Computer aided ligand based screening for identification of promising molecules against enzymes involved in peptidoglycan biosynthetic pathway from Acinetobacter baumannii

Gizachew Muluneh Amera; Rameez Jabeer Khan; Amita Pathak; Rajat Kumar Jha; Jayaraman Muthukumaran; Amit Kumar Singh

doi:10.1016/j.micpath.2020.104205

Computer aided ligand based screening for identification of promising molecules against enzymes involved in peptidoglycan biosynthetic pathway from Acinetobacter baumannii

Microb Pathog. 2020 Oct:147:104205. doi: 10.1016/j.micpath.2020.104205. Epub 2020 Apr 28.

Authors

Gizachew Muluneh Amera¹, Rameez Jabeer Khan¹, Amita Pathak², Rajat Kumar Jha¹, Jayaraman Muthukumaran¹, Amit Kumar Singh³

Affiliations

¹ Department of Biotechnology, School of Engineering and Technology, Sharda University, P.C, 201310, Greater Noida, U.P, India.
² Department of Chemistry, Indian Institute of Technology, HauzKhas, New Delhi, 110016, India.
³ Department of Biotechnology, School of Engineering and Technology, Sharda University, P.C, 201310, Greater Noida, U.P, India. Electronic address: amitk.singh@sharda.ac.in.

PMID: 32353580
DOI: 10.1016/j.micpath.2020.104205

Abstract

A. baumannii has been considered as Priority-I as suggested by the World Health Organization (WHO) and the most critical pathogenic microorganism for causing nosocomial infection in imunno-compromised hospital-acquired patients due to multi-drug resistance (MDR). In the current study, we utilized "Computer-aided ligand-based virtual screening approach" for identification of promising molecules against Mur family proteins based on the known inhibitor (Naphthyl Tetronic Acids ((5Z)-3-(4-chlorophenyl)-4-hydroxy-5-(1-naphthylmethylene) furan-2(5H)-one)) of MurB from E. coli. The in-house library was prepared using a similarity search of a known inhibitor (Drug Bank ID: DB07296) against several relevant chemical databases. The molecules obtained from virtual screening of Naphthyl Tetronic Acids in-house library were successively subjected to physicochemical and ADMET screening. After this, the molecules which passed all the filters, subsequently subjected into interaction analysis with the drug target proteins (MurB, MurD, MurE and MurG) of A. baumanni and the results explained that four molecules were promising (CHEMBL468144, DB07296, Enamine_T5956969 and 54723243) for further molecular dynamics simulations. The free and ligand bounded proteins that undergone MD simulation are listed as follows: MurB, MurB-CHEMBL468144, MurB-DB07296, MurE, MurE-54723243, MurE-DB07296, MurD, MurD-Enamine_T5956969, MurD-DB07296, MurG, MurG-CHEMBL468144, and MurG-DB07296. Based on global and essential dynamics analysis, the stability order of molecules towards MurB (CHEMBL468144 > DB07296); MurD (Enamine_T5956969 > DB07296); MurE (54723243 > DB07296) and MurG (CHEMBL468144 > DB07296) indicates that the newly identified molecules are more promising one in comparison with the existing inhibitor. Based on all the docking and MD simulation results, the stability order of the free and ligand bounded protein are as follows; MurB and MurB-ligand complexes > MurD and MurD-ligand complexes > MurG and MurG-ligand complexes > MurE and MurE-ligand complexes. Finally, the selected compounds would be recommended for further experimental investigations and used as promising inhibitors of the infection caused by A. baumannii.

Keywords: Acinetobacter baumannii; LBDD; Mur family; Naphthyl tetronic acid; Simulation.

MeSH terms

Acinetobacter baumannii* / metabolism
Biosynthetic Pathways
Computers
Escherichia coli / metabolism
Humans
Ligands
Molecular Dynamics Simulation
Peptide Synthases / metabolism
Peptidoglycan*

Substances

Ligands
Peptidoglycan
Peptide Synthases