| Literature DB >> 34356816 |
Mahmoud A A Ibrahim1, Alaa H M Abdelrahman1, Mohamed A M Atia2, Tarik A Mohamed3, Mahmoud F Moustafa4,5, Abdulrahim R Hakami6, Shaden A M Khalifa7, Fahad A Alhumaydhi8, Faris Alrumaihi8, Syed Hani Abidi9, Khaled S Allemailem8, Thomas Efferth10, Mahmoud E Soliman11, Paul W Paré12, Hesham R El-Seedi13,14,15, Mohamed-Elamir F Hegazy3,10.
Abstract
The coronavirus pandemic has affected more than 150 million people, while over 3.25 million people have died from the coronavirus disease 2019 (COVID-19). As there are no established therapies for COVID-19 treatment, drugs that inhibit viral replication are a promising target; specifically, the main protease (Mpro) that process CoV-encoded polyproteins serves as an Achilles heel for assembly of replication-transcription machinery as well as down-stream viral replication. In the search for potential antiviral drugs that target Mpro, a series of cembranoid diterpenes from the biologically active soft-coral genus Sarcophyton have been examined as SARS-CoV-2 Mpro inhibitors. Over 360 metabolites from the genus were screened using molecular docking calculations. Promising diterpenes were further characterized by molecular dynamics (MD) simulations based on molecular mechanics-generalized Born surface area (MM-GBSA) binding energy calculations. According to in silico calculations, five cembranoid diterpenes manifested adequate binding affinities as Mpro inhibitors with ΔGbinding < -33.0 kcal/mol. Binding energy and structural analyses of the most potent Sarcophyton inhibitor, bislatumlide A (340), was compared to darunavir, an HIV protease inhibitor that has been recently subjected to clinical-trial as an anti-COVID-19 drug. In silico analysis indicates that 340 has a higher binding affinity against Mpro than darunavir with ΔGbinding values of -43.8 and -34.8 kcal/mol, respectively throughout 100 ns MD simulations. Drug-likeness calculations revealed robust bioavailability and protein-protein interactions were identified for 340; biochemical signaling genes included ACE, MAPK14 and ESR1 as identified based on a STRING database. Pathway enrichment analysis combined with reactome mining revealed that 340 has the capability to re-modulate the p38 MAPK pathway hijacked by SARS-CoV-2 and antagonize injurious effects. These findings justify further in vivo and in vitro testing of 340 as an antiviral agent against SARS-CoV-2.Entities:
Keywords: SARS-CoV-2 main protease; cembranoid diterpenes metabolites; genus Sarcophyton; molecular docking; molecular dynamics; reactome
Year: 2021 PMID: 34356816 DOI: 10.3390/md19070391
Source DB: PubMed Journal: Mar Drugs ISSN: 1660-3397 Impact factor: 5.118