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  4. Novel pharmaceutical co-crystals of gefitinib: synthesis, dissolution, cytotoxicity, and theoretical studies
 
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Novel pharmaceutical co-crystals of gefitinib: synthesis, dissolution, cytotoxicity, and theoretical studies

Source
Crystengcomm
Date Issued
2023-03-22
Author(s)
Shaik, Althaf
Bhagwat, Pranav Umesh
Palanisamy, Parimaladevi
Chhabria, Dimple
Dubey, Pankaj
Kirubakaran, Sivapriya  
Thiruvenkatam, Vijay  
DOI
10.1039/d3ce00056g
Volume
25
Issue
17
Abstract
Gefitinib (GEF) is an ATP-competitive inhibitor used in the treatment of advanced non-small cell lung cancer. However, the pharmaceutical efficacy of this drug is currently limited due to poor aqueous solubility (2.55 μg mL<sup>−1</sup>). Therefore, we engineered three co-crystals of GEF with suitable coformers like cinnamic acid (CA), sorbic acid (SA) and resorcinol (RES). Solvent assisted grinding combined with slow evaporation of solvent resulted in three co-crystals. Structural elucidation of the crystals revealed that GEF formed a 1 : 1 co-crystal with CA (GCA), while it formed a 1 : 1 : 1 co-crystal hydrate with RES (GRES·H<inf>2</inf>O) and SA (GSA·H<inf>2</inf>O). Further, dissolution studies showed that there is an increase in the solubility of the cocrystal GCA. The synthesized co-crystals showed a comparable potency with respect to GEF in a cell viability assay. In addition, we quantified various intermolecular interactions in the co-crystals of GEF using Hirshfeld surface and 2D fingerprint plot analysis. The improvement in solubility along with the comparable efficacy of co-crystals cement the importance of pharmaceutical cocrystals in improving the physico-chemical properties of drug molecules.
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URI
https://d8.irins.org/handle/IITG2025/26851
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