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Cited 19 time in webofscience Cited 20 time in scopus
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Formulation and evaluation of carrier-free dry powder inhaler containing sildenafil

Authors
Thi-Tram NguyenYi, Eun-JinHwang, Kyu-MokCho, Cheol-HeePark, Chun-WoongKim, Ju-YoungRhee, Yun-SeokPark, Eun-Seok
Issue Date
Feb-2019
Publisher
SPRINGER HEIDELBERG
Keywords
Pulmonary delivery; Carrier-free DPI; L-leucine; Spray drying; Calu-3 cells
Citation
DRUG DELIVERY AND TRANSLATIONAL RESEARCH, v.9, no.1, pp 319 - 333
Pages
15
Indexed
SCIE
SCOPUS
Journal Title
DRUG DELIVERY AND TRANSLATIONAL RESEARCH
Volume
9
Number
1
Start Page
319
End Page
333
URI
https://scholarworks.gnu.ac.kr/handle/sw.gnu/9506
DOI
10.1007/s13346-018-0586-5
ISSN
2190-393X
2190-3948
Abstract
Pulmonary delivery of sildenafil for the treatment of pulmonary arterial hypertension could overcome the limitations of intravenous and oral administration routes, such as poor patient compliance and systemic side effects. In this study, a carrier-free dry powder inhaler (DPI) formulation was developed, using spray drying technique and L-leucine as a dispersibility enhancer. Sildenafil citrate salt and sildenafil free base were evaluated for drug transport using a Calu-3 cell model, and their suitability for DPI production by spray drying was tested. Characteristics of the resultant carrier-free DPI powders were examined, namely crystallinity, morphology, size distribution, density, zeta potential, and aerodynamic performance. A Box-Behnken design was adopted to optimize the formulation and process conditions, including leucine amount, fraction of methanol in spraying solvent, and inlet temperature. While both sildenafil forms exhibited sufficient permeability for lung absorption, only sildenafil base resulted in DPI powders which were stable for 6months. The introduction of leucine into the formulations effectively enhanced aerodynamic performance of the powders and particles with favorable size, shape, and density were produced. The optimal DPI formulation determined from experimental design possesses excellent aerodynamic performance with 89.39% emitted dose and 80.08% fine particle fraction, indicating the possibility of incorporating sildenafil into carrier-free DPIs for pulmonary delivery.
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