The Impact of Amorphisation and Spheronization Techniques on the Improved in Vitro & in Vivo Performance of Glimepiride Tablets

The Impact of Amorphisation and Spheronization Techniques on the Improved in Vitro & in Vivo Performance of Glimepiride Tablets

Purpose: Triple solid dispersion adsorbates (TSDads) and spherical agglomerates (SA) present new techniques that extensively enhance dissolution of poorly soluble drugs. The aim of the present study is to hasten the onset of hypoglycemic effect of glimepiride through enhancing its rate of release fr...

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Main Authors: Rana Refaat Makar, Randa Latif, Ehab Ahmed Hosni, Omaima Naim El Gazayerly
Format: Article
Language:English
Published: Tabriz University of Medical Sciences 2017-12-01
Series:Advanced Pharmaceutical Bulletin
Subjects:
Dissolution
Pharmacodynamic study
Blood glucose level
Matrix tablets
Spherical agglomeration
Triple solid dispersion adsorbate
Online Access:http://apb.tbzmed.ac.ir/PDF/apb-7-557.pdf
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spelling doaj-4b3f52f1bb1d492f9caa43ad52ef7f9b2020-11-24T21:16:58ZengTabriz University of Medical Sciences Advanced Pharmaceutical Bulletin2228-58812251-73082017-12-017455756710.15171/apb.2017.067APB_19255_20170401000756The Impact of Amorphisation and Spheronization Techniques on the Improved in Vitro & in Vivo Performance of Glimepiride TabletsRana Refaat Makar0Randa Latif1Ehab Ahmed Hosni2Omaima Naim El Gazayerly3Faculty of Pharmacy, Ahram Canadian University, Egypt.Faculty of Pharmacy, Department of Pharmaceutics, Cairo University, Cairo, Egypt.Faculty of Pharmacy, Russian University, Egypt.Faculty of Pharmacy, Department of Pharmaceutics, Cairo University, Cairo, Egypt.Purpose: Triple solid dispersion adsorbates (TSDads) and spherical agglomerates (SA) present new techniques that extensively enhance dissolution of poorly soluble drugs. The aim of the present study is to hasten the onset of hypoglycemic effect of glimepiride through enhancing its rate of release from tablet formulation prepared from either technique. Methods: Drug release from TSDads or SA tablets with different added excipients was explored. Scanning electron microscopy (SEM) and effect of compression on dissolution were illustrated. Pharmacodynamic evaluation was performed on optimized tablets. Results: TSDads & SA tablets with Cross Povidone showed least disintegration times of 1.48 and 0.5 min. respectively. Kinetics of drug release recorded least half-lives (54.13 and 59.83min for both techniques respectively). Cross section in tablets displayed an organized interconnected matrix under SEM, accounting for the rapid access of dissolution media to the tablet core. Components of tablets filled into capsules showed a similar release profile to that of tablets after compression as indicated by similarity factor. The onset time of maximum reduction in blood glucose in male albino rabbits was hastened to 2h instead of 3h for commercial tablets. Conclusion: After optimization of tablet excipients that interacted differently with respect to their effect on drug release, we could conclude that both amorphisation and spheronization were equally successful in promoting in vitro dissolution enhancement as well as providing a more rapid onset time for drug action in vivo.http://apb.tbzmed.ac.ir/PDF/apb-7-557.pdfDissolutionPharmacodynamic studyBlood glucose levelMatrix tabletsSpherical agglomerationTriple solid dispersion adsorbate
collection DOAJ
language English
format Article
sources DOAJ
author Rana Refaat Makar
Randa Latif
Ehab Ahmed Hosni
Omaima Naim El Gazayerly
spellingShingle Rana Refaat Makar
Randa Latif
Ehab Ahmed Hosni
Omaima Naim El Gazayerly
The Impact of Amorphisation and Spheronization Techniques on the Improved in Vitro & in Vivo Performance of Glimepiride Tablets
Advanced Pharmaceutical Bulletin
Dissolution
Pharmacodynamic study
Blood glucose level
Matrix tablets
Spherical agglomeration
Triple solid dispersion adsorbate
author_facet Rana Refaat Makar
Randa Latif
Ehab Ahmed Hosni
Omaima Naim El Gazayerly
author_sort Rana Refaat Makar
title The Impact of Amorphisation and Spheronization Techniques on the Improved in Vitro & in Vivo Performance of Glimepiride Tablets
title_short The Impact of Amorphisation and Spheronization Techniques on the Improved in Vitro & in Vivo Performance of Glimepiride Tablets
title_full The Impact of Amorphisation and Spheronization Techniques on the Improved in Vitro & in Vivo Performance of Glimepiride Tablets
title_fullStr The Impact of Amorphisation and Spheronization Techniques on the Improved in Vitro & in Vivo Performance of Glimepiride Tablets
title_full_unstemmed The Impact of Amorphisation and Spheronization Techniques on the Improved in Vitro & in Vivo Performance of Glimepiride Tablets
title_sort impact of amorphisation and spheronization techniques on the improved in vitro & in vivo performance of glimepiride tablets
publisher Tabriz University of Medical Sciences
series Advanced Pharmaceutical Bulletin
issn 2228-5881
2251-7308
publishDate 2017-12-01
description Purpose: Triple solid dispersion adsorbates (TSDads) and spherical agglomerates (SA) present new techniques that extensively enhance dissolution of poorly soluble drugs. The aim of the present study is to hasten the onset of hypoglycemic effect of glimepiride through enhancing its rate of release from tablet formulation prepared from either technique. Methods: Drug release from TSDads or SA tablets with different added excipients was explored. Scanning electron microscopy (SEM) and effect of compression on dissolution were illustrated. Pharmacodynamic evaluation was performed on optimized tablets. Results: TSDads & SA tablets with Cross Povidone showed least disintegration times of 1.48 and 0.5 min. respectively. Kinetics of drug release recorded least half-lives (54.13 and 59.83min for both techniques respectively). Cross section in tablets displayed an organized interconnected matrix under SEM, accounting for the rapid access of dissolution media to the tablet core. Components of tablets filled into capsules showed a similar release profile to that of tablets after compression as indicated by similarity factor. The onset time of maximum reduction in blood glucose in male albino rabbits was hastened to 2h instead of 3h for commercial tablets. Conclusion: After optimization of tablet excipients that interacted differently with respect to their effect on drug release, we could conclude that both amorphisation and spheronization were equally successful in promoting in vitro dissolution enhancement as well as providing a more rapid onset time for drug action in vivo.
topic Dissolution
Pharmacodynamic study
Blood glucose level
Matrix tablets
Spherical agglomeration
Triple solid dispersion adsorbate
url http://apb.tbzmed.ac.ir/PDF/apb-7-557.pdf
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