Structural basis for potent inhibitory activity of the antibiotic tigecycline during protein synthesis.

Overview

abstract

Here we present an X-ray crystallography structure of the clinically relevant tigecycline antibiotic bound to the 70S ribosome. Our structural and biochemical analysis indicate that the enhanced potency of tigecycline results from a stacking interaction with nucleobase C1054 within the decoding site of the ribosome. Single-molecule fluorescence resonance energy transfer studies reveal that, during decoding, tigecycline inhibits the initial codon recognition step of tRNA accommodation and prevents rescue by the tetracycline-resistance protein TetM.

authors

Jenner, Lasse

Starosta, Agata L

Terry, Daniel S

Mikolajka, Aleksandra

Filonava, Liudmila

Yusupov, Marat

Blanchard, Scott C.
Wilson, Daniel N
Yusupova, Gulnara

publication date

February 19, 2013

published in

Proceedings of the National Academy of Sciences of the United States of America Journal

Research

keywords

Anti-Bacterial Agents
Minocycline

Identity

PubMed Central ID

PMC3593886

Scopus Document Identifier

84874605802

Digital Object Identifier (DOI)

10.1073/pnas.1216691110

PubMed ID

23431179

Additional Document Info

has global citation frequency

148

volume

110

issue

10

VIVO Weill Cornell Medical College

Structural basis for potent inhibitory activity of the antibiotic tigecycline during protein synthesis. Academic Article

Overview

abstract

authors

publication date

published in

Research

keywords

Identity

PubMed Central ID

Scopus Document Identifier

Digital Object Identifier (DOI)

PubMed ID

Additional Document Info

has global citation frequency

volume

issue