Two decades of imipenem therapy

doi:10.1093/jac/dkl354

JAC Advance Access originally published online on September 22, 2006
Journal of Antimicrobial Chemotherapy 2006 58(5):916-929; doi:10.1093/jac/dkl354

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© The Author 2006. Published by Oxford University Press on behalf of the British Society for Antimicrobial Chemotherapy. All rights reserved. For Permissions, please e-mail: journals.permissions@oxfordjournals.org

Review

Two decades of imipenem therapy

A. C. Rodloff¹^,*, E. J. C. Goldstein² and A. Torres³

¹ Institut for Medical Microbiology and Epidemiology of Infectious Diseases, University of Leipzig D-04103 Leipzig, Germany ² R M Alden Research Laboratory Santa Monica, CA 90404, USA ³ Institut Clínic de Pneumologia i Cirurgia Toràcica, Hospital Clínic de Barcelona Spain

^*Corresponding author. Tel: +49-341-97-15-200; Fax +49-341-97-15-209; E-mail: acr{at}medizin.uni-leipzig.de

Imipenem, the first carbapenem discovered, was developed morethan two decades ago in response to an unmet need for a highlypotent, broad-spectrum antimicrobial agent with a strong safetyprofile. It has since been used to treat more than 26 millionpatients. In an era where antibiotic use has driven antibioticresistance, choosing appropriate initial therapy for seriousinfection is critical. Appropriate antibiotic regimens mustcover all likely pathogens, be administered promptly at thecorrect dosage and dosing interval, be well tolerated and preventthe emergence of resistance. While imipenem was initially reservedfor use in intractable, serious infections, the benefits ofearly aggressive therapy are now known, making imipenem a coreagent in de-escalation therapy due to proven efficacy and safetyfor indications such as nosocomial pneumonia, intra-abdominalinfection, sepsis and febrile neutropenia. De-escalation therapywith an agent such as imipenem minimizes resistance developmentby initiating aggressive initial treatment and then tailoringtherapy based on patient response and culture results, switchingto a less expensive, narrower spectrum antibiotic regimen orshortening the duration of therapy. Imipenem has maintainedsustained clinical efficacy, tolerability and in vitro activityagainst important bacterial pathogens for two decades. We reviewthe factors that continue to make imipenem as appropriate anagent for de-escalation therapy now as it was 20 years ago.

Keywords: antibiotics , appropriate therapy , carbapenems , de-escalation , infections , pneumonia

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