Life (Mar 2023)

Synthesis and in Silico Investigation of Organoselenium-Clubbed Schiff Bases as Potential M<sup>pro</sup> Inhibitors for the SARS-CoV-2 Replication

  • Saad Shaaban,
  • Aly Abdou,
  • Abdulrahman G. Alhamzani,
  • Mortaga M. Abou-Krisha,
  • Mahmoud A. Al-Qudah,
  • Mohamed Alaasar,
  • Ibrahim Youssef,
  • Tarek A. Yousef

DOI
https://doi.org/10.3390/life13040912
Journal volume & issue
Vol. 13, no. 4
p. 912

Abstract

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Since the first report of the organoselenium compound, ebselen, as a potent inhibitor of the SARS-CoV-2 Mpro main protease by Z. Jin et al. (Nature, 2020), different OSe analogs have been developed and evaluated for their anti-COVID-19 activities. Herein, organoselenium-clubbed Schiff bases were synthesized in good yields (up to 87%) and characterized using different spectroscopic techniques. Their geometries were studied by DFT using the B3LYP/6–311 (d, p) approach. Ten FDA-approved drugs targeting COVID-19 were used as model pharmacophores to interpret the binding requirements of COVID-19 inhibitors. The antiviral efficiency of the novel organoselenium compounds was assessed by molecular docking against the 6LU7 protein to investigate their possible interactions. Our results showed that the COVID-19 primary protease bound to organoselenium ligands with high binding energy scores ranging from −8.19 to −7.33 Kcal/mol for 4c and 4a to −6.10 to −6.20 Kcal/mol for 6b and 6a. Furthermore, the docking data showed that 4c and 4a are good Mpro inhibitors. Moreover, the drug-likeness studies, including Lipinski’s rule and ADMET properties, were also assessed. Interestingly, the organoselenium candidates manifested solid pharmacokinetic qualities in the ADMET studies. Overall, the results demonstrated that the organoselenium-based Schiff bases might serve as possible drugs for the COVID-19 epidemic.

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