In Silico Investigation of Spice Molecules as Potent Inhibitor of SARS-CoV-2

10.26434/chemrxiv.12323615 ◽

2020 ◽

Cited By ~ 1

Author(s):

Janmejaya Rout ◽

Bikash Chandra Swain ◽

Umakanta Tripathy

Keyword(s):

Infectious Disease ◽

Small Molecules ◽

Potent Inhibitor ◽

Computational Study ◽

Spike Protein ◽

Lab Experiments ◽

Main Protease ◽

Wet Lab ◽

Potential Inhibitors ◽

Adme Property

The severe acute respiratory syndrome Coronavirus 2 (SARS-CoV-2) is a novel infectious disease that is in rapid growth. Several trials are going on worldwide to find a solution for this pandemic. The viral replication can be blocked by inhibiting the SARS-CoV-2 spike protein (SARS-CoV-2 Spro), and the SARS-CoV-2 main protease (SARS-CoV-2 Mpro). The binding of potential small molecules to these proteins can possibly inhibit the replication and transcription of the virus. The spice molecules that are used in our food have the properties of antiviral, antifungal, and antimicrobial nature. As spice molecules are consumed in the diet, hence its antiviral properties against SARS-CoV-2 will benefit in a significant manner. Therefore, in this work, the blind molecular docking of 30 selected spice molecules (through ADME property screening) was performed for the identification of potential inhibitors for the Spro and Mpro of SARS-CoV-2. We found that all the molecules bind actively with the SARS-CoV-2 Spro and Mpro. However, the molecule, Piperine, is found to have the highest binding affinity among the 30 screened molecules. We anticipate immediate wet-lab experiments and clinical trials in support of this computational study might be helpful in inhibiting the SARS-CoV-2 virus.

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In silico investigation of potential inhibitors to main protease and spike protein of SARS-CoV-2 in propolis

Biochemistry and Biophysics Reports ◽

10.1016/j.bbrep.2021.100969 ◽

2021 ◽

pp. 100969

Author(s):

Azza H. Harisna ◽

Rizky Nurdiansyah ◽

Putri H. Syaifie ◽

Dwi W. Nugroho ◽

Kurniawan E. Saputro ◽

...

Keyword(s):

In Silico ◽

Spike Protein ◽

Main Protease ◽

Potential Inhibitors

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Targeting the GRP78-Dependant SARS-CoV-2 Cell Entry by Peptides and Small Molecules

Bioinformatics and Biology Insights ◽

10.1177/1177932220965505 ◽

2020 ◽

Vol 14 ◽

pp. 117793222096550

Author(s):

Loubna Allam ◽

Fatima Ghrifi ◽

Hakmi Mohammed ◽

Naima El Hafidi ◽

Rachid El Jaoudi ◽

...

Keyword(s):

Small Molecules ◽

Binding Sites ◽

Epigallocatechin Gallate ◽

Host Cells ◽

Spike Protein ◽

Target Cells ◽

Binding Affinities ◽

Rapid Spread ◽

Inhibitor Compounds ◽

Potential Inhibitors

The global burden of infections and the rapid spread of viral diseases show the need for new approaches in the prevention and development of effective therapies. To this end, we aimed to explore novel inhibitor compounds that can stop replication or decrease the viral load of the novel severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), for which there is currently no approved treatment. Besides using the angiotensin-converting enzyme (ACE2) receptor as a main gate, the CoV-2 can bind to the glucose-regulating protein 78 (GRP78) receptor to get into the cells to start an infection. Here, we report potential inhibitors comprising small molecules and peptides that could interfere with the interaction of SARS-CoV-2 and its target cells by blocking the recognition of the GRP78 cellular receptor by the viral Spike protein. These inhibitors were discovered through an approach of in silico screening of available databases of bioactive peptides and polyphenolic compounds and the analysis of their docking modes. This process led to the selection of 9 compounds with optimal binding affinities to the target sites. The peptides (satpdb18674, satpdb18446, satpdb12488, satpdb14438, and satpdb28899) act on regions III and IV of the viral Spike protein and on its binding sites in GRP78. However, 4 polyphenols such as epigallocatechin gallate (EGCG), homoeriodictyol, isorhamnetin, and curcumin interact, in addition to the Spike protein and its binding sites in GRP78, with the ATPase domain of GRP78. Our work demonstrates that there are at least 2 approaches to block the spread of SARS-CoV-2 by preventing its fusion with the host cells via GRP78.

