Pharmacodynamics of intravenous ciprofloxacin in seriously ill patients.

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Antimicrob Agents Chemother. 1993 May; 37(5): 1073-1081

Pharmacodynamics of intravenous ciprofloxacin in seriously ill patients.

A Forrest, D E Nix, C H Ballow, T F Goss, M C Birmingham and J J Schentag

Center for Clinical Pharmacy Research, School of Pharmacy, State University of New York, Buffalo 14260.

ABSTRACT

Seventy-four acutely ill patients were treated with intravenousciprofloxacin at dosages ranging between 200 mg every 12 h and400 mg every 8 h. A population pharmacokinetic-pharmacodynamicanalysis relating drug exposure (and other factors) to infectiousoutcome was performed. Plasma samples were obtained and assayedfor ciprofloxacin by high-performance liquid chromatography.Samples from patients were frequently cultured so that the dayof bacterial eradication could be determined. The pharmacokineticdata were fitted by iterative two-stage analysis, assuming alinear two-compartment model. Logistic regression was used tomodel ciprofloxacin exposure (and other potential covariates)versus the probabilities of achieving clinical and microbiologiccures. The same variables were also modelled versus the timeto bacterial eradication by proportional hazards regression.The independent variables considered were dose, site of infection,infecting organism and the MIC for it, percent time above theMIC, peak, peak/MIC ratio, trough, trough/MIC ratio, 24-h areaunder the concentration-time curve (AUC), AUC/MIC ratio (AUIC),presence of other active antibacterial agents, and patient characteristics.The most important predictor for all three measures of ciprofloxacinpharmacodynamics was the AUIC. A 24-h AUIC of 125 SIT-1.h (inverseserum inhibitory titer integrated over time) was found to bea significant breakpoint for probabilities of both clinicaland microbiologic cures. At an AUIC below 125 (19 patients),the percent probabilities of clinical and microbiologic cureswere 42 and 26%, respectively. At an AUIC above 125 (45 patients),the probabilities were 80% (P < 0.005) and 82% (P < 0.001),respectively. There were two significant breakpoints in thetime-to-bacterial-eradication data. At an AUIC below 125 (21patients), the median time to eradication exceeded 32 days;at an AUIC of 125 to 250 (15 patients), time to eradicationwas 6.6 days: and at AUIC above 250 (28 patients), the mediantime to eradication was 1.9 days (groups differed; P < 0.005).These findings, when combined with pharmacokinetic data reportedin the companion article, provide the rationale and tools neededfor targeting the dosage of intravenous ciprofloxacin to individualpatients' pharmacokinetics and their bacterial pathogens' susceptibilities.An a priori dosing algorithm (based on MIC, patient creatineclearance and weight, and the clinician-specified AUIC target)was developed. This approach was shown, retrospectively, tobe more precise than current guidelines, and it can be usedto achieve more rapid bacteriologic and clinical responses tociprofloxacin, as a consequence of targeting the AUIC.

Antimicrob Agents Chemother. 1993 May; 37(5): 1073-1081

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MacGowan, A. P., Rogers, C. A., Holt, H. A., Wootton, M., Bowker, K. E. (2001). Pharmacodynamics of Gemifloxacin against Streptococcus pneumoniae in an In Vitro Pharmacokinetic Model of Infection. Antimicrob. Agents Chemother. 45: 2916-2921 [Abstract] [Full Text]
Malone, R. S., Fish, D. N., Abraham, E., Teitelbaum, I. (2001). Pharmacokinetics of Levofloxacin and Ciprofloxacin during Continuous Renal Replacement Therapy in Critically Ill Patients. Antimicrob. Agents Chemother. 45: 2949-2954 [Abstract] [Full Text]
Rello, J., Paiva, J. A., Baraibar, J., Barcenilla, F., Bodi, M., Castander, D., Correa, H., Diaz, E., Garnacho, J., Llorio, M., Rios, M., Rodriguez, A., Sole-Violan, J. (2001). International Conference for the Development of Consensus on the Diagnosis and Treatment of Ventilator-Associated Pneumonia. Chest 120: 955-970 [Abstract] [Full Text]
Zhanel, G. G., Saunders, D. G., Hoban, D. J., Karlowsky, J. A. (2001). Influence of Human Serum on Antifungal Pharmacodynamics with Candida albicans. Antimicrob. Agents Chemother. 45: 2018-2022 [Abstract] [Full Text]
Mattoes, H. M., Banevicius, M., Li, D., Turley, C., Xuan, D., Nightingale, C. H., Nicolau, D. P. (2001). Pharmacodynamic Assessment of Gatifloxacin against Streptococcus pneumoniae. Antimicrob. Agents Chemother. 45: 2092-2097 [Abstract] [Full Text]
Lister, P. D., Sanders, C. C. (2001). Pharmacodynamics of moxifloxacin, levofloxacin and sparfloxacin against Streptococcus pneumoniae. J Antimicrob Chemother 47: 811-818 [Abstract] [Full Text]
Saravolatz, L., Manzor, O., Check, C., Pawlak, J., Belian, B. (2001). Antimicrobial activity of moxifloxacin, gatifloxacin and six fluoroquinolones against Streptococcus pneumoniae. J Antimicrob Chemother 47: 875-877 [Abstract] [Full Text]
Coyle, E. A., Kaatz, G. W., Rybak, M. J. (2001). Activities of Newer Fluoroquinolones against Ciprofloxacin-Resistant Streptococcus pneumoniae. Antimicrob. Agents Chemother. 45: 1654-1659 [Abstract] [Full Text]
Gee, T., Ellis, R., Marshall, G., Andrews, J., Ashby, J., Wise, R. (2001). Pharmacokinetics and Tissue Penetration of Linezolid following Multiple Oral Doses. Antimicrob. Agents Chemother. 45: 1843-1846 [Abstract] [Full Text]
Bakker-Woudenberg, I. A. J. M., ten Kate, M. T., Guo, L., Working, P., Mouton, J. W. (2001). Improved Efficacy of Ciprofloxacin Administered in Polyethylene Glycol-Coated Liposomes for Treatment of Klebsiella pneumoniae Pneumonia in Rats. Antimicrob. Agents Chemother. 45: 1487-1492 [Abstract] [Full Text]
Zhanel, G. G., Walters, M., Laing, N., Hoban, D. J. (2001). In vitro pharmacodynamic modelling simulating free serum concentrations of fluoroquinolones against multidrug-resistant Streptococcus pneumoniae. J Antimicrob Chemother 47: 435-440 [Abstract] [Full Text]
Louie, A., Kaw, P., Liu, W., Jumbe, N., Miller, M. H., Drusano, G. L. (2001). Pharmacodynamics of Daptomycin in a Murine Thigh Model of Staphylococcus aureus Infection. Antimicrob. Agents Chemother. 45: 845-851 [Abstract] [Full Text]
Drusano, G. L., Preston, S. L., Hardalo, C., Hare, R., Banfield, C., Andes, D., Vesga, O., Craig, W. A. (2001). Use of Preclinical Data for Selection of a Phase II/III Dose for Evernimicin and Identification of a Preclinical MIC Breakpoint. Antimicrob. Agents Chemother. 45: 13-22 [Abstract] [Full Text]

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