Your search keyword '"sars-cov-2 main protease"' showing total 5 results

1. Shedding Light on Dark Chemical Matter: The Discovery of a SARS-CoV-2 M pro Main Protease Inhibitor through Intensive Virtual Screening and In Vitro Evaluation.

Author

Peralta-Moreno, Maria Nuria, Mena, Yago, Ortega-Alarcon, David, Jimenez-Alesanco, Ana, Vega, Sonia, Abian, Olga, Velazquez-Campoy, Adrian, Thomson, Timothy M., Pinto, Marta, Granadino-Roldán, José M., Santos Tomas, Maria, Perez, Juan J., and Rubio-Martinez, Jaime

Subjects

*CHEMICAL inhibitors, *DARK matter, *SARS-CoV-2, *PROTEASE inhibitors, *HIGH throughput screening (Drug development), *DRUG development

Abstract

The development of specific antiviral therapies targeting SARS-CoV-2 remains fundamental because of the continued high incidence of COVID-19 and limited accessibility to antivirals in some countries. In this context, dark chemical matter (DCM), a set of drug-like compounds with outstanding selectivity profiles that have never shown bioactivity despite being extensively assayed, appears to be an excellent starting point for drug development. Accordingly, in this study, we performed a high-throughput screening to identify inhibitors of the SARS-CoV-2 main protease (Mpro) using DCM compounds as ligands. Multiple receptors and two different docking scoring functions were employed to identify the best molecular docking poses. The selected structures were subjected to extensive conventional and Gaussian accelerated molecular dynamics. From the results, four compounds with the best molecular behavior and binding energy were selected for experimental testing, one of which presented inhibitory activity with a Ki value of 48 ± 5 μM. Through virtual screening, we identified a significant starting point for drug development, shedding new light on DCM compounds. [ABSTRACT FROM AUTHOR]

Published

2024

2. Correlation of Experimental and Calculated Inhibition Constants of Protease Inhibitor Complexes.

Author

Goettig, Peter, Chen, Xingchen, and Harris, Jonathan M.

Subjects

*PROTEASE inhibitors, *ANTITHROMBINS, *CYSTEINE proteinases, *SERINE proteinases, *TRYPSIN inhibitors, *METALLOPROTEINASES, *PROTEIN-protein interactions, *FC receptors, *TRYPSIN

Abstract

Predicting the potency of inhibitors is key to in silico screening of promising synthetic or natural compounds. Here we describe a predictive workflow that provides calculated inhibitory values, which concord well with empirical data. Calculations of the free interaction energy ΔG with the YASARA plugin FoldX were used to derive inhibition constants Ki from PDB coordinates of protease–inhibitor complexes. At the same time, corresponding KD values were obtained from the PRODIGY server. These results correlated well with the experimental values, particularly for serine proteases. In addition, analyses were performed for inhibitory complexes of cysteine and aspartic proteases, as well as of metalloproteases, whereby the PRODIGY data appeared to be more consistent. Based on our analyses, we calculated theoretical Ki values for trypsin with sunflower trypsin inhibitor (SFTI-1) variants, which yielded the more rigid Pro14 variant, with probably higher potency than the wild-type inhibitor. Moreover, a hirudin variant with an Arg1 and Trp3 is a promising basis for novel thrombin inhibitors with high potency. Further examples from antibody interaction and a cancer-related effector-receptor system demonstrate that our approach is applicable to protein interaction studies beyond the protease field. [ABSTRACT FROM AUTHOR]

Published

2024

3. Identification of a Putative SARS-CoV-2 Main Protease Inhibitor through In Silico Screening of Self-Designed Molecular Library.

Author

Liu, Nanxin, Yang, Zeyu, Liu, Yuying, Dang, Xintao, Zhang, Qingqing, Wang, Jin, Liu, Xueying, Zhang, Jie, and Pan, Xiaoyan

Subjects

*PROTEASE inhibitors, *MEDICAL screening, *SARS-CoV-2, *SECONDARY amines, *DRUG target, *VIRAL replication

Abstract

There have been outbreaks of SARS-CoV-2 around the world for over three years, and its variants continue to evolve. This has become a major global health threat. The main protease (Mpro, also called 3CLpro) plays a key role in viral replication and proliferation, making it an attractive drug target. Here, we have identified a novel potential inhibitor of Mpro, by applying the virtual screening of hundreds of nilotinib-structure-like compounds that we designed and synthesized. The screened compounds were assessed using SP docking, XP docking, MM-GBSA analysis, IFD docking, MD simulation, ADME/T prediction, and then an enzymatic assay in vitro. We finally identified the compound V291 as a potential SARS-CoV-2 Mpro inhibitor, with a high docking affinity and enzyme inhibitory activity. Moreover, the docking results indicate that His41 is a favorable amino acid for pi-pi interactions, while Glu166 can participate in salt-bridge formation with the protonated primary or secondary amines in the screened molecules. Thus, the compounds reported here are capable of engaging the key amino acids His41 and Glu166 in ligand-receptor interactions. A pharmacophore analysis further validates this assertion. [ABSTRACT FROM AUTHOR]

