Computational Investigation of Bioactive Phytoconstituents as Sars-Cov-2 Main Protease Inhibitors Through Molecular Docking and Interaction Fingerprint Studies

Rajitha Galla^1*, Vidya Rani Murthi¹, Yasmintaj Shaik¹, Saritha Karnati², Umakanth Naik Vankadoth³ and Umamaheswari Amineni³

¹Institute of Pharmaceutical technology, Sri Padmavati Mahila Visvavidyalayam, Tirupati, Andhra Pradesh, India

²KVSR Siddhartha College of Pharmaceutical Sciences, Vijayawada, 520010, Andhra Pradesh, India

³Department of Bioinformatics, Sri Venkateswara Institute of Medical Sciences, Tirupati-517502, Andhra Pradesh, India

Corresponding Author E-mail: grajitha@spmvv.ac.in

Abstract: Since 2019, the SARS-CoV-2 infection has continued to cause significant human suffering. Numerous investigations into the viral pathogenesis have led to converging conclusions on how the virus enters and spreads within the host. The main protease (M^pro) of coronaviruses has been considered as an attractive therapeutic target because of its important role in processing polyproteins translated from viral RNA. Many studies discovered that phytoconstituents possess potent antiviral activities. Hence, in the present work, 439 co-crystal ligands of SARS-CoV-2 M^pro were collected and docked with M^pro of SARS-CoV-2 (PDB ID:7AEH) to identify best crystal ligand. Among all the crystal ligands collected, HF0 (7-O-methyl-dihydromyricetin) showed good XP G score -7.872 Kcal/Mol and it was selected as reference to compare the docking scores of phytoconstituents. Then, molecular docking study was performed for 274 antiviral phytoconstituents from various medicinal plants against M^pro of SARS-CoV-2. Molecular docking studies found that seven phytoconstituents exhibited better docking scores than best co-crystal ligand HF0. Among the seven best docked phytoconstituents, 3,4-dicaffeoylquinic acid showed good interactions with key amino acid residues in substrate binding site of M^pro with XPG Score –9.721 Kcal/Mol. Qikprop results indicated that the most phytoconstituents have demonstrated favourable pharmacological characteristics. Interaction fingerprint analysis revealed that all the seven best docked phytoconstituents of the present study bound to Glu166, key residue situated in the centre of the substrate binding site of M^pro resulting in the reduction of the catalytic activity of main protease thus blocking the replication of SARS-CoV-2.

Keywords: Antiviral; Interaction fingerprint; Molecular docking; Main protease; Phytoconstituents; SARS-CoV-2

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