Abstract
Recently the E protein of SARS-CoV-2 has become a very important target in the potential treatment of COVID-19 since it is known to regulate different stages of the viral cycle. There is biochemical evidence that E protein exists in two forms, as monomer and homopentamer. An in silico screening analysis was carried out employing 5852 ligands (from Zinc databases), and performing an ADMET analysis, remaining a set of 2155 compounds. Furthermore, docking analysis was performed on specific sites and different forms of the E protein. From this study we could identify that the following ligands showed the highest binding affinity: nilotinib, dutasteride, irinotecan, saquinavir and alectinib. We carried out some molecular dynamics simulations and free energy MM–PBSA calculations of the protein–ligand complexes (with the mentioned ligands). Of worthy interest is that saquinavir, nilotinib and alectinib are also considered as a promising multitarget ligand because it seems to inhibit three targets, which play an important role in the viral cycle. On the other side, saquinavir was shown to be able to bind to E protein both in its monomeric as well as pentameric forms. Finally, further experimental assays are needed to probe our hypothesis derived from in silico studies.
| Original language | English |
|---|---|
| Article number | 296 |
| Number of pages | 19 |
| Journal | Pharmaceuticals |
| Volume | 16 |
| Issue number | 2 |
| DOIs | |
| Publication status | Published - Feb 2023 |
Bibliographical note
Funding Information:National Grants (Secretaria de Investigación y Posgrado (SIP) del Instituto Politécnico Nacional):20230833, 20230987, and 20230991. CONACYT: PAACTI 312807 and Instituto Politécnico Nacional (IPN).
Publisher Copyright:
© 2023 by the authors.
Keywords
- COVID-19
- E protein
- SARS-CoV-2
- drug repositioning
- in silico studies