Structural Characterization of an Alternative Mode of Tigecycline Binding to the Bacterial Ribosome

Author:

Schedlbauer Andreas,Kaminishi Tatsuya,Ochoa-Lizarralde Borja,Dhimole Neha,Zhou Shu,López-Alonso Jorge P.,Connell Sean R.ORCID,Fucini Paola

Abstract

ABSTRACTAlthough both tetracycline and tigecycline inhibit protein synthesis by sterically hindering the binding of tRNA to the ribosomal A site, tigecycline shows increased efficacy in bothin vitroandin vivoactivity assays and escapes the most common resistance mechanisms associated with the tetracycline class of antibiotics. These differences in activities are attributed to thetert-butyl-glycylamido side chain found in tigecycline. Our structural analysis by X-ray crystallography shows that tigecycline binds the bacterial 30S ribosomal subunit with its tail in an extended conformation and makes extensive interactions with the 16S rRNA nucleotide C1054. These interactions restrict the mobility of C1054 and contribute to the antimicrobial activity of tigecycline, including its resistance to the ribosomal protection proteins.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology

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