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


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.

SUBMITTER: Jenner L 

PROVIDER: S-EPMC3593886 | biostudies-other | 2013 Mar

REPOSITORIES: biostudies-other

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

Jenner Lasse L   Starosta Agata L AL   Terry Daniel S DS   Mikolajka Aleksandra A   Filonava Liudmila L   Yusupov Marat M   Blanchard Scott C SC   Wilson Daniel N DN   Yusupova Gulnara G  

Proceedings of the National Academy of Sciences of the United States of America 20130219 10


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 prevent  ...[more]

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