Simulated Intravenous versus Inhaled Tobramycin with or without Intravenous Ceftazidime Evaluated against Hypermutable Pseudomonas aeruginosa via a Dynamic Biofilm Model and Mechanism-Based Modeling

Hajira Bilal; Jessica R Tait; Yinzhi Lang; Jieqiang Zhou; Phillip J Bergen; Anton Y Peleg; Jürgen B Bulitta; Antonio Oliver; Roger L Nation; Cornelia B Landersdorfer

doi:10.1128/aac.02203-21

Simulated Intravenous versus Inhaled Tobramycin with or without Intravenous Ceftazidime Evaluated against Hypermutable Pseudomonas aeruginosa via a Dynamic Biofilm Model and Mechanism-Based Modeling

Antimicrob Agents Chemother. 2022 Mar 15;66(3):e0220321. doi: 10.1128/aac.02203-21. Epub 2022 Jan 18.

Authors

Affiliations

¹ Centre for Medicine Use and Safety, Monash Institute of Pharmaceutical Sciences, Monash Universitygrid.1002.3, Parkville, Victoria, Australia.
² Drug Delivery, Disposition and Dynamics, Monash Institute of Pharmaceutical Sciences, Monash Universitygrid.1002.3, Parkville, Victoria, Australia.
³ Department of Pharmacotherapy and Translational Research, College of Pharmacy, University of Floridagrid.15276.37, Orlando, Florida, USA.
⁴ Department of Infectious Diseases, The Alfred Hospital and Central Clinical School, Monash Universitygrid.1002.3, Melbourne, Australia.
⁵ Hospital Universitario Son Espasesgrid.411164.7, Palma de Mallorca, Spain.

Abstract

Acute exacerbations of chronic respiratory infections in patients with cystic fibrosis are highly challenging due to hypermutable Pseudomonas aeruginosa, biofilm formation and resistance emergence. We aimed to systematically evaluate the effects of intravenous versus inhaled tobramycin (TOB) with and without intravenous ceftazidime (CAZ). Two hypermutable P. aeruginosa isolates, CW30 (MIC_CAZ, 0.5 mg/liter; MIC_TOB, 2 mg/liter) and CW8 (MIC_CAZ, 2 mg/liter; MIC_TOB, 8 mg/liter), were investigated for 120 h in dynamic in vitro biofilm studies. Treatments were intravenous ceftazidime, 9 g/day (33% lung fluid penetration); intravenous tobramycin, 10 mg/kg of body every 24 h (50% lung fluid penetration); inhaled tobramycin, 300 mg every 12 h; and both ceftazidime-tobramycin combinations. Total and less susceptible planktonic and biofilm bacteria were quantified over 120 h. Mechanism-based modeling was performed. All monotherapies were ineffective for both isolates, with regrowth of planktonic (≥4.7 log₁₀ CFU/ml) and biofilm (>3.8 log₁₀ CFU/cm²) bacteria and resistance amplification by 120 h. Both combination treatments demonstrated synergistic or enhanced bacterial killing of planktonic and biofilm bacteria. With the combination simulating tobramycin inhalation, planktonic bacterial counts of the two isolates at 120 h were 0.47% and 36% of those for the combination with intravenous tobramycin; for biofilm bacteria the corresponding values were 8.2% and 13%. Combination regimens achieved substantial suppression of resistance of planktonic and biofilm bacteria compared to each antibiotic in monotherapy for both isolates. Mechanism-based modeling well described all planktonic and biofilm counts and indicated synergy of the combination regimens despite reduced activity of tobramycin in biofilm. Combination regimens of inhaled tobramycin with ceftazidime hold promise to treat acute exacerbations caused by hypermutable P. aeruginosa strains and warrant further investigation.

Keywords: Pseudomonas aeruginosa; dosage regimen optimization; dynamic infection model; mathematical modeling; pharmacodynamics; pharmacokinetics.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Anti-Bacterial Agents / pharmacology
Anti-Bacterial Agents / therapeutic use
Biofilms
Ceftazidime / pharmacology
Ceftazidime / therapeutic use
Humans
Microbial Sensitivity Tests
Pseudomonas Infections* / drug therapy
Pseudomonas Infections* / microbiology
Pseudomonas aeruginosa*
Tobramycin / pharmacology
Tobramycin / therapeutic use

Substances

Anti-Bacterial Agents
Ceftazidime
Tobramycin