Colistin loading dose in renal failure
Colistin Dosing in Renally Impaired Patients Special Feature By Jessica C. Song, MA, PharmD, Assistant Professor, Pharmacy Practice, University of the Pacific, Stockton, CA, Pharmacy Clerkship and Coordinator, Santa Clara Valley Medical Center, Section Editor, Managed Care, is Associate Editor for Infectious Disease Alert. Dr. Song reports no financial relationships relevant to this field of study. Colistin (Ppolymyxin E) was isolated from bacillus colistinus 60 years ago and, during the 1960s, a new intravenous formulation (Coly-Mycin M Parenteral) became available for use in clinical practice.1-3 Despite widespread use of colistin during the first two decades after its introduction, the emergence of reports of serious adverse events caused this agent to fall out of favor in the medical community.4 At present, expansion of multi-drug resistant (MDR) bacteria, including Acinetobacter baumannii, Pseudomonas aeruginosa, and carbapenemase-producing Enterobacteriaceae, has resulted in renewed interest in old antimicrobial agents such as colistin.5 To date, most information available about the dosing of colistin in renally impaired patients is from studies conducted four decades ago and may not apply to patients requiring treatment at the present time.6-8 The purpose of this review is to discuss the pharmacokinetics of colistin in dialysis patients and to review dosing of this drug in renally impaired patients included in published studies. Renal Dose Adjustment of Colistin Two forms of colistin are distributed as commercially available products: colistin sulfate and colistimethate sodium (also known as colistin methanesulfonate, colistin sulphomethate sodium). Because of its toxicity profile, colistin sulfate is restricted to topical use; colistimethate is used for parenteral or nebulized administration.4 Numerous commercial preparations of colistimethate are available worldwide, and their differences have made evaluation of doses reported in clinical studies difficult to interpret when drug formulations were not fully described by investigators.9 Colistimethate, a polyanion at physiological pH, undergoes hydrolysis to yield a series of methanesulphonated derivatives and colistin, which is a polycation entity. Coly-Mycin M Parenteral is produced by JHP Pharmaceuticals, LLC, in the United States.10 The current FDA-approved package insert for Coly-Mycin M Parenteral states that each vial contains 150 mg of colistin base and should be given at a dose of 2.5 to 5 mg/kg/day (not to exceed 300 mg/day, based on ideal body weight) in 2-4 divided doses. Given that there is 360 mg of colistimethate per 150 mg of colistin base, this translates into a 2.4-fold higher recommended dose of the colistimethate equivalent.11 A commonly used formulation of colistimethate in Europe is Colomycin injection, produced by Dumex-Alpharma A/S (Copenhagen, Denmark). The package insert states that each million unit of the product contains 80 mg of colistimethate (12,500 units/milligram). The colistin formulation distributed by Norma Pharmaceuticals (Greece) has been reported to consist of 12,500 to 13,300 units per milligram.11 The FDA-approved package insert for Coly-Mycin states that patients with a serum creatinine of 1.3 to 1.5 mg/dL should be given 2.5 mg/kg to 3.8 mg/kg of colistin base (6-9.1 mg/kg colistimethate) daily, in two divided doses. Patients with a serum creatinine of 1.6 to 2.5 mg/dL should be given 2.5 mg/kg of colistin base (6 mg/kg colistimethate) daily, in one or two divided doses. When serum creatinine increases to 2.6 to 4.0 mg/dL, the patient should receive 1.5 mg/kg of colistin base (3.6 mg/kg colistimethate) every 36 hours. The manufacturer does not provide dosing recommendations for hemodialysis patients or for peritoneal dialysis patients.10 Renal dose adjustments of colistimethate reported in clinical trials are summarized in Table 1.
