Identification of Novel Inhibitors of Bacterial Translation Elongation Factors

Author:

Jayasekera Maithri M. K.1,Onheiber Keysha1,Keith John1,Venkatesan Hariharan1,Santillan Alejandro1,Stocking Emily M.1,Tang Liu1,Miller Jennifer1,Gomez Leslie1,Rhead Brooke1,Delcamp Tavner1,Huang Shaoming1,Wolin Ronald1,Bobkova Ekaterina V.1,Shaw Karen Joy1

Affiliation:

1. Infectious Diseases, Johnson & Johnson Pharmaceutical Research and Development, L.L.C., La Jolla, California

Abstract

ABSTRACT Bacterial elongation factor Tu (EF-Tu) and EF-Ts are interacting proteins involved in polypeptide chain elongation in protein biosynthesis. A novel scintillation proximity assay for the detection of inhibitors of EF-Tu and EF-Ts, as well as the interaction between them, was developed and used in a high-throughput screen of a chemical library. Several compounds from a variety of chemical series with inhibitory properties were identified, including certain indole dipeptides, benzimidazole amidines, 2-arylbenzimidazoles, N-substituted imidazoles, and N-substituted guanidines. The in vitro activities of these compounds were confirmed in a coupled bacterial transcription-translation assay. Several indole dipeptides were identified as inhibitors of bacterial translation, with compound 2 exhibiting a 50% inhibitory concentration of 14 μM and an MIC for S. aureus ATCC 29213 of 5.6 μg/ml. Structure-activity relationship studies around the dipeptidic indoles generated additional analogs with low micromolar MICs for both gram-negative and gram-positive bacteria. To assess the specificity of antibacterial action, these compounds were evaluated in a metabolic labeling assay with Staphylococcus aureus . Inhibition of translation, as well as limited effects on other macromolecular pathways for some of the analogs studied, indicated a possible contribution from a non-target-based antibacterial mechanism of action.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology

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