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Multispectral and Molecular Docking Studies Reveal Potential Effectiveness of Antidepressant Fluoxetine by Forming π-Acceptor Complexes

by Alsanie, Walaa F. , Alamri, Abdulhakeem S. , Alyami, Hussain , Raafat, Bassem M. , Habeeballah, Hamza , Felimban, Raed I. , Alhomrani, Majid , Alamri, Abdulwahab , Refat, Moamen S. , Alkhatabi, Heba A. , Gaber, Ahmed , Shakya, Sonam , Alhabeeb, Abdulhameed Abdullah

in Amino acids / Antidepressants / Care and treatment / Density functionals / Depression, Mental / Dopamine / Fluorine / Fluoxetine / fluoxetine HCl / Hydrogen / Ligands / major depressive disorder / molecular docking / Pharmaceuticals / Serotonin / spectroscopy / Testing / π-acceptor complexes

2022

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Multispectral and Molecular Docking Studies Reveal Potential Effectiveness of Antidepressant Fluoxetine by Forming π-Acceptor Complexes

2022

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Multispectral and Molecular Docking Studies Reveal Potential Effectiveness of Antidepressant Fluoxetine by Forming π-Acceptor Complexes

2022

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Journal Article

Multispectral and Molecular Docking Studies Reveal Potential Effectiveness of Antidepressant Fluoxetine by Forming π-Acceptor Complexes

Alsanie, Walaa F.,

Alamri, Abdulhakeem S.,

Alyami, Hussain,

Raafat, Bassem M.,

Habeeballah, Hamza,

Felimban, Raed I.,

Alhomrani, Majid,

Alamri, Abdulwahab,

Refat, Moamen S.,

Alkhatabi, Heba A.,

Gaber, Ahmed,

Shakya, Sonam,

Alhabeeb, Abdulhameed Abdullah

2022

Overview

Poor mood, lack of pleasure, reduced focus, remorse, unpleasant thoughts, and sleep difficulties are all symptoms of depression. The only approved treatment for children and adolescents with major depressive disorder (MDD) is fluoxetine hydrochloride (FXN), a serotonin selective reuptake inhibitor antidepressant. MDD is the most common cause of disability worldwide. In the present research, picric acid (PA); dinitrobenzene; p-nitro benzoic acid; 2,6-dichloroquinone-4-chloroimide; 2,6-dibromoquinone-4-chloroimide; and 7,7′,8,8′-tetracyanoquinodimethane were used to make 1:1 FXN charge-transfer compounds in solid and liquid forms. The isolated complexes were then characterized by elemental analysis, conductivity, infrared, Raman, and 1H-NMR spectra, thermogravimetric analysis, scanning electron microscopy, and X-ray powder diffraction. Additionally, a molecular docking investigation was conducted on the donor moiety using FXN alone and the resulting charge transfer complex [(FXN)(PA)] as an acceptor to examine the interactions against two protein receptors (serotonin or dopamine). Interestingly, the [(FXN)(PA)] complex binds to both serotonin and dopamine more effectively than the FXN drug alone. Furthermore, [(FXN)(PA)]–serotonin had a greater binding energy than [FXN]–serotonin. Theoretical data were also generated by density functional theory simulations, which aided the molecular geometry investigation and could be beneficial to researchers in the future.

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Publisher

MDPI AG,MDPI

Subject

Amino acids

/ Antidepressants

/ Care and treatment

/ Density functionals

/ Depression, Mental

/ Dopamine

/ Fluorine