mg/kg per day or up to 1.5 mg/kg when given on alternate days. sporotrichosis: therapy with intravenous amphotericin b for sporotrichosis has ranged up to nine months with a total dose up to 2.5 g. aspergillosis: aspergillosis has been treated with amphotericin b intravenously for a period up to 11 months with a total dose up to 3.6 g. rhinocerebral phycomycosis: this fulminating disease generally occurs in association with diabetic ketoacidosis. it is, therefore, imperative that diabetic control be restored in order for treatment with amphotericin b for injection to be successful. in contradistinction, pulmonary phycomycosis, which is more common in association with hematologic malignancies, is often an incidental finding at autopsy. a cumulative dose of at least 3 g of amphotericin b is recommended to treat rhinocerebral phycomycosis. although a total dose of 3 to 4 g will infrequently cause lasting renal impairment, this would seem a reasonable minimum where there is clinical evidence of invasion of deep tissue. since rhinocerebral phycomycosis usually follows a rapidly fatal course, the therapeutic approach must necessarily be more aggressive than that used in more indolent mycoses. preparation of solutions reconstitute as follows: an initial concentrate of 5 mg amphotericin b per ml is first prepared by rapidly expressing 10 ml sterile water for injection usp without a bacteriostatic agent directly into the lyophilized cake, using a sterile needle (minimum diameter: 20 gauge) and syringe. shake the vial immediately until the colloidal solution is clear. the infusion solution, providing 0.1 mg amphotericin b per ml, is then obtained by further dilution (1:50) with 5% dextrose injection usp of ph above 4.2. the ph of each container of dextrose injection should be ascertained before use. commercial dextrose injection usually has a ph above 4.2; however, if it is below 4.2, then 1 or 2 ml of buffer should be added to the dextrose injection before it is used to dilute the concentrated solution of amphotericin b. the recommended buffer has the following composition: dibasic sodium phosphate (anhydrous) 1.59 g monobasic sodium phosphate (anhydrous) 0.96 g water for injection usp qs 100.0 ml the buffer should be sterilized before it is added to the dextrose injection, either by filtration through a bacterial retentive stone, mat, or membrane, or by autoclaving for 30 minutes at 15 lb pressure (121˚c). caution: aseptic technique must be strictly observed in all handling , since no preservative or bacteriostatic agent is present in the antibiotic or in the materials used to prepare it for administration. all entries into the vial or into the diluents must be made with a sterile needle. do not reconstitute with saline solutions. the use of any diluent other than the ones recommended or the presence of a bacteriostatic agent (e.g., benzyl alcohol) in the diluent may cause precipitation of the antibiotic. do not use the initial concentrate or the infusion solution if there is any evidence of precipitation or foreign matter in either one. an in-line membrane filter may be used for intravenous infusion of amphotericin b; however, the mean pore diameter of the filter should not be less than 1.0 micron in order to assure passage of the antibiotic dispersion.

y cause chemical irritation. the adverse reactions most commonly observed are: general (body as a whole): fever (sometimes accompanied by shaking chills usually occurring within 15 to 20 minutes after initiation of treatment); malaise; weight loss. cardiopulmonary: hypotension; tachypnea. gastrointestinal: anorexia; nausea; vomiting; diarrhea; dyspepsia; cramping epigastric pain. hematologic: normochromic, normocytic anemia. local: pain at the injection site with or without phlebitis or thrombophlebitis. musculoskeletal: generalized pain, including muscle and joint pains. neurologic: headache. renal: decreased renal function and renal function abnormalities including: azotemia, hypokalemia, hyposthenuria, renal tubular acidosis; and nephrocalcinosis. these usually improve with interruption of therapy. however, some permanent impairment often occurs, especially in those patients receiving large amounts (over 5 g) of amphotericin b or receiving other nephrotoxic agents. in some patients hydration and sodium repletion prior to amphotericin b administration may reduce the risk of developing nephrotoxicity. supplemental alkali medication may decrease renal tubular acidosis. the following adverse reactions have also been reported: general (body as a whole): flushing. allergic: anaphylactoid and other allergic reactions; bronchospasm; wheezing. cardiopulmonary: cardiac arrest; shock; cardiac failure; pulmonary edema; hypersensitivity pneumonitis; arrhythmias, including ventricular fibrillation; dyspnea; hypertension. dermatologic: rash, in particular maculopapular; pruritus. skin exfoliation, toxic epidermal necrolysis, and stevens-johnson syndrome have been reported during post-marketing surveillance. gastrointestinal: acute liver failure; hepatitis; jaundice; hemorrhagic gastroenteritis; melena. hematologic: agranulocytosis; coagulation defects; thrombocytopenia; leukopenia; eosinophilia; leukocytosis. neurologic: convulsions; hearing loss; tinnitus; transient vertigo; visual impairment; diplopia; peripheral neuropathy; encephalopathy (see precautions ); other neurologic symptoms. renal: acute renal failure; anuria; oliguria. nephrogenic diabetes insipidus has been reported during post-marketing surveillance. altered laboratory findings serum electrolytes: hypomagnesemia; hypo- and hyperkalemia; hypocalcemia. liver function tests: elevations of ast, alt, ggt, bilirubin, and alkaline phosphatase. renal function tests: elevations of bun and serum creatinine.

