BackgroundAn isolate originally labeled Bacillus megaterium CDC 684 was found to contain both pXO1 and pXO2, was non-hemolytic, sensitive to gamma-phage, and produced both the protective antigen and the poly-D-glutamic acid capsule. These phenotypes prompted Ezzell et al., (J. Clin. Microbiol. 28:223) to reclassify this isolate to Bacillus anthracis in 1990.ResultsWe demonstrate that despite these B. anthracis features, the isolate is severely attenuated in a guinea pig model. This prompted whole genome sequencing and closure. The comparative analysis of CDC 684 to other sequenced B. anthracis isolates and further analysis reveals: a) CDC 684 is a close relative of a virulent strain, Vollum A0488; b) CDC 684 defines a new B. anthracis lineage (at least 51 SNPs) that includes 15 other isolates; c) the genome of CDC 684 contains a large chromosomal inversion that spans 3.3 Mbp; d) this inversion has caused a displacement of the usual spatial orientation of the origin of replication (ori) to the termination of replication (ter) from 180&deg; in wild-type B. anthracis to 120&deg; in CDC 684 and e) this isolate also has altered growth kinetics in liquid media.ConclusionsWe propose two alternative hypotheses explaining the attenuated phenotype of this isolate. Hypothesis 1 suggests that the skewed ori/ter relationship in CDC 684 has altered its DNA replication and/or transcriptome processes resulting in altered growth kinetics and virulence capacity. Hypothesis 2 suggests that one or more of the single nucleotide polymorphisms in CDC 684 has altered the expression of a regulatory element or other genes necessary for virulence

Beckstrom-Sternberg, Stephen M.

Challacombe, Jean

Chung, Wai Kwan

Friedlander, Arthur

Gruendike, Jeffrey M.

Hill, Karen K.

Ivins, Bruce E.

Keim, Paul

Munk, Chris

Okinaka, Richard T.

Pearson, Talima

Price, Erin P.

Schupp, James M.

Wolken, Spenser R.

Xie, Gary

PubMed

Background: An isolate originally labeled Bacillus megaterium CDC 684 was found to contain both pXO1 and pXO2, was non-hemolytic, sensitive to gamma-phage, and produced both the protective antigen and the poly-D-glutamic acid capsule. These phenotypes prompted Ezzell et al., (J. Clin. Microbiol. 28:223) to reclassify this isolate to Bacillus anthracis in 1990.Results: We demonstrate that despite these B. anthracis features, the isolate is severely attenuated in a guinea pig model. This prompted whole genome sequencing and closure. The comparative analysis of CDC 684 to other sequenced B. anthracis isolates and further analysis reveals: a) CDC 684 is a close relative of a virulent strain, Vollum A0488; b) CDC 684 defines a new B. anthracis lineage (at least 51 SNPs) that includes 15 other isolates; c) the genome of CDC 684 contains a large chromosomal inversion that spans 3.3 Mbp; d) this inversion has caused a displacement of the usual spatial orientation of the origin of replication (ori) to the termination of replication (ter) from 180° in wild-type B. anthracis to 120° in CDC 684 and e) this isolate also has altered growth kinetics in liquid media.Conclusions: We propose two alternative hypotheses explaining the attenuated phenotype of this isolate. Hypothesis 1 suggests that the skewed ori/ter relationship in CDC 684 has altered its DNA replication and/or transcriptome processes resulting in altered growth kinetics and virulence capacity. Hypothesis 2 suggests that one or more of the single nucleotide polymorphisms in CDC 684 has altered the expression of a regulatory element or other genes necessary for virulence. © 2011 Okinaka et al; licensee BioMed Central Ltd

Okinaka, R T

Price, Erin P

Wolken, S R

Gruendike, J M

Chung, W K

Pearson, T

Xie, G

Munk, C

Hill, K K

Challacombe, J

Ivins, B E

Schupp, J M

Beckstrom-Sternberg, S M

Friedlander, A

Keim, P

USC Research Bank - University of the Sunshine Coast

An attenuated strain of Bacillus anthracis (CDC 684) has a large chromosomal inversion and altered growth kinetics

Richard T Okinaka

Erin P Price

Spenser R Wolken

Jeffrey M Gruendike

Wai Kwan Chung

Talima Pearson

Gary Xie

Chris Munk

Karen K Hill

Jean Challacombe

Bruce E Ivins

James M Schupp

Stephen M Beckstrom-Sternberg

Arthur Friedlander

Paul Keim

Springer - Publisher Connector

An isolate originally labeled Bacillus megaterium CDC 684 was found to contain both pXO1 and pXO2, was non-hemolytic, sensitive to gamma-phage, and produced both the protective antigen and the poly-D-glutamic acid capsule. These phenotypes prompted Ezzell et al., (J. Clin. Microbiol. 28:223) to reclassify this isolate to Bacillus anthracis in 1990. PMID: 2196202

Okinaka, Richard T

Chung, Wai K.

