Structure-Based Screening of Non-β-Lactam Inhibitors against Class D β-Lactamases: An Approach of Docking and Molecular Dynamics | Zendy

Divya Gupta | Zendy; Aditi Singh | Zendy; Pallavi Somvanshi | Zendy; Ajeet Singh | Zendy; Asad U. Khan | Zendy

Open Access

Structure-Based Screening of Non-β-Lactam Inhibitors against Class D β-Lactamases: An Approach of Docking and Molecular Dynamics

Author(s) -

Divya Gupta,

Aditi Singh,

Pallavi Somvanshi,

Ajeet Singh,

Asad U. Khan

Publication year - 2020

Publication title -

acs omega

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.779

H-Index - 40

ISSN - 2470-1343

DOI - 10.1021/acsomega.0c00356

Subject(s) - docking (animal) , virtual screening , serine , chemistry , active site , lactam , stereochemistry , enzyme , valine , molecular dynamics , combinatorial chemistry , hydrolysis , amino acid , biochemistry , computational biology , biology , computational chemistry , medicine , nursing

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.

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