Cereulide synthetase gene cluster from emetic Bacillus cereus: structure and location on a mega virulence plasmid related to Bacillus anthracis toxin plasmid pXO1

Monika Ehling-Schulz; Martina Fricker; Harald Grallert; Petra Rieck; Martin Wagner; Siegfried Scherer

doi:10.1186/1471-2180-6-20

Cereulide synthetase gene cluster from emetic Bacillus cereus: structure and location on a mega virulence plasmid related to Bacillus anthracis toxin plasmid pXO1

BMC Microbiol. 2006 Mar 2:6:20. doi: 10.1186/1471-2180-6-20.

Authors

Monika Ehling-Schulz¹, Martina Fricker, Harald Grallert, Petra Rieck, Martin Wagner, Siegfried Scherer

Affiliation

¹ Lehrstuhl für Mikrobielle Okologie, Department für Biowissenschaftliche Grundlagen, WZW, Technische Universität München, Freising, Germany. Monika.Ehling-Schulz@wzw.tum.de

Abstract

Background: Cereulide, a depsipeptide structurally related to valinomycin, is responsible for the emetic type of gastrointestinal disease caused by Bacillus cereus. Recently, it has been shown that this toxin is produced by a nonribosomal peptide synthetase (NRPS), but its exact genetic organization and biochemical synthesis is unknown.

Results: The complete sequence of the cereulide synthetase (ces) gene cluster, which encodes the enzymatic machinery required for the biosynthesis of cereulide, was dissected. The 24 kb ces gene cluster comprises 7 CDSs and includes, besides the typical NRPS genes like a phosphopantetheinyl transferase and two CDSs encoding enzyme modules for the activation and incorporation of monomers in the growing peptide chain, a CDS encoding a putative hydrolase in the upstream region and an ABC transporter in the downstream part. The enzyme modules responsible for incorporation of the hydroxyl acids showed an unusual structure while the modules responsible for the activation of the amino acids Ala and Val showed the typical domain organization of NRPS. The ces gene locus is flanked by genetic regions with high homology to virulence plasmids of B. cereus, Bacillus thuringiensis and Bacillus anthracis. PFGE and Southern hybridization showed that the ces genes are restricted to emetic B. cereus and indeed located on a 208 kb megaplasmid, which has high similarities to pXO1-like plasmids.

Conclusion: The ces gene cluster that is located on a pXO1-like virulence plasmid represents, beside the insecticidal and the anthrax toxins, a third type of B. cereus group toxins encoded on megaplasmids. The ces genes are restricted to emetic toxin producers, but pXO1-like plasmids are also present in emetic-like strains. These data might indicate the presence of an ancient plasmid in B. cereus which has acquired different virulence genes over time. Due to the unusual structure of the hydroxyl acid incorporating enzyme modules of Ces, substantial biochemical efforts will be required to dissect the complete biochemical pathway of cereulide synthesis.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Antigens, Bacterial / genetics*
Bacillus anthracis / genetics*
Bacillus anthracis / pathogenicity
Bacillus cereus / genetics*
Bacillus cereus / pathogenicity
Bacterial Toxins / genetics*
Base Sequence
Depsipeptides / biosynthesis*
Electrophoresis, Gel, Pulsed-Field
Molecular Sequence Data
Multigene Family*
Nucleic Acid Hybridization
Operon
Peptide Synthases / genetics*
Plasmids*
Protein Structure, Tertiary
Virulence

Substances

Antigens, Bacterial
Bacterial Toxins
Depsipeptides
anthrax toxin
cereulide
Peptide Synthases
non-ribosomal peptide synthase