Dissolution performance improvement of fenofibrate through secondary solid dispersion using PEG6000 and croscarmellose sodium combination

Dissolution performance improvement of fenofibrate through secondary solid dispersion using PEG6000 and croscarmellose sodium combination

This project report is submitted in a partial fulfillment of the requirements for the degree of Bachelor of Pharmacy, 2016

Xehetasun bibliografikoak
Egile nagusia: Khan, Tonima Akter
Beste egile batzuk: Sharmin, Shahana
Formatua: Project report
Hizkuntza:English
Argitaratua: BRAC University 2016
Gaiak:
Pharmacy
PEG6000
Sarrera elektronikoa:http://hdl.handle.net/10361/5302
id 10361-5302
record_format dspace
spelling 10361-53022019-09-30T02:56:15Z Dissolution performance improvement of fenofibrate through secondary solid dispersion using PEG6000 and croscarmellose sodium combination Khan, Tonima Akter Sharmin, Shahana Department of Pharmacy, BRAC University Pharmacy PEG6000 This project report is submitted in a partial fulfillment of the requirements for the degree of Bachelor of Pharmacy, 2016 Cataloged from PDF version of Internship report. Includes bibliographical references (page 54-55). The potential of solid dispersion based formulation using the combination of PEG6000 and croscarmellose sodium as drug carrier to enhance the dissolution performance and oral bioavailability of Fenofibrate, a poorly water soluble drug was investigated. Fenofibrate is a hydrophobic drug in fibrate class of drug which is mainly used in patients at risk of cardiovascular disease in the treatment of hypercholesterolemia and hypertriglyceridemia. Solid dispersions with different drug-to-carrier ratios were prepared by the physical mixture method and solvent method and characterized by dissolution testing within 30minutes. In vitro drug release were performed using US pharmacopeia type II apparatus (paddle-method) in 1000ml distilled water containing 0.75% w/v sodium lauryl sulfate at 75rpm for 30minutes. UV visible spectrophotometric method was selected for dissolution performance investigation at max 290 nm. In physical mixture method F5 (32.5%) and F11 (83%) and in solvent method F6 (39%) and F11 (38.5%) have showed good percentage of drug release. Tonima Akter Khan B. Pharmacy 2016-05-18T10:21:37Z 2016-05-18T10:21:37Z 2016 2016-02 Project report ID 12146039 http://hdl.handle.net/10361/5302 en BRAC University project report are protected by copyright. They may be viewed from this source for any purpose, but reproduction or distribution in any format is prohibited without written permission. 55 pages application/pdf BRAC University
institution Brac University
collection Institutional Repository
language English
topic Pharmacy
PEG6000
spellingShingle Pharmacy
PEG6000
Khan, Tonima Akter
Dissolution performance improvement of fenofibrate through secondary solid dispersion using PEG6000 and croscarmellose sodium combination
description This project report is submitted in a partial fulfillment of the requirements for the degree of Bachelor of Pharmacy, 2016
author2 Sharmin, Shahana
author_facet Sharmin, Shahana
Khan, Tonima Akter
format Project report
author Khan, Tonima Akter
author_sort Khan, Tonima Akter
title Dissolution performance improvement of fenofibrate through secondary solid dispersion using PEG6000 and croscarmellose sodium combination
title_short Dissolution performance improvement of fenofibrate through secondary solid dispersion using PEG6000 and croscarmellose sodium combination
title_full Dissolution performance improvement of fenofibrate through secondary solid dispersion using PEG6000 and croscarmellose sodium combination
title_fullStr Dissolution performance improvement of fenofibrate through secondary solid dispersion using PEG6000 and croscarmellose sodium combination
title_full_unstemmed Dissolution performance improvement of fenofibrate through secondary solid dispersion using PEG6000 and croscarmellose sodium combination
title_sort dissolution performance improvement of fenofibrate through secondary solid dispersion using peg6000 and croscarmellose sodium combination
publisher BRAC University
publishDate 2016
url http://hdl.handle.net/10361/5302
work_keys_str_mv AT khantonimaakter dissolutionperformanceimprovementoffenofibratethroughsecondarysoliddispersionusingpeg6000andcroscarmellosesodiumcombination
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