Mobile elements drive recombination hotspots in the core genome of Staphylococcus aureus

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作者
Richard G. Everitt
Xavier Didelot
Elizabeth M. Batty
Ruth R Miller
Kyle Knox
Bernadette C. Young
Rory Bowden
Adam Auton
Antonina Votintseva
Hanna Larner-Svensson
Jane Charlesworth
Tanya Golubchik
Camilla L. C. Ip
Heather Godwin
Rowena Fung
Tim E. A. Peto
A. Sarah Walker
Derrick W. Crook
Daniel J. Wilson
机构
[1] University of Oxford,Nuffield Department of Medicine
[2] John Radcliffe Hospital,Department of Statistics
[3] University of Oxford,Department of Primary Care Health Sciences
[4] Wellcome Trust Centre for Human Genetics,undefined
[5] Roosevelt Drive,undefined
[6] University of Oxford,undefined
[7] Oxford University Hospitals National Health Service Trust,undefined
[8] John Radcliffe Hospital,undefined
[9] Present addresses: Department of Mathematics and Statistics,undefined
[10] University of Reading,undefined
[11] Reading RG6 6AX,undefined
[12] UK (R.G.V.),undefined
[13] Present addresses: Department of Infectious Disease Epidemiology,undefined
[14] Imperial College,undefined
[15] London SW7 2AZ,undefined
[16] UK (X.D.),undefined
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Horizontal gene transfer is an important driver of bacterial evolution, but genetic exchange in the core genome of clonal species, including the major pathogen Staphylococcus aureus, is incompletely understood. Here we reveal widespread homologous recombination in S. aureus at the species level, in contrast to its near-complete absence between closely related strains. We discover a patchwork of hotspots and coldspots at fine scales falling against a backdrop of broad-scale trends in rate variation. Over megabases, homoplasy rates fluctuate 1.9-fold, peaking towards the origin-of-replication. Over kilobases, we find core recombination hotspots of up to 2.5-fold enrichment situated near fault lines in the genome associated with mobile elements. The strongest hotspots include regions flanking conjugative transposon ICE6013, the staphylococcal cassette chromosome (SCC) and genomic island νSaα. Mobile element-driven core genome transfer represents an opportunity for adaptation and challenges our understanding of the recombination landscape in predominantly clonal pathogens, with important implications for genotype–phenotype mapping.
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