Abstract

BackgroundYersinia pseudotuberculosis is a zoonotic pathogen, causing mild gastrointestinal infection in humans. From this comparatively benign pathogenic species emerged the highly virulent plague bacillus, Yersinia pestis, which has experienced significant genetic divergence in a relatively short time span. Much of our knowledge of Yersinia spp. evolution stems from genomic comparison and gene expression studies. Here we apply transposon-directed insertion site sequencing (TraDIS) to describe the essential gene set of Y. pseudotuberculosis IP32953 in optimised in vitro growth conditions, and contrast these with the published essential genes of Y. pestis.ResultsThe essential genes of an organism are the core genetic elements required for basic survival processes in a given growth condition, and are therefore attractive targets for antimicrobials. One such gene we identified is yptb3665, which encodes a peptide deformylase, and here we report for the first time, the sensitivity of Y. pseudotuberculosis to actinonin, a deformylase inhibitor. Comparison of the essential genes of Y. pseudotuberculosis with those of Y. pestis revealed the genes whose importance are shared by both species, as well as genes that were differentially required for growth. In particular, we find that the two species uniquely rely upon different iron acquisition and respiratory metabolic pathways under similar in vitro conditions.ConclusionsThe discovery of uniquely essential genes between the closely related Yersinia spp. represent some of the fundamental, species-defining points of divergence that arose during the evolution of Y. pestis from its ancestor. Furthermore, the shared essential genes represent ideal candidates for the development of novel antimicrobials against both species.

Highlights

  • Yersinia pseudotuberculosis is a zoonotic pathogen, causing mild gastrointestinal infection in humans

  • We demonstrate the efficacy of actinonin, a deformylase inhibitor, against Y. pseudotuberculosis based on the discovery that peptide deformylase, yptb3665, is required for growth in vitro

  • The Ez-Tn5-Kan transposome complex was used to generate a library of approximately 40,000 mutants in Y. pseudotuberculosis IP32953

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Summary

Introduction

Yersinia pseudotuberculosis is a zoonotic pathogen, causing mild gastrointestinal infection in humans From this comparatively benign pathogenic species emerged the highly virulent plague bacillus, Yersinia pestis, which has experienced significant genetic divergence in a relatively short time span. Yersinia pseudotuberculosis can colonise a wide range of animal and bird hosts, from which human infection can arise causing gastrointestinal illness. It is an important disease of young cattle in particular, and can result in chronic morbidity, or acute septicaemia, haemorrhagic diarrhoea and death [1]. The study of Y. pseudotuberculosis has added significance because of its genetic similarity to the plague bacillus, Yersinia pestis, a recently emerged and highly virulent species [4]. That strain is itself thought to have emerged from a less virulent ancestor that diverged from Y. pseudotuberculosis about 54,000 years ago.

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