Physicochemical Characterization, Molecular Docking, and In Vitro Dissolution of GlimepirideCaptisol Inclusion Complexes

Pal, Arpita; Roy, Sudeep; Kumar, Akhil; Mahmood, Syed; Khodapanah, Nasrin; Thomas, Sabu; Agatemor, Christian; Ghosal, Kajal

Physicochemical Characterization, Molecular Docking, and In Vitro Dissolution of GlimepirideCaptisol Inclusion Complexes

dc.contributor.author	Pal, Arpita	cs
dc.contributor.author	Roy, Sudeep	cs
dc.contributor.author	Kumar, Akhil	cs
dc.contributor.author	Mahmood, Syed	cs
dc.contributor.author	Khodapanah, Nasrin	cs
dc.contributor.author	Thomas, Sabu	cs
dc.contributor.author	Agatemor, Christian	cs
dc.contributor.author	Ghosal, Kajal	cs
dc.coverage.issue	32	cs
dc.coverage.volume	5	cs
dc.date.issued	2020-08-01	cs
dc.description.abstract	This present study investigated the effect of Captisol, a chemically modified cyclodextrin, on the in vitro dissolution of glimepiride. We prepared glimepirideCaptisol complexes of different mass ratios (1:1, 1:2, and 1:3 w/w) by a physical mixing or freeze-drying technique, and found that complexation with Captisol enhanced the water solubility of glimepiride. Molecular docking and dynamic simulation predicted complex formation; at the same time, Fourier transform infrared spectroscopy, differential scanning calorimetry, powder X-ray diffractometry, and scanning electron microscope indicated molecular interactions that support complexation. We also found that an inclusion complex was better than a physical mixture in enhancing the complexation of glimepiride with Captisol and enhancing water solubility. Phase solubility study of the glimepirideCaptisol complex showed an AL-type profile, implying the formation of a 1:1 inclusion complex. The study also revealed that pH influenced the stability of the complex because the stability constant of the glimepirideCaptisol complex was higher in distilled water of pH 6.0 than in phosphate buffer of pH 7.2.	en
dc.format	text	cs
dc.format.extent	19968-19977	cs
dc.format.mimetype	application/pdf	cs
dc.identifier.citation	ACS OMEGA. 2020, vol. 5, issue 32, p. 19968-19977.	en
dc.identifier.doi	10.1021/acsomega.0c01228	cs
dc.identifier.issn	2470-1343	cs
dc.identifier.orcid	0000-0002-7825-0152	cs
dc.identifier.other	165567	cs
dc.identifier.scopus	000000278250152	cs
dc.identifier.uri	http://hdl.handle.net/11012/196516
dc.language.iso	en	cs
dc.publisher	American Chemical Society	cs
dc.relation.ispartof	ACS OMEGA	cs
dc.relation.uri	https://pubs.acs.org/doi/10.1021/acsomega.0c01228	cs
dc.rights	(C) American Chemical Society	cs
dc.rights.access	openAccess	cs
dc.rights.sherpa	http://www.sherpa.ac.uk/romeo/issn/2470-1343/	cs
dc.subject	Glimepiride	en
dc.subject	Captisol	en
dc.subject	molecular docking	en
dc.subject	molecular simulation	en
dc.title	Physicochemical Characterization, Molecular Docking, and In Vitro Dissolution of GlimepirideCaptisol Inclusion Complexes	en
dc.type.driver	article	en
dc.type.status	Peer-reviewed	en
dc.type.version	publishedVersion	en
sync.item.dbid	VAV-165567	en
sync.item.dbtype	VAV	en
sync.item.insts	2025.02.03 15:39:46	en
sync.item.modts	2025.01.17 16:34:38	en
thesis.grantor	Vysoké učení technické v Brně. Fakulta elektrotechniky a komunikačních technologií. Ústav biomedicínského inženýrství	cs

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