Dosing of colistin in hemodialysis patients has varied in published reports. Michalopoulos and colleagues used a dose of Colomycin 3 million units (240 mg colistimethate; 100 mg colistin base) IV every 36 hours in patients with serum creatinine levels of 2.6 mg/dL or higher, and administered 1 million units (80 mg colistimethate; 33.3 mg colistin base) post-dialysis.15 Similarly, Falagas and colleagues used Colomycin 2 million units (160 mg colistimethate; 66.7 mg colistin base) IV every 36 hours in patients with serum creatinine levels of 2.6 mg/dL or higher, and used a post-dialysis dose of 1 million units of this agent in hemodialysis patients.16 A daily dose of 1 mg/kg Coly-Mycin was administered to hemodialysis patients enrolled in a study conducted by Linden and colleagues.18 Recently, a case report of two patients highlighted the possibility of dosing colistin more frequently in patients receiving intermittent hemodialysis.19 Marchand et al reported the use of more frequent dosing of colistimethate in two male patients with acute renal failure who presented with pulmonary infection caused by MDR gram-negative bacteria susceptible to this antibiotic. The patients received intermittent hemodialysis (Gambro, AK 200), with a blood flow setting of 300 mL/minute and dialysis effluent at 500 mL/minute for four hours, using a 1.6 m2 B3 polymethylmethacrylate membrane (Toray Industries, Tokyo, Japan). The first patient received 1 million units of colistimethate (80 mg colistimethate, 33.3 mg colistin base) every 48 hours, with hemodialysis sessions occurring every 48 hours. The second patient received 2 million units of colistimethate (160 mg colistimethate; 66.7 mg colistin base) every 12 hours, and received hemodialysis on a daily basis. Marchand et al discovered that a dosing regimen of 1 million units every 48 hours resulted in sub-therapeutic pre-dialysis levels of colistimethate. The first patient had a pre-dialysis colistin plasma concentration of 0.45 mg/L, which was far below the European Committee on Antimicrobial Susceptibility Testing minimum inhibitory concentration (MIC) breakpoint of 2 mg/liter. Consequently, a higher dose of colistimethate was administered to the second patient. The second patient did exhibit pre-dialysis colistin plasma concentrations close to the MIC breakpoint of 2 mg/L. The time-averaged dialysis clearances of colistin and colistimethate were approximately 134-140 mL/minute and 90 mL/minute, respectively. Because intermittent hemodialysis removed a significant quantity of colistin and colistimethate, Marchand et al recommended a dose of colistimethate 160 mg (colistin base 66.7 mg) every 12 hours in patients receiving intermittent hemodialysis. Li and colleagues reported a case of a 53-year-old female (ideal body weight, 61 kg) who required colistin therapy for a new MDR Pseudomonas aeruginosa strain isolated in endotracheal aspirate.20 The patient received continuous venovenous hemodiafiltration (CVVHDF) with 1 L/hour of dialysate and 2 L/hour of post-dilution replacement fluid, yielding 3 L/hour of dialysis effluent; an extracorporeal circuit containing a hospital AN69HF hemofilter was used and the blood flow was set at 200 mL/minute. The patient received intravenous Coly-Mycin 2.5 mg/kg (colistin base; colistimethate equivalent, 6 mg/kg) every 48 hours. The MIC of colistin against the P. aeruginosa isolate from the patient was 1.0 mg/L; the concentrations of colistin in plasma were below the MIC for 42 hours of the 48-hour dosing interval. Consequently, Li et al suggested that a dose of intravenous colistin base 2-3 mg/kg (colistimethate 4.8-7.2 mg/kg) every 12 hours would have been more appropriate for their patient. Dosing recommendations for peritoneal dialysis patients are even less clear, given that studies were conducted four decades ago in this population.6,7 Curtis et al described the pharmacokinetics of colistin in three peritoneal dialysis patients (weight range, 50-60 kg) who received colistimethate 2-3 mg/kg during dialysis.6 The investigators used Dialaflex solution and 2 L exchanges with 30-minute equilibration periods. The patients exhibited a mean peritoneal clearance of 9.8 mL/minute, showing poor clearance of colistin during peritoneal dialysis. Curtis et al proposed a dose of 2-3 mg/kg colistimethate (0.8-1.2 mg/kg colistin base) given intravenously every 72 hours for peritoneal dialysis patients. Conclusion Colistin has not been studied extensively in renally impaired patients, especially those requiring hemodialysis or peritoneal dialysis. In light of these limitations, the following recommendations can be made:
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