Quantitative drug susceptibility testing for Mycobacterium tuberculosis using unassembled sequencing data and machine learning

The CRyPTIC Consortium

doi:10.1371/journal.pcbi.1012260

Quantitative drug susceptibility testing for Mycobacterium tuberculosis using unassembled sequencing data and machine learning

The CRyPTIC Consortium

University of Oxford
Research Center Borstel - Leibniz Lung Center
IRCCS San Raffaele Scientific Institute
Instituto Oswaldo Cruz
Instituto Adolfo Lutz
Stanford University
Scottish Mycobacteria Reference Laboratory
Yale University
Universidad Peruana Cayetano Heredia
Wadsworth Center for Laboratories and Research
Chinese Center for Disease Control and Prevention
Bill and Melinda Gates Foundation
UK Health Security Agency
Vita-Salute San Raffaele University
University College London
The University of Sydney
Public Health Agency of Sweden
University of British Columbia
Public Health Ontario
SYNLAB Gauting
WHO-SRL
European Molecular Biology Laboratory
National Health Laboratory Services
Taiwan Centers for Disease Control
P.D. Hinduja National Hospital and Medical Research Centre
University of Cape Town
University of Surrey
Imperial College London
University of Montreal
Instituto Nacional de Salud, Lima
The Foundation for Medical Research India
Africa Health Research Institute
London School of Hygiene and Tropical Medicine
German Center for Infection Research (DZIF)
National University of Singapore
Institut Pasteur de Madagascar
FIND
University of California at San Diego
Center for Infection and Immunity of Lille (CIIL)
National TB Control Program
University of Antwerp
University of Edinburgh
Stellenbosch University
Wellcome Centre for Infectious Diseases Research in Africa
Francis Crick Institute
CAS - Institute of Microbiology
University of Belgrade
National Academy of Medical Sciences of Ukraine
Liverpool School of Tropical Medicine
Biomedicine Institute of Valencia IBV-CSIC
University Medical Hospital Schleswig-Holstein
University of Melbourne
Harvard Medical School
Irish Mycobacteria Reference Laboratory
Universidad de Valencia
Pham NgocThach Hospital
Monash University
Baker Heart and Diabetes Institute
National Institute of Diseases of the Chest and Hospital
Belgian Reference Laboratory for M. Tuberculosis
Trinity College Dublin
Azienda Ospedaliera Careggi
Republican Scientific and Practical Centre for Pulmonology and TB
National Institute of Public Health and the Environment
Leeds Teaching Hospitals NHS Trust
World Health Organization

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4 Citas (Scopus)

Resumen

There remains a clinical need for better approaches to rapid drug susceptibility testing in view of the increasing burden of multidrug resistant tuberculosis. Binary susceptibility phenotypes only capture changes in minimum inhibitory concentration when these cross the critical concentration, even though other changes may be clinically relevant. We developed a machine learning system to predict minimum inhibitory concentration from unassembled whole-genome sequencing data for 13 anti-tuberculosis drugs. We trained, validated and tested the system on 10,859 isolates from the CRyPTIC dataset. Essential agreement rates (predicted MIC within one doubling dilution of observed MIC) were above 92% for first-line drugs, 91% for fluoroquinolones and aminoglycosides, and 90% for new and repurposed drugs, albeit with a significant drop in performance for the very few phenotypically resistant isolates in the latter group. To further validate the model in the absence of external MIC datasets, we predicted MIC and converted values to binary for an external set of 15,239 isolates with binary phenotypes, and compare their performance against a previously validated mutation catalogue, the expected performance of existing molecular assays, and World Health Organization Target Product Profiles. The sensitivity of the model on the external dataset was greater than 90% for all drugs except ethionamide, clofazimine and linezolid. Specificity was greater than 95% for all drugs except ethambutol, ethionamide, bedaquiline, delamanid and clofazimine. The proposed system can provide quantitative susceptibility phenotyping to help guide antimicrobial therapy, although further data collection and validation are required before machine learning can be used clinically for all drugs.

Idioma original	Inglés
Número de artículo	e1012260
Publicación	PLoS Computational Biology
Volumen	20
N.º	8 August
DOI	https://doi.org/10.1371/journal.pcbi.1012260
Estado	Publicada - ago. 2024
Publicado de forma externa	Sí

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title = "Quantitative drug susceptibility testing for Mycobacterium tuberculosis using unassembled sequencing data and machine learning",

abstract = "There remains a clinical need for better approaches to rapid drug susceptibility testing in view of the increasing burden of multidrug resistant tuberculosis. Binary susceptibility phenotypes only capture changes in minimum inhibitory concentration when these cross the critical concentration, even though other changes may be clinically relevant. We developed a machine learning system to predict minimum inhibitory concentration from unassembled whole-genome sequencing data for 13 anti-tuberculosis drugs. We trained, validated and tested the system on 10,859 isolates from the CRyPTIC dataset. Essential agreement rates (predicted MIC within one doubling dilution of observed MIC) were above 92\% for first-line drugs, 91\% for fluoroquinolones and aminoglycosides, and 90\% for new and repurposed drugs, albeit with a significant drop in performance for the very few phenotypically resistant isolates in the latter group. To further validate the model in the absence of external MIC datasets, we predicted MIC and converted values to binary for an external set of 15,239 isolates with binary phenotypes, and compare their performance against a previously validated mutation catalogue, the expected performance of existing molecular assays, and World Health Organization Target Product Profiles. The sensitivity of the model on the external dataset was greater than 90\% for all drugs except ethionamide, clofazimine and linezolid. Specificity was greater than 95\% for all drugs except ethambutol, ethionamide, bedaquiline, delamanid and clofazimine. The proposed system can provide quantitative susceptibility phenotyping to help guide antimicrobial therapy, although further data collection and validation are required before machine learning can be used clinically for all drugs.",

