Targeting the Main Protease (M<sup>pro</sup>, nsp5) by Growth of Fragment Scaffolds Exploiting Structure-Based Methodologies

Altincekic, Nadide; Jores, Nathalie; Löhr, Frank; Richter, Christian; Ehrhardt, Claus; Blommers, Marcel J. J.; Berg, Hannes; Öztürk, Sare; Gande, Santosh L.; Linhard, Verena; Orts, Julien; Abi Saad, Marie Jose; Bütikofer, Matthias; Kaderli, Janina; Karlsson, B. Göran; Brath, Ulrika; Hedenström, Mattias; Gröbner, Gerhard; Sauer, Uwe H.; Perrakis, Anastassis; Langer, Julian; Banci, Lucia; Cantini, Francesca; Fragai, Marco; Grifagni, Deborah; Barthel, Tatjana; Wollenhaupt, Jan; Weiss, Manfred S.; Robertson, Angus; Bax, Adriaan; Sreeramulu, Sridhar; Schwalbe, Harald

doi:10.1021/acschembio.3c00720

ACS Chem. Biol.

2024

DOI: 10.1021/acschembio.3c00720

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Targeting the Main Protease (M^pro, nsp5) by Growth of Fragment Scaffolds Exploiting Structure-Based Methodologies

Nadide Altincekic,

Nathalie Jores,

Frank Löhr

et al.

Abstract: The main protease M pro , nsp5, of SARS-CoV-2 (SCoV2) is one of its most attractive drug targets. Here, we report primary screening data using nuclear magnetic resonance spectroscopy (NMR) of four different libraries and detailed follow-up synthesis on the promising uracil-containing fragment Z604 derived from these libraries. Z604 shows time-dependent binding. Its inhibitory effect is sensitive to reducing conditions. Starting with Z604, we synthesized and characterized 13 compounds designed by fragment growt… Show more

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Computational Assessment of Clinical Drugs against SARS‐CoV‐2: Foreseeing Molecular Mechanisms and Potent Mpro Inhibitors

Panda,

Pani,

Sen Gupta

et al. 2024

ChemPhysChem

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The emergence of new SARS‐CoV‐2 variants of concern (VOC) is a propulsion for accelerated potential therapeutic discovery. SARS‐CoV‐2’s main protease (Mpro), essential for host cell viral replication, is a pre‐eminent druggable protein target. Here, we perform extensive drug re‐profiling of the comprehensive Excelra database, which compiles various under‐trial drug candidates for COVID‐19 treatment. For mechanistic understanding, the most promising screened‐out molecules with targets are subjected to molecular dynamics (MD) simulations. Post‐MD analyses demonstrate Darunavir, Ponatinib, and Tomivosertib forming a stable complex with Mpro, characterized by less fluctuation of Cα atoms, smooth and stable root‐mean‐square deviation (RMSD), and robust contact with the active site residues. Likewise, they all have lower binding free energy with Mpro, demonstrating strong affinity. In free energy landscape profiles, the distances from His41 and Cys145 exhibit a single energy minima basin, implying their preponderance in proximity to Mpro’s catalytic dyad. Overall, the computational assessment earmarks promising candidates from the Excelra database, emphasizing on carrying out exhaustive biochemical experiments along with clinical trials. The work lays the foundation for potential therapeutic interventions in treating COVID‐19.

show abstract

Computational Assessment of Clinical Drugs against SARS‐CoV‐2: Foreseeing Molecular Mechanisms and Potent Mpro Inhibitors

Panda,

Pani,

Sen Gupta

et al. 2024

ChemPhysChem

View full text Add to dashboard Cite

show abstract

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Targeting the Main Protease (M^pro, nsp5) by Growth of Fragment Scaffolds Exploiting Structure-Based Methodologies

Cited by 1 publication

References 64 publications

Computational Assessment of Clinical Drugs against SARS‐CoV‐2: Foreseeing Molecular Mechanisms and Potent Mpro Inhibitors

Computational Assessment of Clinical Drugs against SARS‐CoV‐2: Foreseeing Molecular Mechanisms and Potent Mpro Inhibitors

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Targeting the Main Protease (Mpro, nsp5) by Growth of Fragment Scaffolds Exploiting Structure-Based Methodologies

Cited by 1 publication

References 64 publications

Computational Assessment of Clinical Drugs against SARS‐CoV‐2: Foreseeing Molecular Mechanisms and Potent Mpro Inhibitors

Computational Assessment of Clinical Drugs against SARS‐CoV‐2: Foreseeing Molecular Mechanisms and Potent Mpro Inhibitors

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Product

Resources

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Targeting the Main Protease (M^pro, nsp5) by Growth of Fragment Scaffolds Exploiting Structure-Based Methodologies