Please use this identifier to cite or link to this item: http://10.1.7.192:80/jspui/handle/123456789/8299
Title: Rifampicin loaded chitosan nanoparticle dry powder presents: An improved therapeutic approach for alveolar tuberculosis
Authors: Rawal, Tejal
Parmar, Rajesh
Tyagi, Rajeev K.
Butani, Shital
Keywords: Rifampicin
Chitosan
Nanoparticles
Freeze drying
Pulmonary
Dry powder
Issue Date: 2017
Publisher: Elsevier
Series/Report no.: IPFP0307;
Abstract: Current treatment therapeutic approach for tuberculosis is the administration of first line drugs in the form of tablets and capsules for 4–6 months. However, this approach leads to severe adverse effects. Therefore, present study was designed to achieving local and sustained targeting of anti-tubercular drugs in order to reduce dose and frequency. The nanoparticle based dry powder formulation of rifampicin was developed and analyzed with respect to its direct targeting potential of lungs. Rifampicin loaded nanoparticles were formulated by ionic gelation probe sonication method, and characterized with respect to particle size, zeta potential, entrapment and drug loading efficiency. The range of size and entrapment efficiency of prepared nanoparticles was estimated from 124.1 ± 0.2 to 402.3 ± 2.8 nm and 72.00 ± 0.1%, respectively. The freeze-dried powder of nanoparticle formulation was used to carry out in vitro lung deposition studies through Andersen cascade impactor. The cumulative in vitro drug release studies with developed nanoparticle formulation showed sustained release up to 24 h. Our in vitro sustained drug release results were corroborated by the extended residence and slow clearance of rifampicin from the lungs. Furthermore, our results suggest the minimum lung distribution of drug in treated rats which confirms the negligible toxicity rendered by nanoparticle dry powder formulation. Moreover, pharmacokinetic and toxicity studies carried out with prepared NPs dry powder inhalation (DPI) formulations and compared with conventional DPI.
Description: Colloids and Surfaces B: Bio interfaces, 154 (2017): 321–330
URI: http://10.1.7.192:80/jspui/handle/123456789/8299
Appears in Collections:Faculty Papers

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