Serum and dialysate levels of amikacin were determined at appropriate intervals after a 300-mg intravenous dose as a continuous infusion in six patients with end-stage renal failure undergoing hemodialysis and in three patients on peritoneal dialysis. The mean serum half-life of amikacin was 3.75 h during (or after) hemodialysis and 29 h during (or after) peritoneal dialysis. Although not on hemodialysis in the same six patients, the serum half-life was 28 h. The results indicate that the maintenance dose of amikacin should be markedly decreased in patients with severe renal failure even ifthey are treated with peritoneal dialysis, and that serial serum antibiotic concentrations are essential to prevent cumulative toxicity of the drug.Amikacin is a new aminoglycoside antibiotic with an antibacterial spectrum comparable to gentamicin and tobramycin (3, 4). Since aminoglycosides are excreted mainly through the kidney and not metabolized in the body, their toxic effects are increased in renal failure. However, these antibiotics may be the only available agents to treat life-threatening infections. It, therefore, is important to know how renal failure and renal dialysis effect the pharmacology of amikacin. We accordingly determined the serum concentration, half-life, and dialysate concentration of amikacin in patients with renal failure who were being dialyzed, and the results are the subject of this report.MATERIALS AND METHODS Patient selection. Studies were performed in six patients undergoing a 4-h hemodialysis using two Cordis-Dow model no. 4 hollow fiber kidneys. Blood flow during dialysis was approximately 200 ml/min, and dialysate flow was 500 ml/min. Three patients who were being treated with peritoneal dialysis using Impersol solution run at 2 liters/h for 48 h were studied. The patients had stable creatinine clearance values below 10 mg/min.Patients with congestive heart failure, concurrent hepatic disease, and acute blood loss were excluded from this study. The age, sex, body weight, serum creatinine, total protein, and serum albumin levels in six patients with end-stage renal disease on hemodialysis are summarized in Table 1. All patients were evaluated before and 1 week after amikacin administration for adverse effects, and no changes were found in the histories and physical examinations, blood count, urinalysis, bilirubin, serum glutamic oxalacetic transaminase, alkaline phosphatase, serum protein, serum albumin, creatinine, blood urea nitrogen, and serum electrolytes.Collection of specimens. Patients on hemodialysis. A single dose of 300 mg of amikacin was administered intravenously (i.v.) over a period of 60 min starting 75 min before the onset of dialysis. Blood samples were drawn at the beginning of dialysis and thereafter at 5, 30, 90, 210, and 270 min and 12 and 24 h. The dialysate was collected and pooled. Volumes were measured, and a 20-ml sample was taken for antibiotic assay and then frozen immediately. The same dose of amikacin was given 10 to 14 days later to the same six patients on a day...
