Gram-negative bacteria Yersinia secrete virulence factors that invade eukaryotic cells via type III secretion system. One particular virulence member, Yersinia outer protein E (YopE), targets Rho family of small GTPases by mimicking regulator GAP protein activity, and its secretion mainly induces cytoskeletal disruption and depolymerization of actin stress fibers within the host cell. In this work, potent drug-like inhibitors of YopE are investigated with virtual screening approaches. More than 500,000 unique small molecules from ZINC database were screened with a five-point pharmacophore, comprising three hydrogen acceptors, one hydrogen donor, and one ring, and derived from different salicylidene acylhydrazides. Binding modes and features of these molecules were investigated with a multistep molecular docking approach using Glide software. Virtual screening hits were further analyzed based on their docking score, chemical similarity, pharmacokinetic properties, and the key Arg144 interaction along with other active site residue interactions with the receptor. As a final outcome, a diverse set of ligands with inhibitory potential were proposed.
Keyphrases
- molecular docking
- molecular dynamics simulations
- protein protein
- small molecule
- molecular dynamics
- type iii
- pseudomonas aeruginosa
- escherichia coli
- staphylococcus aureus
- binding protein
- biofilm formation
- induced apoptosis
- amino acid
- antimicrobial resistance
- atomic force microscopy
- high throughput
- transcription factor
- stem cells
- single cell
- cell therapy
- cell cycle arrest
- adverse drug
- endoplasmic reticulum stress
- risk assessment
- human health
- heat stress
- cell migration
- mass spectrometry
- anti inflammatory
- bone marrow
- dna binding
- signaling pathway