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COMPUTATIONAL SCREENING AND MOLECULAR DOCKING OF LICHEN SECONDARY METABOLITES AGAINST SEVERE ACUTE RESPIRATORY SYNDROME-COV-2 MAIN PROTEASE AND SPIKE PROTEIN

Asian Journal of Pharmaceutical and Clinical Research ◽

10.22159/ajpcr.2021.v14i12.43227 ◽

2021 ◽

pp. 100-104

Author(s):

SENTHIL PRABHU S ◽

SATHISHKUMAR R ◽

KIRUTHIKA B

Keyword(s):

Molecular Docking ◽

Severe Acute Respiratory Syndrome ◽

Study Finding ◽

Spike Protein ◽

Protein Targets ◽

Lipinski’S Rule ◽

Computational Screening ◽

Main Protease ◽

Lichen Compounds ◽

Potential Inhibitors

Objective: At present, the coronavirus disease (COVID)-19 pandemic is increasing global health concerns. This coronavirus outbreak is caused by severe acute respiratory syndrome coronavirus (SARS-CoV)-2. Since, no specific antiviral for treatment against COVID-19, so identification of new therapeutics is an urgent need. The objective of this study is to the analysis of lichen compounds against main protease and spike protein targets of SARS-CoV-2 using in silico approach. Methods: A total of 108 lichen compounds were subjected to ADMET analysis and 14 compounds were selected based on the ADMET properties and Lipinski’s rule of five. Molecular docking was performed for screening of selected individual lichen metabolites against the main protease and spike proteins of SARS-CoV-2 by Schrodinger Glide module software. Results: Among the lead compounds, fallacinol showed the highest binding energy value of −11.83 kcal/mol against spike protein, 4-O-Demethylbarbatic acid exhibited the highest dock score of −11.67 kcal/mol against main protease. Conclusion: This study finding suggests that lichen substances may be potential inhibitors of SARS-CoV-2.

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Naturally occurring anthraquinones as potential inhibitors of SARS-CoV-2 main protease: an integrated computational study

Biologia ◽

10.1007/s11756-021-01004-4 ◽

2022 ◽

Author(s):

Sourav Das ◽

Anirudh Singh ◽

Sintu Kumar Samanta ◽

Atanu Singha Roy

Keyword(s):

Computational Study ◽

Naturally Occurring ◽

Main Protease ◽

Potential Inhibitors

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Docking Studies of Usnic Acid and Sodium Usnate on SARS CoV-2 Main Protease and Spike Protein RBD

10.26434/chemrxiv.12638906 ◽

2020 ◽

Author(s):

Roopa Guthappa

Keyword(s):

Infectious Disease ◽

Antiviral Agents ◽

Usnic Acid ◽

Docking Studies ◽

Spike Protein ◽

Binding Affinities ◽

Herbal Supplements ◽

Main Protease ◽

The World ◽

Mouth Wash

SARS CoV-2 a pandemic influenza like infectious disease emerged in December 2019 has spread throughout the world within few months. Scientists are trying their best to find medicine and vaccine. Usnic acid and its derivatives as herbal supplements are widely used as mouth wash, cosmetics, antiviral agents. In this study, usnic acid and its derivative-sodium usnate in comparison with favipiravir are docked with main protease and spike protein RBD 6M0J of SARS Cov-2. Usnic acid and sodium usnate exhibit better binding affinities for main protease and spike RBD. The data has been compared with favipiravir. Favipiravir, usnic acid, sodium usnate shows binding affinity of -4.25, -8.05 and -8.55 kcal/mol respectively with main protease. While favipiravir, usnic acid and sodium usnate exhibit binding affinities of -4.25, -6.02 and -6.53 kcal/mol with spike RBD respectively. One of the interesting features is that the inhibition constant values of usnic acid is 1.27 µM and sodium usnate is 539.86 nM in comparison to favipiravir (764.13 µM) with main protease.

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A Computational Study to Identify Potential Inhibitors of SARS-CoV-2 Main Protease (Mpro) from Eucalyptus Active Compounds

Computation ◽

10.3390/computation8030079 ◽

2020 ◽

Vol 8 (3) ◽

pp. 79

Author(s):

Ibrahim Ahmad Muhammad ◽

Kanikar Muangchoo ◽

Auwal Muhammad ◽

Ya’u Sabo Ajingi ◽

Ibrahim Yahaya Muhammad ◽

...

Keyword(s):

Molecular Docking ◽

Binding Energy ◽

Computational Study ◽

Md Simulations ◽

Binding Energies ◽

Drug Candidate ◽

Global Public Health ◽

Main Protease ◽

Poisson Boltzmann ◽

Potential Inhibitors

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) was found to be a severe threat to global public health in late 2019. Nevertheless, no approved medicines have been found to inhibit the virus effectively. Anti-malarial and antiviral medicines have been reported to target the SARS-CoV-2 virus. This paper chose eight natural eucalyptus compounds to study their binding interactions with the SARS-CoV-2 main protease (Mpro) to assess their potential for becoming herbal drugs for the new SARS-CoV-2 infection virus. In-silico methods such as molecular docking, molecular dynamics (MD) simulations, and Molecular Mechanics Poisson Boltzmann Surface Area (MM/PBSA) analysis were used to examine interactions at the atomistic level. The results of molecular docking indicate that Mpro has good binding energy for all compounds studied. Three docked compounds, α-gurjunene, aromadendrene, and allo-aromadendrene, with highest binding energies of −7.34 kcal/mol (−30.75 kJ/mol), −7.23 kcal/mol (−30.25 kJ/mol), and −7.17 kcal/mol (−29.99 kJ/mol) respectively, were simulated with GROningen MAchine for Chemical Simulations (GROMACS) to measure the molecular interactions between Mpro and inhibitors in detail. Our MD simulation results show that α-gurjunene has the strongest binding energy of −20.37 kcal/mol (−85.21 kJ/mol), followed by aromadendrene with −18.99 kcal/mol (−79.45 kJ/mol), and finally allo-aromadendrene with −17.91 kcal/mol (−74.95 kJ/mol). The findings indicate that eucalyptus may be used to inhibit the Mpro enzyme as a drug candidate. This is the first computational analysis that gives an insight into the potential role of structural flexibility during interactions with eucalyptus compounds. It also sheds light on the structural design of new herbal medicinal products against Mpro.

