Issue 38, 2021
From the journal:

New Journal of Chemistry

Structural, QSAR, machine learning and molecular docking studies of 5-thiophen-2-yl pyrazole derivatives as potent and selective cannabinoid-1 receptor antagonists

Riadh Hanachi,a   Ridha Ben Said,*ab   Hamza Allal, ORCID logo cd   Seyfeddine Rahali,be   Mohammed A. M. Alkhalifah,f   Faisal Alresheedi,g   Bahoueddine Tangour ORCID logo e  and  Majdi Hochlaf ORCID logo *h  

* Corresponding authors

a Laboratoire de Caractérisations, Applications et Modélisations des Matériaux, Faculté des Sciences de Tunis, Université Tunis El Manar, Tunis, Tunisia

b Department of Chemistry, College of Science and Arts, Qassim University, ArRass, Saudi Arabia
E-mail: ben.said.ridha@gmail.com

c Department of Technology, Faculty of Technology, 20 August 1955 University of Skikda, P.O. Box 26, El Hadaik Road, 21000 Skikda, Algeria

d Research Unit of Environmental Chemistry and Molecular Structural (CHEMS), University of Constantine-1, 25000, Constantine, Algeria

e Research Unit of Modelization on Fundamental Sciences and Didactics. Universitéde Tunis El Manar, Tunis 2092, Tunisia

f Department of Chemistry, College of Science, Qassim University, Buraidah 51452, Saudi Arabia

g Department of Physics, College of Science, Qassim University, Buraidah 51452, Saudi Arabia

h Université Gustave Eiffel, COSYS/LISIS, 5 Bd Descartes, 77454, Champs sur Marne, France
E-mail: hochlaf@univ-mlv.fr

Abstract

We performed a structural study followed by theoretical analysis of the chemical descriptors and biological activity of a series of 5-thiophen-2-yl pyrazole derivatives as potent and selective cannabinoid-1 (CB1) receptor antagonists. The structures and molecular properties of these compounds were obtained using a DFT-D3 (B3LYP(+D3)) approach in conjunction with the 6-311G(d,p) basis set. We also derived the physicochemical properties and the binding of these derivatives interacting with the CB1 receptor. Computations show that all of them present the same molecular subunit structure, miming that of rimonabant, an efficient CB1 antagonist. The 3D structure of this subunit, important for the interaction with the receptor, is strongly influenced by long-range interactions. Moreover, we derived a QSAR equation to model the biological activity of this series. Close agreement with experimental data is found. Moreover, molecular docking studies were carried out between the most active compound and both the inactive and active states of the CB1 receptor. Results reveal high affinity between this compound and the inactive CB1 conformation, mainly governed by van der Waals forces. In conclusion, our work suggests that this compound could be a novel efficient inhibitor of CB1.

Graphical abstract: Structural, QSAR, machine learning and molecular docking studies of 5-thiophen-2-yl pyrazole derivatives as potent and selective cannabinoid-1 receptor antagonists

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Article information

DOI
https://doi.org/10.1039/D1NJ02261J
Article type
Paper
Submitted
08 May 2021
Accepted
23 Aug 2021
First published
23 Aug 2021

New J. Chem., 2021,45, 17796-17807

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Structural, QSAR, machine learning and molecular docking studies of 5-thiophen-2-yl pyrazole derivatives as potent and selective cannabinoid-1 receptor antagonists

R. Hanachi, R. Ben Said, H. Allal, S. Rahali, M. A. M. Alkhalifah, F. Alresheedi, B. Tangour and M. Hochlaf, New J. Chem., 2021, 45, 17796 DOI: 10.1039/D1NJ02261J

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