Litcius/Paper detail

Inhaled dry powder liposomal azithromycin for treatment of chronic lower respiratory tract infection

Yahya H. Dallal Bashi, Ahlam Ali, Yuosef Al Ayoub, K.H. Assi, Rachel Mairs, Helen O. McCarthy, Michael M. Tunney, Victoria Kett

2024International Journal of Pharmaceutics14 citationsDOIOpen Access PDF

Abstract

A dry powder inhaled liposomal azithromycin formulation was developed for the treatment of chronic respiratory diseases such as cystic fibrosis and bronchiectasis. Key properties including liposome size, charge and encapsulation efficiency powder size, shape, glass transition temperature (Tg), water content and in vitro respiratory deposition were determined. Antimicrobial activity against cystic fibrosis (CF) respiratory pathogens was determined by MIC, MBC and biofilm assays. Cytotoxicity and cellular uptake studies were performed using A549 cells. The average liposome size was 105 nm, charge was 55 mV and encapsulation efficiency was 75 %. The mean powder particle size d[v,50] of 4.54 µm and Mass Median Aerodynamic Diameter (MMAD) was 5.23 µm with a mean Tg of 76˚C and water content of 2.1 %. These excellent physicochemical characteristics were maintained over one year. Liposomal loaded azithromycin demonstrated enhanced activity against P. aeruginosa clinical isolates grown in biofilm. The formulation was rapidly delivered into bacterial cells with > 75 % uptake in 1 h. Rapid uptake into A549 cells via a cholesterol-dependent endocytosis pathway with no cytotoxic effects apparent. These data demonstrate that this formulation could offer benefits over current treatment regimens for people with chronic respiratory infection.

Topics & Concepts

AzithromycinMedicineLiposomeRespiratory tractAntibacterial agentRespiratory systemRespiratory tract infectionsPharmacologyAntibioticsMicrobiologyInternal medicineChemistryBiologyBiochemistryInhalation and Respiratory Drug DeliveryAsthma and respiratory diseasesRespiratory and Cough-Related Research