Peptidomimetic antibiotics disrupt the lipopolysaccharide transport bridge of drug-resistant Enterobacteriaceae

Author:

Schuster Matthias1ORCID,Brabet Emile2ORCID,Oi Kathryn K.1ORCID,Desjonquères Nicolas2,Moehle Kerstin1ORCID,Le Poupon Karen2,Hell Sophie2,Gable Stéphane2,Rithié Virginie2,Dillinger Séverine2,Zbinden Peter2ORCID,Luther Anatol2ORCID,Li Claudia2,Stiegeler Sarah2ORCID,D’Arco Carolin2ORCID,Locher Hans2,Remus Tobias2ORCID,DiMaio Selena2,Motta Paola2ORCID,Wach Achim2ORCID,Jung Françoise2ORCID,Upert Grégory2ORCID,Obrecht Daniel2ORCID,Benghezal Mohammed2ORCID,Zerbe Oliver1ORCID

Affiliation:

1. University of Zürich, Winterthurerstrasse 190, CH-8057 Zürich, Switzerland.

2. Spexis AG, Hegenheimermattweg 125, CH-4112 Allschwil, Switzerland.

Abstract

The rise of antimicrobial resistance poses a substantial threat to our health system, and, hence, development of drugs against novel targets is urgently needed. The natural peptide thanatin kills Gram-negative bacteria by targeting proteins of the lipopolysaccharide transport (Lpt) machinery. Using the thanatin scaffold together with phenotypic medicinal chemistry, structural data, and a target-focused approach, we developed antimicrobial peptides with drug-like properties. They exhibit potent activity against Enterobacteriaceae both in vitro and in vivo while eliciting low frequencies of resistance. We show that the peptides bind LptA of both wild-type and thanatin-resistant Escherichia coli and Klebsiella pneumoniae strains with low-nanomolar affinities. Mode of action studies revealed that the antimicrobial activity involves the specific disruption of the Lpt periplasmic protein bridge.

Publisher

American Association for the Advancement of Science (AAAS)

Subject

Multidisciplinary

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