Solubility enhancement of mefenamic acid by inclusion complex with β-cyclodextrin: in silico modelling, formulation, characterisation, and in vitro studies

Dounia Sid; Milad Baitiche; Zineb Elbahri; Ferhat Djerboua; Mokhtar Boutahala; Zouhair Bouaziz; Marc Le Borgne

doi:10.1080/14756366.2020.1869225

Journal of Enzyme Inhibition and Medicinal Chemistry (Jan 2021)

Solubility enhancement of mefenamic acid by inclusion complex with β-cyclodextrin: in silico modelling, formulation, characterisation, and in vitro studies

Dounia Sid,
Milad Baitiche,
Zineb Elbahri,
Ferhat Djerboua,
Mokhtar Boutahala,
Zouhair Bouaziz,
Marc Le Borgne

Affiliations

Dounia Sid: Département de Génie des Procédés, Faculté de Technologie, Laboratoire de Préparation, Modification et Applications des Matériaux Polymériques Multiphasiques, Université Ferhat Abbas Sétif-1
Milad Baitiche: Département de Génie des Procédés, Faculté de Technologie, Laboratoire de Préparation, Modification et Applications des Matériaux Polymériques Multiphasiques, Université Ferhat Abbas Sétif-1
Zineb Elbahri: Faculty of Exact Sciences, Laboratory of Materials and Catalysis, Djillali Liabès University of Sidi Bel Abbès
Ferhat Djerboua: Département de Génie des Procédés, Faculté de Technologie, Laboratoire de Préparation, Modification et Applications des Matériaux Polymériques Multiphasiques, Université Ferhat Abbas Sétif-1
Mokhtar Boutahala: Département de Génie des Procédés, Faculté de Technologie, Laboratoire de Génie des Procédés Chimiques, Université Ferhat Abbas Sétif-1
Zouhair Bouaziz: EA 4446 Bioactive Molecules and Medicinal Chemistry, SFR Santé Lyon-Est CNRS UMS3453 – INSERM US7, Université Claude Bernard Lyon 1, Univ Lyon
Marc Le Borgne: EA 4446 Bioactive Molecules and Medicinal Chemistry, SFR Santé Lyon-Est CNRS UMS3453 – INSERM US7, Université Claude Bernard Lyon 1, Univ Lyon

DOI: https://doi.org/10.1080/14756366.2020.1869225
Journal volume & issue: Vol. 36, no. 1
pp. 605 – 617

Abstract

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The aim of this study was to prepare and characterise inclusion complexes of a low water-soluble drug, mefenamic acid (MA), with β-cyclodextrin (β-CD). First, the phase solubility diagram of MA in β-CD was drawn from 0 to 21 × 10−3 M of β-CD concentration. A job’s plot experiment was used to determine the stoichiometry of the MA:β-CD complex (2:1). The stability of this complex was confirmed by molecular modelling simulation. Three methods, namely solvent co-evaporation (CE), kneading (KN), and physical mixture (PM), were used to prepare the (2:1) MA:β-CD complexes. All complexes were fully characterised. The drug dissolution tests were established in simulated liquid gastric and the MA water solubility at pH 1.2 from complexes was significantly improved. The mechanism of MA released from the β-CD complexes was illustrated through a mathematical treatment. Finally, two in vitro experiments confirmed the interest to use a (2:1) MA:β-CD complex.

Published in Journal of Enzyme Inhibition and Medicinal Chemistry

ISSN: 1475-6366 (Print); 1475-6374 (Online)
Publisher: Taylor & Francis Group
Country of publisher: United Kingdom
LCC subjects: Medicine: Therapeutics. Pharmacology
Website: https://www.tandfonline.com/journals/ienz

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