Author:
Aron Zachary D.,Mehrani Atousa,Hoffer Eric D.,Connolly Kristie L.,Torhan Matthew C.,Alumasa John N.,Srinivas Pooja,Cabrera Mynthia,Hosangadi Divya,Barbor Jay S.,Cardinale Steven C.,Kwasny Steven M.,Morin Lucas R.,Butler Michelle M.,Opperman Timothy J.,Bowlin Terry L.,Jerse Ann,Stagg Scott M.,Dunham Christine M.,Keiler Kenneth C.
Abstract
AbstractThe trans-translation pathway for rescuing stalled ribosomes is conserved and essential in bacterial pathogens but has no mammalian homolog, making it an ideal target for new antibiotics. We previously reported the discovery of a family of acylaminooxadiazoles that selectively inhibit trans-translation, resulting in broad-spectrum antibiotic activity. Optimization of the pharmacokinetic and antibiotic properties of the acylaminooxadiazoles produced MBX-4132, which cleared multiple-drug resistant Neisseria gonorrhoeae infection in mice after a single oral dose. Cryo-EM studies of non-stop ribosomes showed that acylaminooxadiazoles bind to a unique site near the peptidyl-transfer center and significantly alter the conformation of ribosomal protein L27, suggesting a novel mechanism for specific inhibition of trans-translation by these molecules.One Sentence SummaryRibosome rescue inhibitors reveal a new conformation of the ribosome and kill drug-resistant Neisseria gonorrhoeae in vivo.
Publisher
Cold Spring Harbor Laboratory
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1. Ribosome Rescue Pathways in Bacteria;Frontiers in Microbiology;2021-03-18