Targeting Iron - Respiratory Reciprocity Promotes Bacterial Death

Author:

Sharifian Gh. MohammadORCID,Norouzi FatemehORCID,Sorci MircoORCID,Zaid Tanweer S,Pier Gerald B.ORCID,Achimovich Alecia,Ongwae George M.ORCID,Liang Binyong,Ryan Margaret,Lemke Michael,Belfort GeorgesORCID,Gadjeva MihaelaORCID,Gahlmann AndreasORCID,Pires Marcos M.ORCID,Venter HenriettaORCID,Harris Thurl E.ORCID,Laurie Gordon W.ORCID

Abstract

ABSTRACTDiscovering new bacterial signaling pathways offers unique antibiotic strategies. Here, through an unbiased resistance screen of 3,884 gene knockout strains, we uncovered a previously unknown non-lytic bactericidal mechanism that sequentially couples three transporters and downstream transcription to lethally suppress respiration of the highly virulentP. aeruginosastrain PA14 - one of three species on the WHO’s ‘Priority 1: Critical’ list. By targeting outer membrane YaiW, cationic lacritin peptide ‘N-104’ translocates into the periplasm where it ligates outer loops 4 and 2 of the inner membrane transporters FeoB and PotH, respectively, to suppress both ferrous iron and polyamine uptake. This broadly shuts down transcription of many biofilm-associated genes, including ferrous iron-dependent TauD and ExbB1. The mechanism is innate to the surface of the eye and is enhanced by synergistic coupling with thrombin peptide GKY20. This is the first example of an inhibitor of multiple bacterial transporters.

Publisher

Cold Spring Harbor Laboratory

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