Surface Solid Dispersion and Solid Dispersion of Meloxicam: Comparison and Product Development

Purpose: A comparative study was carried out between surface solid dispersion (SSD) and solid dispersion (SD) of meloxicam (MLX) to assess the solubility and dissolution enhancement approach and thereafter develop as patient friendly orodispersible tablet. Methods: Crospovidone (CPV), a hydrophilic...

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Main Authors: Mayank Chaturvedi, Manish Kumar, Kamla Pathak, Shailendra Bhatt, Vipin Saini
Format: Article
Language:English
Published: Tabriz University of Medical Sciences 2017-12-01
Series:Advanced Pharmaceutical Bulletin
Subjects:
Online Access:http://apb.tbzmed.ac.ir/PDF/apb-7-569.pdf
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spelling doaj-a2dab52ea35a4b55a17e0ed04d584ecb2020-11-24T20:42:16ZengTabriz University of Medical Sciences Advanced Pharmaceutical Bulletin2228-58812251-73082017-12-017456957710.15171/apb.2017.068APB_19378_20170512133116Surface Solid Dispersion and Solid Dispersion of Meloxicam: Comparison and Product DevelopmentMayank Chaturvedi0Manish Kumar1Kamla Pathak2Shailendra Bhatt3Vipin Saini4Department of Pharmaceutics, Rajiv Academy for Pharmacy, Chattikkara, Mathura, India.Department of Pharmaceutics, M M College of Pharmacy, Maharishi Markandeshwar University,Mullana, Ambala-133207, Haryana, India.Department of Pharmaceutics, Pharmacy College Saifai, Uttar Pradesh University of Medical sciences, Saifai, Etawah , 206130, Uttar Pradesh, India.Department of Pharmaceutics, M M College of Pharmacy, Maharishi Markandeshwar University,Mullana, Ambala-133207, Haryana, India.Department of Pharmaceutics, M M College of Pharmacy, Maharishi Markandeshwar University,Mullana, Ambala-133207, Haryana, India.Purpose: A comparative study was carried out between surface solid dispersion (SSD) and solid dispersion (SD) of meloxicam (MLX) to assess the solubility and dissolution enhancement approach and thereafter develop as patient friendly orodispersible tablet. Methods: Crospovidone (CPV), a hydrophilic carrier was selected for SSD preparation on the basis of 89% in- vitro MLX adsorption, 19% hydration capacity and high swelling index. SD on the other hand was made with PEG4000. Both were prepared by co-grinding and solvent evaporation method using drug: carrier ratios of 1:1, 1:4, and 1:8. Formulation SSDS3 (MLX: CPV in 1:8 ratio) made by solvent evaporation method showed t50% of 28 min and 80.9% DE50min which was higher in comparison to the corresponding solid dispersion, SDS3 (t50% of 35min and 76.4% DE50min). Both SSDS3 and SDS3 were developed as orodispersible tablets and evaluated. Results: Tablet formulation F3 made with SSD3 with a disintegration time of 11 secs, by wetting time= 6 sec, high water absorption of 78%by wt and cumulative drug release of 97% proved to be superior than the tablet made with SD3. Conclusion: Conclusively, the SSD of meloxicam has the potential to be developed as fast acing formulation that can ensure almost complete release of drug.http://apb.tbzmed.ac.ir/PDF/apb-7-569.pdfSurface solid dispersionSolid dispersionDissolutionOrodispersible tablet
collection DOAJ
language English
format Article
sources DOAJ
author Mayank Chaturvedi
Manish Kumar
Kamla Pathak
Shailendra Bhatt
Vipin Saini
spellingShingle Mayank Chaturvedi
Manish Kumar
Kamla Pathak
Shailendra Bhatt
Vipin Saini
Surface Solid Dispersion and Solid Dispersion of Meloxicam: Comparison and Product Development
Advanced Pharmaceutical Bulletin
Surface solid dispersion
Solid dispersion
Dissolution
Orodispersible tablet
author_facet Mayank Chaturvedi
Manish Kumar
Kamla Pathak
Shailendra Bhatt
Vipin Saini
author_sort Mayank Chaturvedi
title Surface Solid Dispersion and Solid Dispersion of Meloxicam: Comparison and Product Development
title_short Surface Solid Dispersion and Solid Dispersion of Meloxicam: Comparison and Product Development
title_full Surface Solid Dispersion and Solid Dispersion of Meloxicam: Comparison and Product Development
title_fullStr Surface Solid Dispersion and Solid Dispersion of Meloxicam: Comparison and Product Development
title_full_unstemmed Surface Solid Dispersion and Solid Dispersion of Meloxicam: Comparison and Product Development
title_sort surface solid dispersion and solid dispersion of meloxicam: comparison and product development
publisher Tabriz University of Medical Sciences
series Advanced Pharmaceutical Bulletin
issn 2228-5881
2251-7308
publishDate 2017-12-01
description Purpose: A comparative study was carried out between surface solid dispersion (SSD) and solid dispersion (SD) of meloxicam (MLX) to assess the solubility and dissolution enhancement approach and thereafter develop as patient friendly orodispersible tablet. Methods: Crospovidone (CPV), a hydrophilic carrier was selected for SSD preparation on the basis of 89% in- vitro MLX adsorption, 19% hydration capacity and high swelling index. SD on the other hand was made with PEG4000. Both were prepared by co-grinding and solvent evaporation method using drug: carrier ratios of 1:1, 1:4, and 1:8. Formulation SSDS3 (MLX: CPV in 1:8 ratio) made by solvent evaporation method showed t50% of 28 min and 80.9% DE50min which was higher in comparison to the corresponding solid dispersion, SDS3 (t50% of 35min and 76.4% DE50min). Both SSDS3 and SDS3 were developed as orodispersible tablets and evaluated. Results: Tablet formulation F3 made with SSD3 with a disintegration time of 11 secs, by wetting time= 6 sec, high water absorption of 78%by wt and cumulative drug release of 97% proved to be superior than the tablet made with SD3. Conclusion: Conclusively, the SSD of meloxicam has the potential to be developed as fast acing formulation that can ensure almost complete release of drug.
topic Surface solid dispersion
Solid dispersion
Dissolution
Orodispersible tablet
url http://apb.tbzmed.ac.ir/PDF/apb-7-569.pdf
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