A Metabolic Intermediate of the Fructose-asparagine Utilization Pathway Inhibits Growth of a Salmonella FraB Mutant

Overview

Journal Sci Rep

Specialty Science

Date 2016 Jul 13

PMID 27403719

Citations 16

Authors

Anice Sabag-Daigle

Henry M Blunk

Anindita Sengupta

Jikang Wu

Alexander J Bogard

Mohamed M Ali

Christopher Stahl

Vicki H Wysocki

Venkat Gopalan

Edward J Behrman

Brian M M Ahmer

Affiliations

Soon will be listed here.

Abstract

Insertions in the Salmonella enterica fra locus, which encodes the fructose-asparagine (F-Asn) utilization pathway, are highly attenuated in mouse models of inflammation (>1000-fold competitive index). Here, we report that F-Asn is bacteriostatic to a fraB mutant (IC50 19 μM), but not to the wild-type or a fra island deletion mutant. We hypothesized that the presence of FraD kinase and absence of FraB deglycase causes build-up of a toxic metabolite: 6-phosphofructose-aspartate (6-P-F-Asp). We used biochemical assays to assess FraB and FraD activities, and mass spectrometry to confirm that the fraB mutant accumulates 6-P-F-Asp. These results, together with our finding that mutants lacking fraD or the fra island are not attenuated in mice, suggest that the extreme attenuation of a fraB mutant stems from 6-P-F-Asp toxicity. Salmonella FraB is therefore an excellent drug target, a prospect strengthened by the absence of the fra locus in most of the gut microbiota.

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