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Consensus virtual screening of dark chemical matter and food chemicals uncover potential inhibitors of SARS-CoV-2 main protease

RSC Advances ◽

10.1039/d0ra04922k ◽

2020 ◽

Vol 10 (42) ◽

pp. 25089-25099 ◽

Cited By ~ 4

Author(s):

Marisa G. Santibáñez-Morán ◽

Edgar López-López ◽

Fernando D. Prieto-Martínez ◽

Norberto Sánchez-Cruz ◽

José L. Medina-Franco

Keyword(s):

Virtual Screening ◽

Small Molecules ◽

Screening Strategy ◽

Drug Candidates ◽

Main Protease ◽

Potential Inhibitors ◽

Chemical Matter

As part of a global effort to identify drug candidates for the treatment of COVID-19, herein, we report small molecules commercially available selected from a consensus virtual screening strategy.

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Docking Studies of Usnic Acid and Sodium Usnate on SARS CoV-2 Main Protease and Spike Protein RBD

10.26434/chemrxiv.12638906.v1 ◽

2020 ◽

Author(s):

Roopa Guthappa

Keyword(s):

Infectious Disease ◽

Antiviral Agents ◽

Usnic Acid ◽

Docking Studies ◽

Spike Protein ◽

Binding Affinities ◽

Herbal Supplements ◽

Main Protease ◽

The World ◽

Mouth Wash

SARS CoV-2 a pandemic influenza like infectious disease emerged in December 2019 has spread throughout the world within few months. Scientists are trying their best to find medicine and vaccine. Usnic acid and its derivatives as herbal supplements are widely used as mouth wash, cosmetics, antiviral agents. In this study, usnic acid and its derivative-sodium usnate in comparison with favipiravir are docked with main protease and spike protein RBD 6M0J of SARS Cov-2. Usnic acid and sodium usnate exhibit better binding affinities for main protease and spike RBD. The data has been compared with favipiravir. Favipiravir, usnic acid, sodium usnate shows binding affinity of -4.25, -8.05 and -8.55 kcal/mol respectively with main protease. While favipiravir, usnic acid and sodium usnate exhibit binding affinities of -4.25, -6.02 and -6.53 kcal/mol with spike RBD respectively. One of the interesting features is that the inhibition constant values of usnic acid is 1.27 µM and sodium usnate is 539.86 nM in comparison to favipiravir (764.13 µM) with main protease.

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Identification of saquinavir as a potent inhibitor of dimeric SARS-CoV2 main protease through MM/GBSA

10.21203/rs.3.rs-27406/v1 ◽

2020 ◽

Author(s):

Bello Martiniano ◽

Martínez-Muñoz Alberto ◽

Balbuena-Rebolledo Irving

Keyword(s):

Md Simulation ◽

Potent Inhibitor ◽

Drug Repurposing ◽

Md Simulations ◽

Generalized Born ◽

Main Protease ◽

Promising Target ◽

Approved Drugs ◽

Potential Inhibitors ◽

Fda Approved Drugs

Abstract Among targets selected for studies aimed to identify potential inhibitors against COVID-19, SARS-CoV2 main proteinase (Mpro) is highlighted. Mpro is indispensable for virus replication, and is a promising target of potential inhibitors of COVID-19. Recently, monomeric SARS-CoV2 Mpro, drug repurposing and docking methods have facilitated the identification of several potential inhibitors. Results were refined through the assessment of dimeric SARS-CoV2 Mpro, which represents the functional state of enzyme. Docking and molecular dynamics (MD) simulations combined with molecular mechanics/generalized Born surface area (MM/GBSA) studies indicated that dimeric Mpro most significantly impacts binding affinity tendency compared with the monomeric state, which suggesting that dimeric state is most useful when performing studies aimed to identify drugs targeting Mpro. In this study, we extend previous research by performing docking and MD simulation studies coupled with an MM/GBSA approach to assess binding of dimeric SARS-CoV2 Mpro to 12 FDA-approved drugs (darunavir, indinavir, saquinavir, tipranavir, diosmin, hesperidin, rutin, raltegravir, velpatasvir, ledipasvir, rosuvastatin and bortezomib), which were identified as the best candidates for treatment of COVID-19 in some previous dockings studies involving monomeric SARS-CoV2 Mpro. This analysis identified saquinavir as a potent inhibitor of dimeric SARS-CoV2 Mpro, therefore, the compound may have clinical utility against COVID-19.

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