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Toward Repositioning Niclosamide for Antivirulence Therapy of Pseudomonas aeruginosa Lung Infections: Development of Inhalable Formulations through Nanosuspension Technology

Authors :
Agnese Miro
Francesco Imperi
Francesca Ungaro
Gabriella Costabile
Raffaella Sorrentino
Roberta d'Emmanuele di Villa Bianca
Emma Mitidieri
Fabiana Quaglia
Giordano Rampioni
Livia Leoni
Barbara Pompili
Ivana d'Angelo
Roslen Bondì
Fiorentina Ascenzioni
Costabile, Gabriella
D'Angelo, I
Rampioni, G
Bondì, R
Pompili, B
Ascenzioni, F
Mitidieri, Emma
D'EMMANUELE DI VILLA BIANCA, Roberta
Sorrentino, Raffaella
Miro, Agnese
Quaglia, Fabiana
Imperi, F
Leoni, L
Ungaro, Francesca
D'Angelo, Ivana
Rampioni, Giordano
Bondì, Roslen
Pompili, Barbara
Ascenzioni, Fiorentina
d'Emmanuele di Villa Bianca, Roberta
Imperi, Francesco
Leoni, Livia
Bondi, Roslen
Bianca Roberta d'Emrnanuele di, Villa
Publication Year :
2015

Abstract

Inhaled antivirulence drugs are currently considered a promising therapeutic option to treat Pseudomonas aeruginosa lung infections in cystic fibrosis (CF). We have recently shown that the anthelmintic drug niclosamide (NCL) has strong quorum sensing (QS) inhibiting activity against P. aeruginosa and could be repurposed as an antivirulence drug. In this work, we developed dry powders containing NCL nanoparticles that can be reconstituted in saline solution to produce inhalable nanosuspensions. NCL nanoparticles were produced by high-pressure homogenization (HPH) using polysorbate 20 or polysorbate 80 as stabilizers. After 20 cycles of HPH, all formulations showed similar properties in the form of needle-shape nanocrystals with a hydrodynamic diameter of approximately 450 nm and a zeta potential of -20 mV. Nanosuspensions stabilized with polysorbate 80 at 10% w/w to NCL (T80_10) showed an optimal solubility profile in simulated interstitial lung fluid. T80_10 was successfully dried into mannitol-based dry powder by spray drying. Dry powder (T80_10 DP) was reconstituted in saline solution and showed optimal in vitro aerosol performance. Both T80_10 and T80_10 DP were able to inhibit P. aeruginosa QS at NCL concentrations of 2.5-10 mu M. NCL, and these formulations did not significantly affect the viability of CF bronchial epithelial cells in vitro at microbiologically active concentrations (i.e.

Subjects

Subjects :
Lung Diseases
Male
Chemistry, Pharmaceutical
Drug Evaluation, Preclinical
pulmonary delivery
Pharmaceutical Science
Pharmacology
antivirulence drug
nasuspension
medicine.disease_cause
antivirulence drugs
cystic fibrosis
chemistry.chemical_compound
In vivo
Drug Discovery
Administration, Inhalation
medicine
Animals
rat
Pseudomonas Infections
Rats, Wistar
Niclosamide
cystic fibrosi
nanosuspension
Virulence
Chemistry
Pseudomonas aeruginosa
Drug Discovery3003 Pharmaceutical Science
niclosamide
Drug Repositioning
quorum sensing
nanosuspensions
Acute toxicity
3003
Molecular Medicine
Anti-Bacterial Agents
Rats
Spray drying
Toxicity
Nanoparticles
Polysorbate 20
Mannitol
Pseudomonas aeruginosa, anti-virulence drugs, cystic fibrosis, nanosuspensions, niclosamide, pulmonary delivery, quorum sensing, rat
Powders
medicine.drug

Details

Language :
English
Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....dd89bb64e233c2210a9c15bc9d8d5ea0

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Authors Abstract Subjects Details