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Journal of Clinical Microbiology
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Mycobacteriology and Aerobic Actinomycetes

Rapid Whole-Genome Sequencing of Mycobacterium tuberculosis Isolates Directly from Clinical Samples

Amanda C. Brown, Josephine M. Bryant, Katja Einer-Jensen, Jolyon Holdstock, Darren T. Houniet, Jacqueline Z. M. Chan, Daniel P. Depledge, Vladyslav Nikolayevskyy, Agnieszka Broda, Madeline J. Stone, Mette T. Christiansen, Rachel Williams, Michael B. McAndrew, Helena Tutill, Julianne Brown, Mark Melzer, Caryn Rosmarin, Timothy D. McHugh, Robert J. Shorten, Francis Drobniewski, Graham Speight, Judith Breuer
G. A. Land, Editor
Amanda C. Brown
aOxford Gene Technology, Oxford, United Kingdom
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Josephine M. Bryant
bUCL, Division of Infection and Immunity, London, United Kingdom
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  • ORCID record for Josephine M. Bryant
Katja Einer-Jensen
cQiagen-AAR, Aarhus, Denmark
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Jolyon Holdstock
aOxford Gene Technology, Oxford, United Kingdom
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Darren T. Houniet
aOxford Gene Technology, Oxford, United Kingdom
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Jacqueline Z. M. Chan
aOxford Gene Technology, Oxford, United Kingdom
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Daniel P. Depledge
bUCL, Division of Infection and Immunity, London, United Kingdom
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Vladyslav Nikolayevskyy
dNational Mycobacterium Reference Laboratory (NMRL), ICMS, London, United Kingdom
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Agnieszka Broda
dNational Mycobacterium Reference Laboratory (NMRL), ICMS, London, United Kingdom
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Madeline J. Stone
eDept. Microbiology, Frimley Health NHS Foundation Trust, Wexham Park Hospital, Berkshire, United Kingdom
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Mette T. Christiansen
bUCL, Division of Infection and Immunity, London, United Kingdom
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Rachel Williams
bUCL, Division of Infection and Immunity, London, United Kingdom
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Michael B. McAndrew
aOxford Gene Technology, Oxford, United Kingdom
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Helena Tutill
bUCL, Division of Infection and Immunity, London, United Kingdom
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Julianne Brown
bUCL, Division of Infection and Immunity, London, United Kingdom
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Mark Melzer
fBarts Health NHS Trust, West Smithfield, London, United Kingdom
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Caryn Rosmarin
fBarts Health NHS Trust, West Smithfield, London, United Kingdom
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Timothy D. McHugh
gCentre for Clinical Microbiology, UCL, Royal Free Campus, London, United Kingdom
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Robert J. Shorten
gCentre for Clinical Microbiology, UCL, Royal Free Campus, London, United Kingdom
hSpecialist Microbiology Network, Public Health Laboratory Manchester, Manchester Royal Infirmary, Manchester, United Kingdom
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Francis Drobniewski
dNational Mycobacterium Reference Laboratory (NMRL), ICMS, London, United Kingdom
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Graham Speight
aOxford Gene Technology, Oxford, United Kingdom
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Judith Breuer
bUCL, Division of Infection and Immunity, London, United Kingdom
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G. A. Land
Roles: Editor
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DOI: 10.1128/JCM.00486-15
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ABSTRACT

The rapid identification of antimicrobial resistance is essential for effective treatment of highly resistant Mycobacterium tuberculosis. Whole-genome sequencing provides comprehensive data on resistance mutations and strain typing for monitoring transmission, but unlike for conventional molecular tests, this has previously been achievable only from cultures of M. tuberculosis. Here we describe a method utilizing biotinylated RNA baits designed specifically for M. tuberculosis DNA to capture full M. tuberculosis genomes directly from infected sputum samples, allowing whole-genome sequencing without the requirement of culture. This was carried out on 24 smear-positive sputum samples, collected from the United Kingdom and Lithuania where a matched culture sample was available, and 2 samples that had failed to grow in culture. M. tuberculosis sequencing data were obtained directly from all 24 smear-positive culture-positive sputa, of which 20 were of high quality (>20× depth and >90% of the genome covered). Results were compared with those of conventional molecular and culture-based methods, and high levels of concordance between phenotypical resistance and predicted resistance based on genotype were observed. High-quality sequence data were obtained from one smear-positive culture-negative case. This study demonstrated for the first time the successful and accurate sequencing of M. tuberculosis genomes directly from uncultured sputa. Identification of known resistance mutations within a week of sample receipt offers the prospect for personalized rather than empirical treatment of drug-resistant tuberculosis, including the use of antimicrobial-sparing regimens, leading to improved outcomes.

FOOTNOTES

    • Received 23 February 2015.
    • Returned for modification 3 April 2015.
    • Accepted 23 April 2015.
    • Accepted manuscript posted online 13 May 2015.
  • Supplemental material for this article may be found at http://dx.doi.org/10.1128/JCM.00486-15.

  • Copyright © 2015, American Society for Microbiology. All Rights Reserved.
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Rapid Whole-Genome Sequencing of Mycobacterium tuberculosis Isolates Directly from Clinical Samples
Amanda C. Brown, Josephine M. Bryant, Katja Einer-Jensen, Jolyon Holdstock, Darren T. Houniet, Jacqueline Z. M. Chan, Daniel P. Depledge, Vladyslav Nikolayevskyy, Agnieszka Broda, Madeline J. Stone, Mette T. Christiansen, Rachel Williams, Michael B. McAndrew, Helena Tutill, Julianne Brown, Mark Melzer, Caryn Rosmarin, Timothy D. McHugh, Robert J. Shorten, Francis Drobniewski, Graham Speight, Judith Breuer
Journal of Clinical Microbiology Jun 2015, 53 (7) 2230-2237; DOI: 10.1128/JCM.00486-15

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Rapid Whole-Genome Sequencing of Mycobacterium tuberculosis Isolates Directly from Clinical Samples
Amanda C. Brown, Josephine M. Bryant, Katja Einer-Jensen, Jolyon Holdstock, Darren T. Houniet, Jacqueline Z. M. Chan, Daniel P. Depledge, Vladyslav Nikolayevskyy, Agnieszka Broda, Madeline J. Stone, Mette T. Christiansen, Rachel Williams, Michael B. McAndrew, Helena Tutill, Julianne Brown, Mark Melzer, Caryn Rosmarin, Timothy D. McHugh, Robert J. Shorten, Francis Drobniewski, Graham Speight, Judith Breuer
Journal of Clinical Microbiology Jun 2015, 53 (7) 2230-2237; DOI: 10.1128/JCM.00486-15
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