Evaluation of Imipenem for Prophylaxis and Therapy of Yersinia pestis Delivered by Aerosol in a Mouse Model of Pneumonic Plague

It has been previously shown that mice subjected to an aerosol exposure to Yersinia pestis and treated with β-lactam antibiotics after a delay of 42 h died at an accelerated rate compared to controls. It was hypothesized that endotoxin release in antibiotic-treated mice accounted for the accelerated...

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Bibliographic Details
Published in:Antimicrobial agents and chemotherapy 2014-06, Vol.58 (6), p.3276-3284
Main Authors: HEINE, Henry S, LOUIE, Arnold, KINZIG-SCHIPPERS, Martina, DRUSANO, George L, ADAMOVICZ, Jeffrey J, AMEMYA, Kei, FAST, Randy L, MILLER, Lynda, OPAL, Steven M, PALARDY, John, PAREJO, Nicolas A, SÖRGEL, Fritz
Format: Article
Language:English
Subjects:
Aerosols
Animals
Anti-Bacterial Agents
Anti-Bacterial Agents - pharmacokinetics
Anti-Bacterial Agents - pharmacology
Anti-Bacterial Agents - therapeutic use
Antibiotics. Antiinfectious agents. Antiparasitic agents
Bacterial diseases
Biological and medical sciences
Ceftazidime - pharmacokinetics
Ceftazidime - pharmacology
Ceftazidime - therapeutic use
Ciprofloxacin - pharmacokinetics
Ciprofloxacin - pharmacology
Ciprofloxacin - therapeutic use
Cytokines - metabolism
Endotoxins - analysis
Experimental Therapeutics
Female
Human bacterial diseases
Imipenem
Imipenem - pharmacokinetics
Imipenem - pharmacology
Imipenem - therapeutic use
Infectious diseases
Medical sciences
Mice
Mice, Inbred BALB C
Microbial Sensitivity Tests
Pharmacology. Drug treatments
Plague
Plague - metabolism
Plague - microbiology
Plague - prevention & control
Survival Analysis
Tropical bacterial diseases
Yersinia pestis
Yersinia pestis - drug effects
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Summary:It has been previously shown that mice subjected to an aerosol exposure to Yersinia pestis and treated with β-lactam antibiotics after a delay of 42 h died at an accelerated rate compared to controls. It was hypothesized that endotoxin release in antibiotic-treated mice accounted for the accelerated death rate in the mice exposed to aerosol Y. pestis. Imipenem, a β-lactam antibiotic, binds to penicillin binding protein 2 with the highest affinity and produces rounded cells. The binding of imipenem causes cells to lyse quickly and thereby to release less free endotoxin. Two imipenem regimens producing fractions of time that the concentration of free, unbound drug was above the MIC (fT>MIC) of approximately 25% (6/24 h) and 40% (9.5/24 h) were evaluated. In the postexposure prophylaxis study, the 40% and 25% regimens produced 90% and 40% survivorship, respectively. In the 42-h treatment study, both regimens demonstrated a 40 to 50% survivorship at therapy cessation and some deaths thereafter, resulting in a 30% survivorship. As this was an improvement over the results with other β-lactams, a comparison of both endotoxin and cytokine levels in mice treated with imipenem and ceftazidime (a β-lactam previously demonstrated to accelerate death in mice during treatment) was performed and supported the original hypotheses; however, the levels observed in animals treated with ciprofloxacin (included as an unrelated antibiotic that is also bactericidal but should cause little lysis due to a different mode of action) were elevated and significantly (7-fold) higher than those with ceftazidime.
ISSN:0066-4804
1098-6596
DOI:10.1128/AAC.02420-14