Litcius/Paper detail

Cellular Stress-Induced Metabolites in <i>Escherichia coli</i>

Alexandra Gatsios, Chung Sub Kim, Autumn G. York, Richard A. Flavell, Jason M. Crawford

2022Journal of Natural Products12 citationsDOIOpen Access PDF

Abstract

Escherichia coli isolates commonly inhabit the human microbiota, yet the majority of E. coli’s small-molecule repertoire remains uncharacterized. We previously employed erythromycin-induced translational stress to facilitate the characterization of autoinducer-3 (AI-3) and structurally related pyrazinones derived from “abortive” tRNA synthetase reactions in pathogenic, commensal, and probiotic E. coli isolates. In this study, we explored the “missing” tryptophan-derived pyrazinone reaction and characterized two other families of metabolites that were similarly upregulated under erythromycin stress. Strikingly, the abortive tryptophanyl-tRNA synthetase reaction leads to a tetracyclic indole alkaloid metabolite (1) rather than a pyrazinone. Furthermore, erythromycin induced two naphthoquinone-functionalized metabolites (MK-hCys, 2; and MK-Cys, 3) and four lumazines (7–10). Using genetic and metabolite analyses coupled with biomimetic synthesis, we provide support that the naphthoquinones are derived from 4-dihydroxy-2-naphthoic acid (DHNA), an intermediate in the menaquinone biosynthetic pathway, and the amino acids homocysteine and cysteine. In contrast, the lumazines are dependent on a flavin intermediate and α-ketoacids from the aminotransferases AspC and TyrB. We show that one of the lumazine members (9), an indole-functionalized analogue, possesses antioxidant properties, modulates the anti-inflammatory fate of isolated TH17 cells, and serves as an aryl-hydrocarbon receptor (AhR) agonist. These three systems described here serve to illustrate that new metabolic branches could be more commonly derived from well-established primary metabolic pathways.

Topics & Concepts

Escherichia coliBiochemistryIndole testBiologyMetaboliteStereochemistryCysteineChemistryEnzymeGeneBioactive Compounds and Antitumor AgentsRNA and protein synthesis mechanismsBacterial Genetics and Biotechnology