Pharmacokinetics of colistin methanesulfonate and colistin in a critically ill patient receiving continuous venovenous hemodiafiltration.

Intravenous colistin methanesulfonate (CMS) is increasingly the last line of defense for multidrug-resistant gram-negative bacteria and is now being used as “salvage” therapy in critically ill patients (1, 7, 9, 11). CMS is converted in vivo to colistin, and these two entities have substantially different pharmacokinetics, antibacterial activities, and toxicities (7), and therefore it is important to understand the dispositions of both. Patients who are currently being treated with CMS include many in the intensive care setting with multiple organ dysfunctions and receiving renal replacement therapy (10). Goodwin et al. reported the effects of renal impairment, peritoneal dialysis, and hemodialysis on the concentrations of CMS in serum (3); unfortunately, the microbiological assays employed failed to measure colistin and CMS separately. Moreover, the efficiency of the hemodialyzer used in the 1968 report of Goodwin et al. may be different from that of current hemofilter units. To date, there is a dearth of information in critically ill patients on the clinical pharmacokinetics of CMS and the generated colistin to guide the selection of dosage regimens of CMS. We describe here the case of a 53-year-old woman (110 kg; ideal body weight, 61 kg) who presented with bowel perforations leading to multiple organ failure requiring continuous venovenous hemodiafiltration (CVVHDF). CVVHDF (2) was performed with 1 liter/h of dialysate and 2 liters/h of postdilution replacement fluid, producing 3 liters/h of dialysis effluent; blood flow was set at 200 ml/min through an extracorporeal circuit containing a Hospal AN69HF hemofilter. Systemic tobramycin had been ceased on day 20 of hospital admission due to decreased renal function and nebulized tobramycin (80 mg every 8 h) was commenced. Due to an infection caused by a new multidrug-resistant Pseudomonas aeruginosa strain isolated in endotracheal aspirate, which was susceptible only to colistin and tobramycin, intravenous CMS at a dosage of 150 mg (equivalent to 2.46 mg per kg of ideal body weight) every 24 h was commenced on day 24 of admission and changed to 150 mg/48 h on day 38 (12, 14). Each dose was administered as a 30-min infusion. Meropenem and nebulized tobramycin were coadministered. After CMS administration on day 44, blood and effluent dialysate were collected up to 48 h postdose for high-performance liquid chromatography quantification of CMS (5) and colistin (4) in plasma and dialysate (accuracy within 14.1% and coefficients of variation less than 6.66%), to permit pharmacokinetic analysis. MICs of CMS and colistin were determined by broth microdilution (13). The concentrations of CMS and colistin in plasma and dialysate are shown in Fig. 1. The maximum concentration of colistin in plasma occurred 30 min after completion of the CMS infusion, consistent with relatively rapid conversion to colistin (6). The terminal half-lives of CMS and colistin in plasma were 6.83 h and 7.52 h, respectively. The total clearance of CMS was 48.7 ml/min and its volume of distribution was 10.9 liters. From 0 to 8 h after dosing, 20.3% of the dose was recovered in the dialysate as CMS and 6.88% as colistin. CVVHDF clearances of CMS (11.2 ml/min) and colistin (11.9 ml/min) were similar. The MICs of CMS and colistin against the P. aeruginosa isolate from the patient were 4.0 mg/liter and 1.0 mg/liter, respectively. The maximum concentrations of CMS and colistin in plasma were 23.3 mg/liter and 1.84 mg/liter, respectively (Fig. 1). Even without the consideration of plasma protein binding, the maximum concentration for CMS in plasma was less than 16 MIC and that for colistin was less than 2 MIC; rapid killing and significant postantibiotic effect in vitro against P. aeruginosa has been shown to occur above these MIC thresholds (8). In addition and importantly, the plasma con-