Structure–function studies of acinetobactin analogs

Justin A. Shapiro; Timothy A. Wencewicz

doi:10.1039/C7MT00064B

Structure–function studies of acinetobactin analogs†

Justin A. Shapiro^a and Timothy A. Wencewicz

*^a

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^a Department of Chemistry, Washington University in St. Louis, One Brookings Drive, St. Louis, MO, USA
E-mail: wencewicz@wustl.edu
Fax: +314-935-6530
Tel: +314-935-7247

Abstract

Pathogenic Acinetobacter baumannii excrete the siderophore pre-acinetobactin as an iron-scavenging virulence factor. Pre-acinetobactin is a 2,3-dihydroxy-phenyl oxazoline that undergoes pH-dependent isomerization to the isooxazolidinone form acinetobactin in order to expand the pH range for iron acquisition by A. baumannii. In this study we establish important structure–function relationships for the kinetics of isomerization, iron(III) binding, and siderophore utilization by A. baumannii. We showed that electronic properties of the phenyl oxazoline influence isomerization kinetics and iron(III) binding. We found that iron(III) chelation was directly correlated with A. baumannii utilization. Our studies provide important structural and mechanistic insight for understanding how pathogenic A. baumannii uses pre-acinetobactin as a 2-for-1 iron-scavenging siderophore virulence factor.

This article is part of the themed collection: Metallomics Recent HOT articles

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Structure–function studies of acinetobactin analogs†

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