Targeting Spike‐ACE2 Interface of SARS‐CoV‐2 and its Omicron Variant: A Comparative Screening of Potential Inhibitors for Existing and Anticipating Variants Using Molecular Modelling Approach - Publication - Bridge of Knowledge

Your account

login

Search

Targeting Spike‐ACE2 Interface of SARS‐CoV‐2 and its Omicron Variant: A Comparative Screening of Potential Inhibitors for Existing and Anticipating Variants Using Molecular Modelling Approach

Abstract

The recent COVID pandemic has shown major impact on public health and economic crisis. Despite the development of many vaccines and drugs against the severe acute respiratory syndrome (SARS) coronavirus 2, the pandemic still persists. The continued spread of the virus is largely driven by the emergence of viral variants such as α, β, γ, delta, epsilon spike, omicron and its subvariants (BA.1,2,3) which can evade the current vaccines through mutations in the spike protein.[1] For instance, spike to omicron has modifications at different mutations (D405N, K417N, S477N, E484A, Q493R, N501Y, Y505H).[1b] These mutations will affect functional properties and hence may alter the specificity towards potential drug candidates. Therefore, it is important to understand the role of these mutations on interactions with existing drug candidates. In this study, we focus on the two forms of SARS-CoV-2, such as wild-type spike and omicron and unveil their interactions with different drugs. For this purpose, we have taken about hundred drugs categorised in twelve groups of anticancer, natural products, enzyme inhibitors, antivirals, antioxidants, anti-bacterials, anti-malarials, antidiabetics, antimicrobials, anti-inflammatory, antifungals and other drugs. We used in-silico methods to understand the effect of these drug molecules on wild type and omicron spike RBD at the interface of ACE2 enzyme. Based on molecular docking results, we have chosen 7 best docked compounds and studied their interaction patterns in detail by molecular dynamics simulation.

Citations

  • 0

    CrossRef

  • 0

    Web of Science

  • 0

    Scopus

Authors (6)

Cite as

Full text

full text is not available in portal

Keywords

Details

Category:
Articles
Type:
artykuły w czasopismach
Published in:
ChemistrySelect no. 8, pages 1 - 13,
ISSN: 2365-6549
Language:
English
Publication year:
2023
Bibliographic description:
Takkella D., Sharma S., Krzemieniecki R., Pabbathi A., Sappati S., Gavvala K.: Targeting Spike‐ACE2 Interface of SARS‐CoV‐2 and its Omicron Variant: A Comparative Screening of Potential Inhibitors for Existing and Anticipating Variants Using Molecular Modelling Approach// ChemistrySelect -Vol. 8,iss. 32 (2023),
DOI:
Digital Object Identifier (open in new tab) 10.1002/slct.202302687
Sources of funding:
  • IDUB
Verified by:
Gdańsk University of Technology

seen 61 times

Recommended for you

Reverse vaccinology-based prediction of a multi-epitope SARS-CoV-2 vaccine and its tailoring to new coronavirus variants

2023

Enhanced susceptibility of SARS-CoV-2 spike RBD protein assay targeted by cellular receptors ACE2 and CD147: Multivariate data analysis of multisine impedimetric response

2022

Highly Conserved Homotrimer Cavity Formed by the SARS-CoV-2 Spike Glycoprotein: A Novel Binding Site

2020

Biochemical, Structural Analysis, and Docking Studies of Spiropyrazoline Derivatives

  • A. Adamus-Grabicka,
  • M. Daśko,
  • P. Hikisz
  • + 3 authors
2022
Meta Tags