Spectroscopic characterization and pharmacokinetic evaluation of amorphous solid dispersions of glibenclamide for bioavailability enhancement in Wistar rats-Reference-Cited by-同舟云学术

Spectroscopic characterization and pharmacokinetic evaluation of amorphous solid dispersions of glibenclamide for bioavailability enhancement in Wistar rats

Published:2024-05-30 Issue:8 Volume:38 Page:
ISSN:0269-3879
Container-title:Biomedical Chromatography
language:en
Short-container-title:Biomedical Chromatography

Author:

Mir Khalid Bashir¹^ORCID,Abrol Vidushi²,Singh Nasseb³⁴,Khan Nisar A.⁵,Dar Alamgir A.⁶^ORCID,Alahmadi Tahani Awad⁷,Ansari Mohammad Javed⁸⁹

Affiliation:

1. School of Medical and Allied Sciences K. R. Mangalam University Gurgaon Haryana India

2. Fermentation and Microbial Biotechnology Division CSIR‐Indian Institute of Integrative Medicine Jammu Tawi India

3. Synthetic Organic Chemistry Laboratory, Faculty of Sciences Shri Mata Vaishno Devi University Katra India

4. Department of Chemistry Govt. Gandhi Memorial Science College Jammu (a Constituent College of Cluster University of Jammu) Jammu and Kashmir India

5. Department of Pharmaceutical Sciences University of Kashmir Srinagar Jammu and Kashmir India

6. Research Centre for Residue and Quality Analysis Sher‐e‐Kashmir University of Agricultural Sciences & Technology of Kashmir, Shalimar Jammu and Kashmir Srinagar India

7. Department of Pediatrics, College of Medicine and King Khalid University Hospital King Saud University Riyadh Saudi Arabia

8. Department of Botany Hindu College Moradabad (Mahatma Jyotiba Phule Rohilkhand University Bareilly) Bareilly Uttar Pradesh India

9. College of Food and Agriculture Sciences King Saud University Riyadh Saudi Arabia

Abstract

AbstractOral bioavailability of glibenclamide (Glb) was appreciably improved by the formation of an amorphous solid dispersion with Poloxamer‐188 (P‐188). Poloxamer‐188 substantially enhanced the solubility and thereby the dissolution rate of the biopharmaceutics classification system (BCS) class II drug Glb and simultaneously exhibited a better stabilizing effect of the amorphous solid dispersion prepared by the solvent evaporation method. The physical state of the dispersed Glb in the polymeric matrix was characterized by differential scanning calorimetry, X‐ray diffraction, scanning electron microscope and Fourier transform infrared studies. In vitro drug release in buffer (pH 7.2) revealed that the amorphous solid dispersion at a Glb–P‐188 ratio of 1:6 (SDE4) improved the dissolution of Glb by 90% within 3 h. A pharmacokinetic study of the solid dispersion formulation SDE4 in Wistar rats showed that the oral bioavailability of the drug was greatly increased as compared with the market tablet formulation, Daonil®. The formulation SDE4 resulted in an AUC0–24h ~2‐fold higher. The SDE4 formulation was found to be stable during the study period of 6 months.

Funder

King Saud University

Publisher

Wiley

Reference41 articles.

1. Chromatography: An important tool for drug discovery

2. A systematic and robust assessment of hot-melt extrusion-based amorphous solid dispersions: Theoretical prediction to practical implementation

3. Physicochemical characterization of nimodipine–polyethylene glycol solid dispersion systems

4. Preparation and evaluation of glibenclamide-polyglycolized glycerides solid dispersions with silicon dioxide by spray drying technique

5. Development of Diclofenac Sodium Controlled Release Solid Dispersions by Spray Drying Using Optimization Strategy I. Powder Formulation