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Vol. 15. Issue 5.
Pages 413-419 (September - October 2011)
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Vol. 15. Issue 5.
Pages 413-419 (September - October 2011)
Original article
Open Access
Assessing the pharmacodynamic profile of intravenous antibiotics against prevalent Gram-negative organisms collected in Colombia
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Maria Virginia Villegas1,
Corresponding author
mariavirginia.villegas@gmail.com

Correspondence to: International Center for Medical, Research & Training (CIDEIM), Carrera 125 # 19 - 225, Cali, Colombia, Phone: (57-2) 555-2164, Fax: (57-2) 555-2638
, David Felipe Briceno2, Sory Jamil Ruiz2, Guilherme H. Furtado3, David P. Nicolau4
1 Principal Investigator, Bacterial Resistance Group, International Center for Medical Research and Training (CIDEIM), Cali, Colombia
2 Research Assistants, Bacterial Resistance Group, CIDEIM, Cali, Colombia
3 Infectious Diseases; Center for Anti-Infective Research and Development, Hartford Hospital, Hartford, CT, USA; Hospital São Paulo, Division of Infectious Diseases, Universidade Federal de São Paulo, São Paulo, Brazil
4 Center for Anti-Infective Research and Development, Hartford Hospital, Hartford, CT, USA; Division of Infectious Diseases, Hartford Hospital, Hartford, CT, USA
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Article information
Abstract
Objectives

This study was designed to simulate standard and optimized dosing regimens for intravenous antibiotics against contemporary populations of Escherichia coli, Klebsiella pneumoniae, Acinetobacter baumannii, and Pseudomonas aeruginosa using MIC distribution data to determine which of the tested carbapenem regimens provided the greatest opportunity for obtaining maximal pharmacodynamic (PD) activity.

Methods

The isolates studied were obtained from the COMPACT-COLOMBIA surveillance program conducted between February and November 2009. Antimicrobial susceptibility testing was conducted by broth microdilution method according to the CLSI guidelines. Doripenem, imipenem-cilastatin, and meropenem, were the modeled antibiotics. A 5,000 patient Monte Carlo simulation was performed for each regimen and PD targets were defined as free drug concentrations above the MIC for at least 40% of the dosing interval.

Results

All carbapenem regimens obtained optimal exposures against E. coli, unlike the other Enterobacteriaceae tested. Against P. aeruginosa, only a prolonged infusion of doripenem exceeded the 90% cumulative fraction of response (CFR) threshold. Worrisomely, no regimens for any of the drugs tested obtained optimal CFR against A. baumannii. For P. aeruginosa intensive care unit (ICU) isolates, CFR was approximately 20% lower for isolates collected in the respiratory tract compared with bloodstream or intra-abdominal for imipenem and meropenem. Noteworthy, all doripenem and meropenem regimens achieved greater than 90% CFR against bloodstream and respiratory isolates of K. pneumoniae.

Conclusions

Our data suggests that higher dosing and prolonged infusion of doripenem or meropenem may be suitable for empirically treating ICU P. aeruginosa, while none of the carbapenems achieved optimal cumulative fraction of response against A. baumannii. Standard dosing regimens of all the carbapenems tested achieved optimal CFR against E. coli isolates, but higher carbapenem dosages might be required for empiric treatment of K. pneumoniae, particularly from an intra-abdominal source. Non-standard dosage regimens studied in this modeling should be proven effective in prospective clinical trials.

Keywords:
drug resistance, bacterial
Gram-negative bacteria
Monte Carlo Method
Colombia
pharmacology
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References
[1.]
P. Koomanachai, C.C. Bulik, J.L. Kuti, et al.
Pharmacodynamic modeling of intravenous antibiotics against gram-negative bacteria collected in the United States.
[2.]
J. Roberts, A. Kwa, P. Montakantikul, et al.
Pharmacodynamic profiling of intravenous antibiotics against prevalent Gram-negative organisms across the globe: The PASSPORT Program – Asia-Pacific Region.
Int J Antimicrob Agents, 37 (2011), pp. 225-229
[3.]
C.A. DeRyke, J.L. Kuti, D.P. Nicolau.
Pharmacodynamic target attainment of six beta-lactams and two fluoroquinolones against Pseudomonas aeruginosa, Acinetobacter baumannii. Escherichia coli, and Klebsiella species collected from United States intensive care units in 2004.
Pharmacotherapy, 27 (2007), pp. 333-342
[4.]
G.L. Drusano.
Antimicrobial pharmacodynamics: critical interactions of bug and drug.
Nat Rev Microbiol, 2 (2004), pp. 289-300
[5.]
Clinical and Laboratory Standards Institute. Performance Standards for Antimicrobial Susceptibility Testing; Tenth Informational Supplement. CLSI document M100-S20-U. Wayne, PA: CLSI. 2010.
[6.]
Doribax (doripenem for infection) [prescribing information]. http://www.doribax.com/doribax/shared/pi/doribax.pdf. Accessed July 19, 2010.
[7.]
M.V. Villegas, K. Lolans, A. Correa, et al.
First detection of the plasmid-mediated class A carbapenemase KPC-2 in clinical isolates of Klebsiella pneumoniae from South America.
Antimicrob Agents Chemother, 50 (2006), pp. 2880-2882
[8.]
M.V. Villegas, J.N. Kattan, A. Correa, et al.
Dissemination of Acinetobacter baumannii clones with OXA-23 Carbapenemase in Colombian hospitals.
Antimicrob Agents Chemother, 51 (2007), pp. 2001-2004
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