Abstract
The manifestation of class D β-lactamases in the community raises significant concern as they can hydrolyze carbapenem antibiotics. Hence, it is exceptionally alluring to design novel inhibitors. Structure-based virtual screening using docking programs and molecular dynamics simulations was employed to identify two novel non-β-lactam compounds that possess the ability to block different OXA variants. Furthermore, the presence of a nonpolar aliphatic amino acid, valine, near the active site serine, was identified in all OXA variants that can be accounted to block the catalytic activity of OXA enzymes.
Cite
CITATION STYLE
Gupta, D., Singh, A., Somvanshi, P., Singh, A., & Khan, A. U. (2020). Structure-Based Screening of Non-β-Lactam Inhibitors against Class D β-Lactamases: An Approach of Docking and Molecular Dynamics. ACS Omega, 5(16), 9356–9365. https://doi.org/10.1021/acsomega.0c00356
Register to see more suggestions
Mendeley helps you to discover research relevant for your work.
