Please use this identifier to cite or link to this item: http://localhost:80/xmlui/handle/123456789/13635
Title: Piroxicam loaded polymer hybrid microspheres based tablets with modified release kinetics: Development, characterization and in vivo evaluation
Authors: Hamid, Hajra Afeera
Khan, Shahzeb
Shah, Syed Muhammad Noor
Asghar, Muhammad
Shahid, Muhammad
Hussain, Zahid
Sohail, Muhammad
Barkat, Ali Khan
Amin, Fazli
Jan, Syed Umer
Elhissi, Abdelbary
Shah, Syed Muhammad Hassan
Minhas, Muhammad Usman
Shah, Syed Wadood Ali
Ahmad, Naveed
Keywords: Piroxicam
microspheres
dissolution
bioavailability
stability
Issue Date: 16-Jan-2021
Publisher: Karachi: Faculty of Pharmacy & Pharmaceutical Sciecnes, University of Karachi
Abstract: Piroxicam (PC) is a non-steroidal anti-inflammatory drug characterized by poor aqueous solubility and reported to cause and impart crucial GIT irritation, bleeding, peptic and duodenal ulcer. Engineering of PC loaded microcapsules and its surface modification using different polymers has become the popular approach to address the said issues. The purpose of the study was to develop new PC loaded gastro-protective polymer hybrid microspheres (PHM) with subsequent conversion to tablet dosage form having modified dissolution rate and improved bioavailability. The crystallinity of the PC loaded PHM were established through powder X-ray diffraction. The optimised microspheres, PCM1 with particle size 32±3.0µm, entrapment efficiency 83.78±2.5% and in vitro drug release 87.1±2.6% were further subjected to tablets development and in vivo evaluation. The in vitro drug release study conducted for PHM at pH media 1.2 and 6.8 demonstrated retarded and enhanced drug release rates (P<0.001) respectively. Both accelerated and real time stability studies confirmed stability of the PC loaded PHM based tablets. A substantial improvement in the drug plasma concentration 12.6±2.36 (P<0.001) was observed for the produced tablets compared to the marketed formulations.
URI: http://142.54.178.187:9060/xmlui/handle/123456789/13635
ISSN: 1011-601X
Appears in Collections:Issue 01 (Supplementary)

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