Studies on the supramolecular complex of a guanosine with beta-cyclodextrin and evaluation of its anti-proliferative activity

Prabu, S. and Samad, N.A. and Ahmad, N.A. and Jumbri, K. and Raoov, M. and Rahim, N.Y. and Samikannu, K. and Mohamad, S. (2020) Studies on the supramolecular complex of a guanosine with beta-cyclodextrin and evaluation of its anti-proliferative activity. Carbohydrate Research, 497.

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Abstract

The behavior of the inclusion behavior of guanosine (GU) with beta-cyclodextrin (β-CD) in the liquid, solid and virtual state were investigated. The absorption and fluorescence spectral were used to determine the inclusion behavior in liquid state. FT-IR, NMR, TGA, DSC, PXRD and FESEM techniques were used to investigate the inclusion behavior in solid-state, meanwhile the virtual state studies are done by molecular docking. The solid inclusion complex (GU: β-CD) was prepared by using the co-precipitation method. The binding constant (K) of (GU: β-CD) was calculated by using Benesi-Hildebrand. Besides that, the 1:1 stoichiometric ratio of inclusion complex was confirmed by using the Benesi-Hildebrand plot and Job's plot of continuous variation method. The most preferable model of GU: β-CD that suggested via molecular docking studies was in good agreement with experimental results. The inclusion complex of GU: β-CD exerted its toxicity effects towards HepG2 cell lines based on the reduced number of cell viability and lowest IC50 value compared to the GU and β-CD viability. © 2020 Elsevier Ltd

Item Type: Article
Impact Factor: cited By 6
Uncontrolled Keywords: Biomolecules; Cell culture; Molecular modeling; Precipitation (chemical), Anti-proliferative activities; Continuous variation methods; Coprecipitation method; Inclusion behavior; Inclusion complex; Solid inclusion complexes; Stoichiometric ratio; Supramolecular complexes, Cyclodextrins, beta cyclodextrin; guanosine; antineoplastic agent; beta cyclodextrin derivative; guanosine, absorption; antiproliferative activity; apoptosis; Article; association constant; cell proliferation; cell viability; controlled study; differential scanning calorimetry; drug toxicity; evaluation study; field emission scanning electron microscopy; fluorescence; Fourier transform infrared spectroscopy; Hep-G2 cell line; human; human cell; IC50; molecular docking; nuclear magnetic resonance; precipitation; priority journal; supramolecular chemistry; thermogravimetry; X ray diffraction; chemistry; conformation; drug effect, Antineoplastic Agents; beta-Cyclodextrins; Cell Proliferation; Guanosine; Hep G2 Cells; Humans; Molecular Conformation; Molecular Docking Simulation
Depositing User: Ms Sharifah Fahimah Saiyed Yeop
Date Deposited: 25 Mar 2022 02:51
Last Modified: 25 Mar 2022 02:51
URI: http://scholars.utp.edu.my/id/eprint/29784

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