Published

2023

4. The Se–S Bond Formation in the Covalent Inhibition Mechanism of SARS-CoV-2 Main Protease by Ebselen-like Inhibitors: A Computational Study

Author

Nino Russo, Tiziana Marino, Angela Parise, and Isabella Romeo

Subjects

QH301-705.5, Stereochemistry, medicine.medical_treatment, Isoindoles, Molecular Dynamics Simulation, Antiviral Agents, DFT, Article, Catalysis, Inorganic Chemistry, chemistry.chemical_compound, Molecular dynamics, SARS-CoV-2 main protease, Catalytic Domain, Organoselenium Compounds, medicine, Humans, Protease Inhibitors, Biology (General), Physical and Theoretical Chemistry, Binding site, QD1-999, Molecular Biology, Coronavirus 3C Proteases, Spectroscopy, Binding Sites, Protease, SARS-CoV-2, Chemistry, Ebselen, Organic Chemistry, Se–S covalent bond, COVID-19, General Medicine, Acceptor, COVID-19 Drug Treatment, Computer Science Applications, Hybrid functional, Molecular Docking Simulation, Covalent bond, Drug Design, Potential energy surface, inhibition mechanism, potential energy surface

Abstract

The inhibition mechanism of the main protease (Mpro) of SARS-CoV-2 by ebselen (EBS) and its analog with a hydroxyl group at position 2 of the benzisoselenazol-3(2H)-one ring (EBS-OH) was studied by using a density functional level of theory. Preliminary molecular dynamics simulations on the apo form of Mpro were performed taking into account both the hydrogen donor and acceptor natures of the Nδ and Nε of His41, a member of the catalytic dyad. The potential energy surfaces for the formation of the Se–S covalent bond mediated by EBS and EBS-OH on Mpro are discussed in detail. The EBS-OH shows a distinctive behavior with respect to EBS in the formation of the noncovalent complex. Due to the presence of canonical H-bonds and noncanonical ones involving less electronegative atoms, such as sulfur and selenium, the influence on the energy barriers and reaction energy of the Minnesota hybrid meta-GGA functionals M06, M06-2X and M08HX, and the more recent range-separated hybrid functional wB97X were also considered. The knowledge of the inhibition mechanism of Mpro by the small protease inhibitors EBS or EBS-OH can enlarge the possibilities for designing more potent and selective inhibitor-based drugs to be used in combination with other antiviral therapies.

Published

2021

5. The Se–S Bond Formation in the Covalent Inhibition Mechanism of SARS-CoV-2 Main Protease by Ebselen-like Inhibitors: A Computational Study.

Author

Parise, Angela, Romeo, Isabella, Russo, Nino, and Marino, Tiziana

Subjects

*SARS-CoV-2, *COVALENT bonds, *PROTEASE inhibitors, *POTENTIAL energy surfaces, *MOLECULAR dynamics

Abstract

The inhibition mechanism of the main protease (Mpro) of SARS-CoV-2 by ebselen (EBS) and its analog with a hydroxyl group at position 2 of the benzisoselenazol-3(2H)-one ring (EBS-OH) was studied by using a density functional level of theory. Preliminary molecular dynamics simulations on the apo form of Mpro were performed taking into account both the hydrogen donor and acceptor natures of the Nδ and Nε of His41, a member of the catalytic dyad. The potential energy surfaces for the formation of the Se–S covalent bond mediated by EBS and EBS-OH on Mpro are discussed in detail. The EBS-OH shows a distinctive behavior with respect to EBS in the formation of the noncovalent complex. Due to the presence of canonical H-bonds and noncanonical ones involving less electronegative atoms, such as sulfur and selenium, the influence on the energy barriers and reaction energy of the Minnesota hybrid meta-GGA functionals M06, M06-2X and M08HX, and the more recent range-separated hybrid functional wB97X were also considered. The knowledge of the inhibition mechanism of Mpro by the small protease inhibitors EBS or EBS-OH can enlarge the possibilities for designing more potent and selective inhibitor-based drugs to be used in combination with other antiviral therapies. [ABSTRACT FROM AUTHOR]

Published

2021