A Hypervariable 130-Kilobase Genomic Region of Magnetospirillum gryphiswaldense Comprises a Magnetosome Island Which Undergoes Frequent Rearrangements during Stationary Growth

doi:10.1128/JB.187.21.7176-7184.2005

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Journal of Bacteriology, November 2005, p. 7176-7184, Vol. 187, No. 21
0021-9193/05/$08.00+0 doi:10.1128/JB.187.21.7176-7184.2005
Copyright © 2005, American Society for Microbiology. All Rights Reserved.

A Hypervariable 130-Kilobase Genomic Region of Magnetospirillum gryphiswaldense Comprises a Magnetosome Island Which Undergoes Frequent Rearrangements during Stationary Growth

Susanne Ullrich,¹ Michael Kube,² Sabrina Schübbe,¹ Richard Reinhardt,² and Dirk Schüler¹^*

Max Planck Institute for Marine Microbiology, Celsiusstr. 1, 28359 Bremen, Germany,¹ Max Planck Institute for Molecular Genetics, Ihnestr. 73, 14195 Berlin, Germany²

Received 31 May 2005/ Accepted 16 July 2005

Genes involved in magnetite biomineralization are clusteredin the genome of the magnetotactic bacterium Magnetospirillumgryphiswaldense. We analyzed a 482-kb genomic fragment, in whichwe identified an approximately 130-kb region representing aputative genomic "magnetosome island" (MAI). In addition toall known magnetosome genes, the MAI contains genes putativelyinvolved in magnetosome biomineralization and numerous geneswith unknown functions, as well as pseudogenes, and it is particularlyrich in insertion elements. Substantial sequence polymorphismof clones from different subcultures indicated that this regionundergoes frequent rearrangements during serial subcultivationin the laboratory. Spontaneous mutants affected in magnetosomeformation arise at a frequency of up to 10^–2 after prolongedstorage of cells at 4°C or exposure to oxidative stress.All nonmagnetic mutants exhibited extended and multiple deletionsin the MAI and had lost either parts of or the entire mms andmam gene clusters encoding magnetosome proteins. The mutationswere polymorphic with respect to the sites and extents of deletions,but all mutations were found to be associated with the lossof various copies of insertion elements, as revealed by Southernhybridization and PCR analysis. Insertions and deletions inthe MAI were also found in different magnetosome-producing clones,indicating that parts of this region are not essential for themagnetic phenotype. Our data suggest that the genomic MAI undergoesfrequent transposition events, which lead to subsequent deletionby homologous recombination under physiological stress conditions.This can be interpreted in terms of adaptation to physiologicalstress and might contribute to the genetic plasticity and mobilizationof the magnetosome island.

* Corresponding author. Mailing address: MPI für Marine Mikrobiologie, Celsiusstr. 1, 28359 Bremen, Germany. Phone: 49-(0)421-2028-746. Fax: 49-(0)421-2028-580. E-mail: dschuele{at}mpi-bremen.de.

Journal of Bacteriology, November 2005, p. 7176-7184, Vol. 187, No. 21
0021-9193/05/$08.00+0 doi:10.1128/JB.187.21.7176-7184.2005
Copyright © 2005, American Society for Microbiology. All Rights Reserved.

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