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Computational identification of a systemic antibiotic for gram-negative bacteria

Nature Microbiology. 2016-07; 
Ryan D. Miller; Akira Iinishi; Seyed Majed Modaresi; Byung-Kuk Yoo; Thomas D. Curtis; Patrick J. Lariviere; Libang Liang; Sangkeun Son; Samantha Nicolau; Rachel Bargabos; Madeleine Morrissette; Michael F. Gates; Norman Pitt; Roman P. Jakob; Parthasarathi Rath; Timm Maier; Andrey G. Malyutin; Jens T. Kaiser; Samantha Niles; Blake Karavas; Meghan Ghiglieri; Sarah E. J. Bowman; Douglas C. Rees; Sebastian Hiller; Kim Lewis
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Peptide Synthesis where the activity of BAM-folded OmpT was quantified by cleavage of the self-quenching fluorogenic reporter peptide Abz-Ala-Arg-Arg-Ala-Tyr(NO2)-NH2 (GenScript). The BAM complex was presented in OMVs, and the functional assay was otherwise performed as previously described 40 , 79 , 80 . In brief, BAM-OMVs pre- Get A Quote

摘要

Discovery of antibiotics acting against Gram-negative species is uniquely challenging due to their restrictive penetration barrier. BamA, which inserts proteins into the outer membrane, is an attractive target due to its surface location. Darobactins produced by Photorhabdus , a nematode gut microbiome symbiont, target BamA. We reasoned that a computational search for genes only distantly related to the darobactin operon may lead to novel compounds. Following this clue, we identified dynobactin A, a novel peptide antibiotic from Photorhabdus australis containing two unlinked rings. Dynobactin is structurally unrelated to darobactins, but also targets BamA. Based on a BamA-dynobactin co-crystal structure and a B... More

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