Inhalable microparticles containing large payload of antituberculosis

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dc.contributor.advisor Muttil, Pavan
dc.contributor.author Kaur, Jatinder en
dc.contributor.author Kumar, Kaushlendra en
dc.contributor.author Yadav, A B en
dc.contributor.author Sharma, Rolee en
dc.contributor.author Misra, Amit en
dc.contributor.author en
dc.date.accessioned 2007-12-26T10:57:24Z
dc.date.available 2007-12-26T10:57:24Z
dc.date.issued 2007
dc.identifier.citation EUROPEAN JOURNAL OF PHARMACEUTICAL SCIENCES 32 (2007) 140-150 en
dc.identifier.uri http://hdl.handle.net/123456789/56
dc.description.abstract Microparticles containing large payloads of two anti-tuberculosis (TB) drugs were prepared and evaluated for suitability as a dry powder inhalation targeting alveolar macrophages. A solution containing one part each of isoniazid and rifabutin, plus two parts poly(lactic acid) (L-PLA) was spraydried. Drug content and in vitro release were assayed by HPLC, and DSC was used to elucidate release behaviour. Particle size was measured by laser scattering and aerosol characteristics by cascade impaction using a Lovelace impactor. Microparticles were administered to mice using an inhouse inhalation apparatus or by intra-tracheal instillation. Drugs in solution were administered orally and by intra-cardiac injection. Flow cytometry and HPLC were used to investigate the specificity and magnitude of targeting macrophages. Microparticles having drug content -50% (w/w), particle size -5 m and satisfactory aerosol characteristics (median mass aerodynamic diameter, MMAD = 3.57 m; geometric standard deviation, GSD = 1.41m; fine particle fraction, FPF <4.6"", = 78.91:1: 8.4%) were obtained in yields of >60%. About 70% of the payload was released in vitro in 10 days. Microparticles targeted macrophages and not epithelial cells on inhalation. Drug concentrations in macrophages were -20 times higher when microparticles were inhaled rather than drug solutions administered. Microparticles were thus deemed suitable for enhanced targeted drug delivery to lung macrophages. en
dc.format.extent 582825 bytes
dc.format.mimetype application/pdf
dc.language.iso en en
dc.relation.ispartofseries CDRI Communication No 6857 en
dc.subject Dry powder inhalation en
dc.subject Respirable microspheres en
dc.subject Targeting en
dc.subject Macrophages en
dc.subject Pulmonary delivery en
dc.subject Tuberculosis en
dc.title Inhalable microparticles containing large payload of antituberculosis en
dc.type Article en


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