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Optical mapping as a routine tool for bacterial genome sequence finishing

Authors :: Brad Barbazuk
Zijin Du
Sophie Gaudriault
Helge B. Bode
Barry S. Goldman
John Henkhaus
Steven C. Slater
Steve Forst
Brad Goodner
Heidi Goodrich-Blair
Stacie Norton
Phil Latreille
Nancy M. Miller
Creg Darby
Monsanto Company
OpGen Technologies
Partenaires INRAE
Donald Danforth Plant Science Center
Saarland University [Saarbrücken]
University of California [San Francisco] (UCSF)
University of California
Department of Biological Sciences
The Open University [Milton Keynes] (OU)
Ecologie microbienne des insectes et interactions hôte-pathogène (EMIP)
Institut National de la Recherche Agronomique (INRA)-Université Montpellier 2 - Sciences et Techniques (UM2)
Hiram College
Department of Bacteriology
Veterinary Laboratories Agency
Arizona State University [Tempe] (ASU)
Source :: BMC Genomics, BMC Genomics, BioMed Central, 2007, 8, pp.321. ⟨10.1186/1471-2164-8-321⟩, BMC Genomics, Vol 8, Iss 1, p 321 (2007), BMC Genomics (8), 321. (2007)
Publisher :: Springer Nature
Abstract: Background In sequencing the genomes of two Xenorhabdus species, we encountered a large number of sequence repeats and assembly anomalies that stalled finishing efforts. This included a stretch of about 12 Kb that is over 99.9% identical between the plasmid and chromosome of X. nematophila. Results Whole genome restriction maps of the sequenced strains were produced through optical mapping technology. These maps allowed rapid resolution of sequence assembly problems, permitted closing of the genome, and allowed correction of a large inversion in a genome assembly that we had considered finished. Conclusion Our experience suggests that routine use of optical mapping in bacterial genome sequence finishing is warranted. When combined with data produced through 454 sequencing, an optical map can rapidly and inexpensively generate an ordered and oriented set of contigs to produce a nearly complete genome sequence assembly.