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Literature DB >> 26926631

Sequential Treatment of Biofilms with Aztreonam and Tobramycin Is a Novel Strategy for Combating Pseudomonas aeruginosa Chronic Respiratory Infections.

Estrella Rojo-Molinero¹, María D Macià², Rosa Rubio³, Bartolomé Moyà², Gabriel Cabot², Carla López-Causapé², José L Pérez², Rafael Cantón⁴, Antonio Oliver².

Abstract

Traditional therapeutic strategies to control chronic colonization in cystic fibrosis (CF) patients are based on the use of a single nebulized antibiotic. In this study, we evaluated the therapeutic efficacy and dynamics of antibiotic resistance in Pseudomonas aeruginosa biofilms under sequential therapy with inhaled aztreonam (ATM) and tobramycin (TOB). Laboratory strains PAO1, PAOMS (hypermutable), PAOMA (mucoid), and PAOMSA (mucoid and hypermutable) and two hypermutable CF strains, 146-HSE (Liverpool epidemic strain [LES-1]) and 1089-HSE (ST1089), were used. Biofilms were developed using the flow cell system. Mature biofilms were challenged with peak and 1/10-peak concentrations of ATM (700 mg/liter and 70 mg/liter), TOB (1,000 mg/liter and 100 mg/liter), and their alternations (ATM/TOB/ATM and TOB/ATM/TOB) for 2 (t = 2), 4 (t = 4), and 6 days (t = 6). The numbers of viable cells (CFU) and resistant mutants were determined. Biofilm structural dynamics were monitored by confocal laser scanning microscopy and processed with COMSTAT and IMARIS software programs. TOB monotherapy produced an intense decrease in CFU that was not always correlated with a reduction in biomass and/or a bactericidal effect on biofilms, particularly for the CF strains. The ATM monotherapy bactericidal effect was lower, but effects on biofilm biomass and/or structure, including intense filamentation, were documented. The alternation of TOB and ATM led to an enhancement of the antibiofilm activity against laboratory and CF strains compared to that with the individual regimens, potentiating the bactericidal effect and/or the reduction in biomass, particularly at peak concentrations. Resistant mutants were not documented in any of the regimens at the peak concentrations and only anecdotally at the 1/10-peak concentrations. These results support the clinical evaluation of sequential regimens with inhaled antibiotics in CF, as opposed to the current maintenance treatments with just one antibiotic in monotherapy.

Entities: Chemical Disease Species

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Year: 2016 PMID： 26926631 PMCID： PMC4862541 DOI： 10.1128/AAC.00196-16

Source DB: PubMed Journal: Antimicrob Agents Chemother ISSN： 0066-4804 Impact factor: 5.191

41 in total

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8 in total

1. Use of Calgary and Microfluidic BioFlux Systems To Test the Activity of Fosfomycin and Tobramycin Alone and in Combination against Cystic Fibrosis Pseudomonas aeruginosa Biofilms.

Authors: María Díez-Aguilar; María Isabel Morosini; Emin Köksal; Antonio Oliver; Miquel Ekkelenkamp; Rafael Cantón
Journal: Antimicrob Agents Chemother Date: 2017-12-21 Impact factor: 5.191

2. Genomic Analysis Identifies Novel Pseudomonas aeruginosa Resistance Genes under Selection during Inhaled Aztreonam Therapy In Vivo.

Authors: Kathryn McLean; Duankun Lee; Elizabeth A Holmes; Kelsi Penewit; Adam Waalkes; Mingxin Ren; Samuel A Lee; Joseph Gasper; Colin Manoil; Stephen J Salipante
Journal: Antimicrob Agents Chemother Date: 2019-08-23 Impact factor: 5.191

3. Blood mRNA biomarkers distinguish variable systemic and sputum inflammation at treatment initiation of inhaled antibiotics in cystic fibrosis: A prospective non-randomized trial.

Authors: Silvia M Caceres; Linda A Sanders; Noel M Rysavy; Katie R Poch; Caroline R Jones; Kyle Pickard; Tasha E Fingerlin; Roland A Marcus; Kenneth C Malcolm; Jennifer L Taylor-Cousar; David P Nichols; Jerry A Nick; Matthew Strand; Milene T Saavedra
Journal: PLoS One Date: 2022-05-05 Impact factor: 3.240

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Authors: Peter Jorth; Kathryn McLean; Anina Ratjen; Patrick R Secor; Gilbert E Bautista; Sumedha Ravishankar; Amir Rezayat; Jayanthi Garudathri; Joe J Harrison; Rachel A Harwood; Kelsi Penewit; Adam Waalkes; Pradeep K Singh; Stephen J Salipante
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Authors: Anaïs Soares; François Caron; Manuel Etienne
Journal: Front Microbiol Date: 2019-09-18 Impact factor: 5.640