Relevancy of Nizatidine’s Release from Floating Tablets with Viscosity of Various Cellulose Ethers
Nizatidine is a gastroprotective drug with a short biological half-life and narrow absorption window. This study aimed at developing floating tablets of nizatidine using various HPMC viscosity grades, namely K4M, E4M, K15 and K200M. Directly compressed tablets revealed an excellent uniformity in har...
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doaj-13780c91534b476e9e951611a9df8e9d2021-04-08T23:00:03ZengMDPI AGSci2413-41552021-04-013222210.3390/sci3020022Relevancy of Nizatidine’s Release from Floating Tablets with Viscosity of Various Cellulose EthersYasser Shahzad0Namra Ibrar1Talib Hussain2Abid Mehmood Yousaf3Ikram Ullah Khan4Syed A. A. Rizvi5Department of Pharmacy, COMSATS University Islamabad, Lahore 54000, PakistanFaculty of Pharmacy, University of Central Punjab, Lahore 54000, PakistanDepartment of Pharmacy, COMSATS University Islamabad, Lahore 54000, PakistanDepartment of Pharmacy, COMSATS University Islamabad, Lahore 54000, PakistanDepartment of Pharmaceutics, Faculty of Pharmaceutical Sciences, Government College University, Faisalabad 38000, PakistanDepartment of Pharmaceutical Sciences, Hampton University School of Pharmacy, Hampton, VA 23668, USANizatidine is a gastroprotective drug with a short biological half-life and narrow absorption window. This study aimed at developing floating tablets of nizatidine using various HPMC viscosity grades, namely K4M, E4M, K15 and K200M. Directly compressed tablets revealed an excellent uniformity in hardness, thickness and weight and nizatidine was evenly distributed within the matrix floating tablets. Buoyancy study revealed floating lag time as low as 18–38 s, and tablets remain buoyant for upto 24 h. However, the later depended upon viscosity grade of HPMC and that the higher the viscosity, the less was the total floating time. In vitro dissolution indicated viscosity dependent nizatidine release from the floating tablets. HPMC K4M and E4M based floating tablets released almost 100% drug in 12 h, whilst higher viscosity polymers such as K15 and K200M only released 81.88% and 75.81% drug, respectively. The drug release followed non-Fickian diffusion from tablets formulated with K4M, K15 and K200M, whilst super case II transport was observed with E4M based tablets. More interestingly, K4M and E4M polymers have similar viscosity yet exhibited different drug release mechanism. This was attributed to the difference in degree of substitution of methoxyl- and hydroxypropoxyl- groups on polymer backbone.https://www.mdpi.com/2413-4155/3/2/22buoyancydissolutionfloating tabletsHPMCnizatidinesubstitution level |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Yasser Shahzad Namra Ibrar Talib Hussain Abid Mehmood Yousaf Ikram Ullah Khan Syed A. A. Rizvi |
spellingShingle |
Yasser Shahzad Namra Ibrar Talib Hussain Abid Mehmood Yousaf Ikram Ullah Khan Syed A. A. Rizvi Relevancy of Nizatidine’s Release from Floating Tablets with Viscosity of Various Cellulose Ethers Sci buoyancy dissolution floating tablets HPMC nizatidine substitution level |
author_facet |
Yasser Shahzad Namra Ibrar Talib Hussain Abid Mehmood Yousaf Ikram Ullah Khan Syed A. A. Rizvi |
author_sort |
Yasser Shahzad |
title |
Relevancy of Nizatidine’s Release from Floating Tablets with Viscosity of Various Cellulose Ethers |
title_short |
Relevancy of Nizatidine’s Release from Floating Tablets with Viscosity of Various Cellulose Ethers |
title_full |
Relevancy of Nizatidine’s Release from Floating Tablets with Viscosity of Various Cellulose Ethers |
title_fullStr |
Relevancy of Nizatidine’s Release from Floating Tablets with Viscosity of Various Cellulose Ethers |
title_full_unstemmed |
Relevancy of Nizatidine’s Release from Floating Tablets with Viscosity of Various Cellulose Ethers |
title_sort |
relevancy of nizatidine’s release from floating tablets with viscosity of various cellulose ethers |
publisher |
MDPI AG |
series |
Sci |
issn |
2413-4155 |
publishDate |
2021-04-01 |
description |
Nizatidine is a gastroprotective drug with a short biological half-life and narrow absorption window. This study aimed at developing floating tablets of nizatidine using various HPMC viscosity grades, namely K4M, E4M, K15 and K200M. Directly compressed tablets revealed an excellent uniformity in hardness, thickness and weight and nizatidine was evenly distributed within the matrix floating tablets. Buoyancy study revealed floating lag time as low as 18–38 s, and tablets remain buoyant for upto 24 h. However, the later depended upon viscosity grade of HPMC and that the higher the viscosity, the less was the total floating time. In vitro dissolution indicated viscosity dependent nizatidine release from the floating tablets. HPMC K4M and E4M based floating tablets released almost 100% drug in 12 h, whilst higher viscosity polymers such as K15 and K200M only released 81.88% and 75.81% drug, respectively. The drug release followed non-Fickian diffusion from tablets formulated with K4M, K15 and K200M, whilst super case II transport was observed with E4M based tablets. More interestingly, K4M and E4M polymers have similar viscosity yet exhibited different drug release mechanism. This was attributed to the difference in degree of substitution of methoxyl- and hydroxypropoxyl- groups on polymer backbone. |
topic |
buoyancy dissolution floating tablets HPMC nizatidine substitution level |
url |
https://www.mdpi.com/2413-4155/3/2/22 |
work_keys_str_mv |
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