pplementation, antibiotic treatment of c. difficile , and surgical evaluation should be instituted as clinically indicated.

n 1%, regardless of drug relationship: abnormal stools, anorexia, constipation, dry mouth, dysuria, ear disorder, fever, flatulence, flu syndrome, hematuria, infection, insomnia, lymphadenopathy, menstrual disorder, migraine, myalgia, nervousness, paresthesia, pruritus, sgpt increased, skin disorder, somnolence, and vomiting. one patient developed unilateral optic neuritis, an event considered possibly related to fosfomycin tromethamine therapy. post-marketing experience: serious adverse events from the marketing experience with fosfomycin tromethamine outside of the united states have been rarely reported and include: angioedema, aplastic anemia, asthma (exacerbation), cholestatic jaundice, hepatic necrosis, and toxic megacolon. although causality has not been established, during post marketing surveillance, the following events have occurred in patients prescribed fosfomycin tromethamine: anaphylaxis and hearing loss. laboratory changes: significant laboratory changes reported in u.s. clinical trials of fosfomycin tromethamine without regard to drug relationship include: increased eosinophil count, increased or decreased wbc count, increased bilirubin, increased sgpt, increased sgot, increased alkaline phosphatase, decreased hematocrit, decreased hemoglobin, increased and decreased platelet count. the changes were generally transient and were not clinically significant.

rug should be used during pregnancy only if clearly needed.

ing oral administration of fosfomycin tromethamine. fosfomycin is not bound to plasma proteins. fosfomycin is distributed to the kidneys, bladder wall, prostate, and seminal vesicles. following a 50 mg/kg dose of fosfomycin to patients undergoing urological surgery for bladder carcinoma, the mean concentration of fosfomycin in the bladder, taken at a distance from the neoplastic site, was 18.0 mcg per gram of tissue at 3 hours after dosing. fosfomycin has been shown to cross the placental barrier in animals and man. excretion: fosfomycin is excreted unchanged in both urine and feces. following oral administration of fosfomycin tromethamine, the mean total body clearance (cl tb ) and mean renal clearance (cl r ) of fosfomycin were 16.9 (± 3.5) l/hr and 6.3 (± 1.7) l/hr, respectively. approximately 38% of a 3-gram dose of fosfomycin tromethamine is recovered from urine, and 18% is recovered from feces. following intravenous administration, the mean cl tb and mean cl r of fosfomycin were 6.1 (±1.0) l/hr and 5.5 (± 1.2) l/hr, respectively. a mean urine fosfomycin concentration of 706 (± 466) mcg/ml was attained within 2 to 4 hours after a single oral 3-gm dose of fosfomycin tromethamine under fasting conditions. the mean urinary concentration of fosfomycin was 10 mcg/ml in samples collected 72 to 84 hours following a single oral dose of fosfomycin tromethamine. following a 3-gram dose of fosfomycin tromethamine granules administered with a high fat meal, a mean urine fosfomycin concentration of 537 (± 252) mcg/ml was attained within 6 to 8 hours. although the rate of urinary excretion of fosfomycin was reduced under fed conditions, the cumulative amount of fosfomycin excreted in the urine was the same, 1118 (± 201) mg (fed) vs. 1140 mg (± 238) (fasting). further, urinary concentrations equal to or greater than 100 mcg/ml were maintained for the same duration, 26 hours, indicating that fosfomycin tromethamine granules for oral solution can be taken without regard to food. special populations: geriatric: based on limited data regarding 24-hour urinary drug concentrations, no differences in urinary excretion of fosfomycin have been observed in elderly subjects. no dosage adjustment is necessary in the elderly. gender: there are no gender differences in the pharmacokinetics of fosfomycin. renal insufficiency: in 5 anuric patients undergoing hemodialysis, the t 1/2 of fosfomycin during hemodialysis was 40 hours. in patients with varying degrees of renal impairment (creatinine clearances varying from 54 ml/min to 7 ml/min), the t 1/2 of fosfomycin increased from 11 hours to 50 hours. the percent of fosfomycin recovered in urine decreased from 32% to 11% indicating that renal impairment significantly decreases the excretion of fosfomycin. following oral administration of fosfomycin tromethamine, the mean half-life for elimination (t 1/2 ) is 5.7 (± 2.8) hours. microbiology fosfomycin (the active component of fosfomycin tromethamine) has in vitro activity against a broad range of gram-positive and gram-negative aerobic microorganisms which are associated with uncomplicated urinary tract infections. fosfomycin is bactericidal in urine at therapeutic doses. the bactericidal action of fosfomycin is due to its inactivation of the enzyme enolpyruvyl transferase, thereby irreversibly blocking the condensation of uridine diphosphate-n-acetylglucosamine with p-enolpyruvate, one of the first steps in bacterial cell wall synthesis. it also reduces adherence of bacteria to uroepithelial cells. there is generally no cross-resistance between fosfomycin and other classes of antibacterial agents such as beta-lactams and aminoglycosides. fosfomycin has been shown to be active against most strains of the following microorganisms, both in vitro and in clinical infections as described in the indications and usage section: aerobic gram-positive microorganisms enterococcus faecalis aerobic gram-negative microorganisms escherichia coli the following in vitro data are available, but their clinical significance is unknown. fosfomycin exhibits in vitro minimum inhibitory concentrations (mic’s) of 64 mcg/ml or less against most (≥ 90%) strains of the following microorganisms; however, the safety and effectiveness of fosfomycin in treating clinical infections due to these microorganisms has not been established in adequate and well-controlled clinical trials: aerobic gram-positive microorganisms enterococcus faecium aerobic gram-negative microorganisms citrobacter diversus citrobacter freundii enterobacter aerogenes klebsiella oxytoca klebsiella pneuomoniae proteus mirabilis proteus vulgaris serratia marcescens susceptibility testing for specific information regarding susceptibility test interpretive criteria and associated test methods and quality control standards recognized by fda for this drug, please see: https://www.fda.gov/stic.

ifference in microbiologic eradication rates 5 to 11 days post therapy) 5 to 11 days post therapy study day 12 to 21 fosfomycin 1 630/771 (82%) 591/771 (77%) 542/771 (70%) ciprofloxacin 7 219/222 (98%) 219/222 (98%) 213/222 (96%) fosfomycin inferior to ciprofloxacin trimethoprim/ sulfamethoxazole 10 194/197 (98%) 194/197 (98%) 186/197 (94%) fosfomycin inferior to trimethoprim/ sulfamethoxazole nitrofurantoin 7 180/238 (76%) 180/238 (76%) 183/238 (77%) fosfomycin equivalent to nitrofurantoin pathogen fosfomycin 3 gram single dose ciprofloxacin 250 mg bid x 7 days trimethoprim/sulfamethoxazole 160 mg/800 mg bid x 10 days nitrofurantoin 100 mg bid x 7 days e. coli 509/644 (79%) 184/187 (98%) 171/174 (98%) 146/187 (78%) e. faecalis 10/10 (100%) 0/0 4/4 (100%) 1/2 (50%)