increasing its cellular uptake and/or impairing its renal excretion. imidazoles (e.g., ketoconazole, miconazole, clotrimazole, fluconazole, etc.): in vitro and animal studies with the combination of amphotericin b and imidazoles suggest that imidazoles may induce fungal resistance to amphotericin b. combination therapy should be administered with caution, especially in immunocompromised patients. other nephrotoxic medications: agents such as aminoglycosides, cyclosporine, and pentamidine may enhance the potential for drug-induced renal toxicity, and should be used concomitantly only with great caution. intensive monitoring of renal function is recommended in patients requiring any combination of nephrotoxic medications (see precautions: laboratory tests ). skeletal muscle relaxants: amphotericin b-induced hypokalemia may enhance the curariform effect of skeletal muscle relaxants (e.g., tubocurarine). serum potassium levels should be monitored and deficiencies corrected. leukocyte transfusions: acute pulmonary toxicity has been reported in patients receiving intravenous amphotericin b and leukocyte transfusions (see precautions: general ).

y fluids and the susceptibility of the fungus. the drug acts by binding to sterols in the cell membrane of susceptible fungi with a resultant change in membrane permeability allowing leakage of intracellular components. mammalian cell membranes also contain sterols and it has been suggested that the damage to human cells and fungal cells may share common mechanisms. an initial intravenous infusion of 1 to 5 mg of amphotericin b per day, gradually increased to 0.4 to 0.6 mg/kg daily, produces peak plasma concentrations ranging from approximately 0.5 to 2 mcg/ml. following a rapid initial fall, plasma concentrations plateau at about 0.5 mcg/ml. an elimination half-life of approximately 15 days follows an initial plasma half-life of about 24 hours. amphotericin b circulating in plasma is highly bound (>90%) to plasma proteins and is poorly dialyzable. approximately two thirds of concurrent plasma concentrations have been detected in fluids from inflamed pleura, peritoneum, synovium, and aqueous humor. concentrations in the cerebrospinal fluid seldom exceed 2.5% of those in the plasma. little amphotericin b penetrates into vitreous humor or normal amniotic fluid. complete details of tissue distribution are not known. amphotericin b is excreted very slowly (over weeks to months) by the kidneys with 2 to 5% of a given dose being excreted in the biologically active form. details of possible metabolic pathways are not known. after treatment is discontinued, the drug can be detected in the urine for at least 7 weeks due to the slow disappearance of the drug. the cumulative urinary output over a 7 day period amounts to approximately 40% of the amount of drug infused.

urrent plasma concentrations have been detected in fluids from inflamed pleura, peritoneum, synovium, and aqueous humor. concentrations in the cerebrospinal fluid seldom exceed 2.5% of those in the plasma. little amphotericin b penetrates into vitreous humor or normal amniotic fluid. complete details of tissue distribution are not known. amphotericin b is excreted very slowly (over weeks to months) by the kidneys with 2 to 5% of a given dose being excreted in the biologically active form. details of possible metabolic pathways are not known. after treatment is discontinued, the drug can be detected in the urine for at least 7 weeks due to the slow disappearance of the drug. the cumulative urinary output over a 7 day period amounts to approximately 40% of the amount of drug infused.

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