In search of SARS CoV-2 replication inhibitors: Virtual screening, molecular dynamics simulations and ADMET analysis
| Autor: | Normi D. Gajjar, Tejas M. Dhameliya, Prinsa R. Nagar |
|---|---|
| Rok vydání: | 2021 |
| Předmět: |
RdRp
NSPs non-structural proteins Molecular model BBB blood-brain barrier In silico Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) LOAEL oral rat chronic toxicity Druggability RNA-dependent RNA polymerase SARS CoV-2 FDA food and drugs administration Computational biology medicine.disease_cause ssRNA single stranded ribonucleic acid Article Analytical Chemistry Autodock vina Inorganic Chemistry E envelope protein RdRp RNA dependent RNA polymerase BOILED brain or intestinal estimated permeation method medicine HBD hydrogen bond donor Spectroscopy Coronavirus Virtual screening MD simulations ACE2 angiotensin converting enzyme 2 S spike glycoprotein Chemistry Organic Chemistry COVID-19 ADMET assay ADMET absorption distribution metabolism excretion and toxicity COVID-19 corona virus disease 2019 MD molecular dynamics N nucleocapsid protein UTR untranslated region HERG human ether-a-go-go-related gene M membrane protein HBA hydrogen bond acceptor Molecular docking WHO world health organization pp1a/b polyproteins SARS CoV-2 severe acute respiratory syndrome 2 |
| Zdroj: | Journal of Molecular Structure |
| ISSN: | 0022-2860 |
| Popis: | Severe acute respiratory syndrome has relapsed recently as novel coronavirus causing a life threat to the entire world in the absence of an effective therapy. To hamper the replication of the deadly SARS CoV-2 inside the host cells, systematic in silico virtual screening of total 267,324 ligands from Asinex EliteSynergy and BioDesign libraries has been performed using AutoDock Vina against RdRp. The molecular modeling studies revealed the identification of twenty-one macrocyclic hits (2–22) with better binding energy than remdesivir (1), marketed SARS CoV-2 inhibitor. Further, the analysis using rules for drug-likeness and their ADMET profile revealed the candidature of these hits due to superior oral bioavailability and druggability. Further, the MD simulation studies of top two hits (2 and 3) performed using GROMACS 2020.1 for 10 ns revealed their stability into the docked complexes. These results provide an important breakthrough in the design of macrocyclic hits as SARS CoV-2 RNA replicase inhibitor. Graphical abstract Image, graphical abstract |
| Databáze: | OpenAIRE |
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