OpenKnowledge@NAU

al: Sequence and organization of pXO1, the large Bacillus anthracis plasmid harboring the anthrax toxin genes.

al: The genome sequence of Bacillus anthracis Ames and comparison to closely related bacteria. Nature

Bacillus anthracis genetics and virulence gene regulation. Curr Top Microbiol Immunol

Base-calling of automated sequencer traces using phred. I. Accuracy assessment. Genome Res

Base-calling of automated sequencer traces using phred. II. Error probabilities. Genome Res

C-A: The dif/Xer Recombination Systems

Characterization of Bacillus anthracis-like bacteria isolated from wild great apes from Cote d’Ivoire and Cameroon. Journal of bacteriology

Characterization of Bacillus cereus isolates associated with fatal pneumonias: strains are closely related to Bacillus anthracis and harbor B. anthracis virulence genes. Journal of clinical microbiology

Cloning and CO2-dependent expression of the genetic region for encapsulation from Bacillus anthracis. Mol Microbiol

Collins RA: Genome rearrangement by replication-directed translocation.

D: dif, a recAindependent recombination site in the terminus region of the chromosome of Escherichia coli. The New biologist

DD: Analysis of the factor V Leiden mutation using the READIT Assay. Mol Diagn

DL: Molecular cloning and expression of the Bacillus anthracis edema factor toxin gene: a calmodulin-dependent adenylate cyclase.

Efficacy of a standard human anthrax vaccine against Bacillus anthracis spore challenge in guinea-pigs. Vaccine

Escherichia coli XerC recombinase is required for chromosomal segregation at cell division. New Biol

et al: Global genetic population structure of Bacillus anthracis. PLoS One

et al: Identification of anthrax toxin genes in a Bacillus cereus associated with an illness resembling inhalation anthrax. Proc Natl Acad Sci USA

et al: Pathogenomic sequence analysis of Bacillus cereus and Bacillus thuringiensis isolates closely related to Bacillus anthracis.

et al: Phylogenetic discovery bias in Bacillus anthracis using single-nucleotide polymorphisms from wholegenome sequencing. Proc Natl Acad Sci USA

Genetic diversity in the protective antigen gene of Bacillus anthracis.

Glucose-dependent activation of Bacillus anthracis toxin gene expression and virulence requires the carbon catabolite protein CcpA.

Hoch JA: Commingling regulatory systems following acquisition of virulence plasmids by Bacillus anthracis. Trends Microbiol

Identification of Bacillus anthracis by using monoclonal antibody to cell wall galactoseN-acetylglucosamine polysaccharide.

Immunization against anthrax with aromatic compound-dependent (Aro-) mutants of Bacillus anthracis and with recombinant strains of Bacillus subtilis that produce anthrax protective antigen. Infection and Immunity

Inhalation anthrax.

Kolsto AB: A complete physical map of a Bacillus thuringiensis chromosome.

Leppla SH: Cloning of the protective antigen gene of Bacillus anthracis. Cell

Mapping and characterization of the Bacillus anthracis plasmids.

MF: Extension of base mispairs by Taq DNA polymerase: implications for single nucleotide discrimination in PCR. Nucleic Acids Res

Monjazeb A: High-throughput single nucleotide polymorphism genotyping by fluorescent 5’ exonuclease assay. Biotechniques

Mutational bias suggests that replication termination occurs near the dif site, not at Ter sites. Molecular Microbiology

Popovic T: Effects of long-term storage on plasmid stability in Bacillus anthracis. Appl Environ Microbiol

Professor Superintendent, The Brown Animal Sanatory Institution (1878-81). J Hyg Camb

Rasooly A: MIcroarray analysis of Bacillus cereus group virulence factors.

Sequence and analysis of the DNA encoding protective antigen of Bacillus anthracis. Gene

SH: Immunization studies with attenuated strains of Bacillus anthracis. Infect Immun

SL: Evidence for symmetric chromosomal inversions around the replication of origin in bacteria. Genome Biology

Stagg AJ: Bacillus anthracis on Gruinard Island. Nature

T: Evidence for plasmid-mediated toxin production in Bacillus anthracis. Infection and immunity

TD: The Bacillus anthracis chromosome contains four conserved, excision-proficient, putative prophages.

The chromosome of Salmonella paratyphi A is inverted by recombination between rrnH and rrnG.

The genome and variation of Bacillus anthracis. Mol Aspects Med

The history of anthrax.

The immunization of laboratory animals against anthrax.

Thilly W: Mismatch amplification mutation assay (MAMA): application to the cH-ras gene. Genome Research

Tseng Y: oriC region and replication termination site, dif, of the Xanthomonas campestris pv. campestris 17 chromosome. Applied and environmental microbiology

Ussery DW: Origins of replication in circular prokaryotic chromosomes. Environmental Microbiology

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An attenuated strain of Bacillus anthracis (CDC 684) has a large chromosomal inversion and altered growth kinetics

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