β-Blockers bearing hydroxyethylamine and hydroxyethylene as potential SARS-CoV-2 Mpro inhibitors: rational based design, in silico, in vitro, and SAR studies for lead optimization

Mohammed I. A. Hamed; Khaled M. Darwish; Raya Soltane; Amani Chrouda; Ahmed Mostafa; Noura M. Abo Shama; Sameh S. Elhady; Hamada S. Abulkhair; Ahmed E. Khodir; Ayman Abo Elmaaty; Ahmed A. Al-karmalawy

doi:10.1039/D1RA04820A

β-Blockers bearing hydroxyethylamine and hydroxyethylene as potential SARS-CoV-2 Mpro inhibitors: rational based design, in silico, in vitro, and SAR studies for lead optimization†

Mohammed I. A. Hamed,‡^a Khaled M. Darwish,‡^b Raya Soltane,‡^cd Amani Chrouda,^efg Ahmed Mostafa,

^h Noura M. Abo Shama,^h Sameh S. Elhady,

ⁱ Hamada S. Abulkhair,

^jk Ahmed E. Khodir,^l Ayman Abo Elmaaty*^m and Ahmed A. Al-karmalawy

*^k

Author affiliations

* Corresponding authors

^a Department of Organic and Medicinal Chemistry, Faculty of Pharmacy, Fayoum University, Fayoum 63514, Egypt
E-mail: mia06@fayoum.edu.eg

^b Department of Medicinal Chemistry, Faculty of Pharmacy, Suez Canal University, Ismailia 41522, Egypt
E-mail: khaled_darwish@pharm.suez.edu.eg

^c Department of Basic Sciences, Adham University College, Umm Al-Qura University, Saudi Arabia
E-mail: rasoltan@uqu.edu.sa

^d Faculty of Sciences, Tunis El Manar University, Tunisia

^e Department of Chemistry, College of Science Al-Zulfi, Majmaah University, Al-Majmaah 11952, Saudi Arabia
E-mail: amain.c@mu.edu.sa

^f Laboratory of Interfaces and Advanced Materials, Faculty of Sciences, Monastir University, Monastir 5000, Tunisia

^g Institute of Analytical Sciences, UMR CNRS-UCBL-ENS 5280, 5 Rue la Doua, 69100 Villeurbanne, France

^h Center of Scientific Excellence for Influenza Viruses, National Research Centre, Dokki, Cairo, Egypt
E-mail: ahmed_elsayed@daad-alumni.de, noura.mahrous1995@gmail.com

ⁱ Department of Natural Products, Faculty of Pharmacy, King Abdulaziz University, Jeddah 21589, Saudi Arabia
E-mail: ssahmed@kau.edu.sa

^j Department of Pharmaceutical Organic Chemistry, Faculty of Pharmacy (Boys), Al-Azhar University, Nasr City 11884, Cairo, Egypt
E-mail: hamadaorganic@azhar.edu.eg

^k Department of Pharmaceutical Chemistry, Faculty of Pharmacy, Horus University-Egypt, New Damietta 34518, Egypt
E-mail: akarmalawy@horus.edu.eg

^l Department of Pharmacology, Faculty of Pharmacy, Horus University-Egypt, New Damietta, Egypt
E-mail: akhodir@horus.edu.eg

^m Department of Medicinal Chemistry, Faculty of Pharmacy, Port Said University, Port Said 42526, Egypt
E-mail: ayman.mohamed@pharm.psu.edu.eg

Abstract

The global COVID-19 pandemic became more threatening especially after the introduction of the second and third waves with the current large expectations for a fourth one as well. This urged scientists to rapidly develop a new effective therapy to combat SARS-CoV-2. Based on the structures of β-adrenergic blockers having the same hydroxyethylamine and hydroxyethylene moieties present in the HIV-1 protease inhibitors which were found previously to inhibit the replication of SARS-CoV, we suggested that they may decrease the SARS-CoV-2 entry into the host cell through their ability to decrease the activity of RAAS and ACE2 as well. Herein, molecular docking of twenty FDA-approved β-blockers was performed targeting SARS-CoV-2 Mpro. Results showed promising inhibitory activities especially for Carvedilol (CAR) and Nebivolol (NEB) members. Moreover, these two drugs together with Bisoprolol (BIS) as an example from the lower active ones were subjected to molecular dynamics simulations at 100 ns. Great stability across the whole 100 ns timeframe was observed for the top docked ligands, CAR and NEB, over BIS. Conformational analysis of the examined drugs and hydrogen bond investigation with the pocket's crucial residues confirm the great affinity and confinement of CAR and NEB within the Mpro binding site. Moreover, the binding-free energy analysis and residue-wise contribution analysis highlight the nature of ligand–protein interaction and provide guidance for lead development and optimization. Furthermore, the examined three drugs were tested for their in vitro inhibitory activities towards SARS-CoV-2. It is worth mentioning that NEB achieved the most potential anti-SARS-CoV-2 activity with an IC₅₀ value of 0.030 μg ml⁻¹. Besides, CAR was found to have a promising inhibitory activity with an IC₅₀ of 0.350 μg ml⁻¹. Also, the IC₅₀ value of BIS was found to be as low as 15.917 μg ml⁻¹. Finally, the SARS-CoV-2 Mpro assay was performed to evaluate and confirm the inhibitory effects of the tested compounds (BIS, CAR, and NEB) towards the SARS-CoV-2 Mpro enzyme. The obtained results showed very promising SARS-CoV-2 Mpro inhibitory activities of BIS, CAR, and NEB (IC₅₀ = 118.50, 204.60, and 60.20 μg ml⁻¹, respectively) compared to lopinavir (IC₅₀ = 73.68 μg ml⁻¹) as a reference standard.

RSC Advances

β-Blockers bearing hydroxyethylamine and hydroxyethylene as potential SARS-CoV-2 Mpro inhibitors: rational based design, in silico, in vitro, and SAR studies for lead optimization†

Abstract

Supplementary files

Article information

Download Citation

Permissions

β-Blockers bearing hydroxyethylamine and hydroxyethylene as potential SARS-CoV-2 Mpro inhibitors: rational based design, in silico, in vitro, and SAR studies for lead optimization

Social activity

Search articles by author

Spotlight

Advertisements