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Venetoclax: a promising repurposed drug against SARS-CoV-2 main protease

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Taylor & Francis Group2022-12-26 更新2026-04-16 收录
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https://tandf.figshare.com/articles/dataset/Venetoclax_a_promising_repurposed_drug_against_SARS-CoV-2_main_protease/16411216/2
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Global health care emergency caused by a new coronavirus (severe acute respiratory syndrome coronavirus 2 or SARS-CoV-2) demands urgent need to repurpose the approved pharmaceutical drugs. Main protease, M<sup>pro</sup> of SARS-CoV-2 draws significant attention as a drug target. Herein, we have screened FDA approved organosulfur drugs (till 2016) and our laboratory synthesized organosulfur and organoselenium compounds (L1-L306) against M<sup>pro</sup>-apo using docking followed by classical MD simulations. Additionally, a series of compounds (L307-L364) were chosen from previous experimental studies, which were reported to exhibit inhibitory potentials towards M<sup>pro</sup>. We found several organosulfur drugs, particularly Venetoclax (FDA approved organosulfur drug for Leukemia) to be a high-affinity binders to the M<sup>pro</sup> of SARS-CoV-2. The results reveal that organosulfur compounds including Venetoclax preferentially bind (non-covalently) to the non-catalytic pocket of the protein located in the dimer interface. We found that the ligand binding is primarily favoured by ligand-protein van der Waals interaction and penalized by desolvation effect. Interestingly, Venetoclax binding alters the local flexibility of M<sup>pro</sup> and exerts pronounced effect in the C-terminal as well as two loop regions (Loop-A and Loop-B) that play important roles in catalysis. These findings highlighted the importance of drug repurposing and explored the non-catalytic pockets of M<sup>pro</sup> in combating COVID-19 infection in addition to the importance of catalytic binding pocket of the protein. Communicated by Ramaswamy H. Sarma
提供机构:
Bhattacherjee, Debojit; Ghosh, Suvankar; Bhabak, Krishna Pada; Satpati, Priyadarshi
创建时间:
2021-08-26
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