Literature DB >> 25432719

Identifying structural variation in haploid microbial genomes from short-read resequencing data using breseq.

Jeffrey E Barrick1, Geoffrey Colburn, Daniel E Deatherage, Charles C Traverse, Matthew D Strand, Jordan J Borges, David B Knoester, Aaron Reba, Austin G Meyer.   

Abstract

BACKGROUND: Mutations that alter chromosomal structure play critical roles in evolution and disease, including in the origin of new lifestyles and pathogenic traits in microbes. Large-scale rearrangements in genomes are often mediated by recombination events involving new or existing copies of mobile genetic elements, recently duplicated genes, or other repetitive sequences. Most current software programs for predicting structural variation from short-read DNA resequencing data are intended primarily for use on human genomes. They typically disregard information in reads mapping to repeat sequences, and significant post-processing and manual examination of their output is often required to rule out false-positive predictions and precisely describe mutational events.
RESULTS: We have implemented an algorithm for identifying structural variation from DNA resequencing data as part of the breseq computational pipeline for predicting mutations in haploid microbial genomes. Our method evaluates the support for new sequence junctions present in a clonal sample from split-read alignments to a reference genome, including matches to repeat sequences. Then, it uses a statistical model of read coverage evenness to accept or reject these predictions. Finally, breseq combines predictions of new junctions and deleted chromosomal regions to output biologically relevant descriptions of mutations and their effects on genes. We demonstrate the performance of breseq on simulated Escherichia coli genomes with deletions generating unique breakpoint sequences, new insertions of mobile genetic elements, and deletions mediated by mobile elements. Then, we reanalyze data from an E. coli K-12 mutation accumulation evolution experiment in which structural variation was not previously identified. Transposon insertions and large-scale chromosomal changes detected by breseq account for ~25% of spontaneous mutations in this strain. In all cases, we find that breseq is able to reliably predict structural variation with modest read-depth coverage of the reference genome (>40-fold).
CONCLUSIONS: Using breseq to predict structural variation should be useful for studies of microbial epidemiology, experimental evolution, synthetic biology, and genetics when a reference genome for a closely related strain is available. In these cases, breseq can discover mutations that may be responsible for important or unintended changes in genomes that might otherwise go undetected.

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Year:  2014        PMID: 25432719      PMCID: PMC4300727          DOI: 10.1186/1471-2164-15-1039

Source DB:  PubMed          Journal:  BMC Genomics        ISSN: 1471-2164            Impact factor:   3.969


  41 in total

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9.  BreakDancer: an algorithm for high-resolution mapping of genomic structural variation.

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  91 in total

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2.  Complex chromosomal neighborhood effects determine the adaptive potential of a gene under selection.

Authors:  Magdalena Steinrueck; Călin C Guet
Journal:  Elife       Date:  2017-07-25       Impact factor: 8.140

3.  Genomic evolution of antibiotic resistance is contingent on genetic background following a long-term experiment with Escherichia coli.

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4.  Cas9-mediated genome editing in the methanogenic archaeon Methanosarcina acetivorans.

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5.  Specificity of genome evolution in experimental populations of Escherichia coli evolved at different temperatures.

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Journal:  Proc Natl Acad Sci U S A       Date:  2017-02-15       Impact factor: 11.205

6.  Testing the Role of Multicopy Plasmids in the Evolution of Antibiotic Resistance.

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7.  Reduced Mutation Rate and Increased Transformability of Transposon-Free Acinetobacter baylyi ADP1-ISx.

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8.  Gene Duplication in Pseudomonas aeruginosa Improves Growth on Adenosine.

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Journal:  J Bacteriol       Date:  2017-10-03       Impact factor: 3.490

9.  Escherichia coli cultures maintain stable subpopulation structure during long-term evolution.

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10.  The birth of a bacterial tRNA gene by large-scale, tandem duplication events.

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