author = "\{The CRyPTIC Consortium\} and Lachapelle, \{Alexander S.\} and Ivan Barilar and Simone Battaglia and Emanuele Borroni and Brandao, \{Angela P.\} and Alice Brankin and Cabibbe, \{Andrea Maurizio\} and Joshua Carter and Cirillo, \{Daniela Maria\} and Pauline Claxton and Clifton, \{David A.\} and Ted Cohen and Jorge Coronel and Crook, \{Derrick W.\} and Viola Dreyer and Earle, \{Sarah G.\} and Vincent Escuyer and Lucilaine Ferrazoli and Fowler, \{Philip W.\} and Gao, \{George Fu\} and Jennifer Gardy and Saheer Gharbia and Ghisi, \{Kelen T.\} and Arash Ghodousi and Cruz, \{Ana Lu{\'i}za Gibertoni\} and Louis Grandjean and Clara Grazian and Ramona Groenheit and Guthrie, \{Jennifer L.\} and Wencong He and Harald Hoffmann and Hoosdally, \{Sarah J.\} and Martin Hunt and Zamin Iqbal and Ismail, \{Nazir Ahmed\} and Lisa Jarrett and Lavania Joseph and Ruwen Jou and Priti Kambli and Rukhsar Khot and Jeff Knaggs and Anastasia Koch and Donna Kohlerschmidt and Samaneh Kouchaki and Ajit Lalvani and Lapierre, \{Simon Grandjean\} and Laurenson, \{Ian F.\} and Brice Letcher and Lin, \{Wan Hsuan\} and Puyen, \{Zully M.\}",

note = "Publisher Copyright: {\textcopyright} 2024 The CRyPTIC consortium. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.",

year = "2024",

month = aug,

doi = "10.1371/journal.pcbi.1012260",

language = "Ingl{\'e}s",

volume = "20",

journal = "PLoS Computational Biology",

issn = "1553-734X",

publisher = "Public Library of Science",

number = "8 August",

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TY - JOUR

T1 - Quantitative drug susceptibility testing for Mycobacterium tuberculosis using unassembled sequencing data and machine learning

AU - The CRyPTIC Consortium

AU - Lachapelle, Alexander S.

AU - Barilar, Ivan

AU - Battaglia, Simone

AU - Borroni, Emanuele

AU - Brandao, Angela P.

AU - Brankin, Alice

AU - Cabibbe, Andrea Maurizio

AU - Carter, Joshua

AU - Cirillo, Daniela Maria

AU - Claxton, Pauline

AU - Clifton, David A.

AU - Cohen, Ted

AU - Coronel, Jorge

AU - Crook, Derrick W.

AU - Dreyer, Viola

AU - Earle, Sarah G.

AU - Escuyer, Vincent

AU - Ferrazoli, Lucilaine

AU - Fowler, Philip W.

AU - Gao, George Fu

AU - Gardy, Jennifer

AU - Gharbia, Saheer

AU - Ghisi, Kelen T.

AU - Ghodousi, Arash

AU - Cruz, Ana Luíza Gibertoni

AU - Grandjean, Louis

AU - Grazian, Clara

AU - Groenheit, Ramona

AU - Guthrie, Jennifer L.

AU - He, Wencong

AU - Hoffmann, Harald

AU - Hoosdally, Sarah J.

AU - Hunt, Martin

AU - Iqbal, Zamin

AU - Ismail, Nazir Ahmed

AU - Jarrett, Lisa

AU - Joseph, Lavania

AU - Jou, Ruwen

AU - Kambli, Priti

AU - Khot, Rukhsar

AU - Knaggs, Jeff

AU - Koch, Anastasia

AU - Kohlerschmidt, Donna

AU - Kouchaki, Samaneh

AU - Lalvani, Ajit

AU - Lapierre, Simon Grandjean

AU - Laurenson, Ian F.

AU - Letcher, Brice

AU - Lin, Wan Hsuan

AU - Puyen, Zully M.

N1 - Publisher Copyright: © 2024 The CRyPTIC consortium. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

PY - 2024/8

Y1 - 2024/8

N2 - There remains a clinical need for better approaches to rapid drug susceptibility testing in view of the increasing burden of multidrug resistant tuberculosis. Binary susceptibility phenotypes only capture changes in minimum inhibitory concentration when these cross the critical concentration, even though other changes may be clinically relevant. We developed a machine learning system to predict minimum inhibitory concentration from unassembled whole-genome sequencing data for 13 anti-tuberculosis drugs. We trained, validated and tested the system on 10,859 isolates from the CRyPTIC dataset. Essential agreement rates (predicted MIC within one doubling dilution of observed MIC) were above 92% for first-line drugs, 91% for fluoroquinolones and aminoglycosides, and 90% for new and repurposed drugs, albeit with a significant drop in performance for the very few phenotypically resistant isolates in the latter group. To further validate the model in the absence of external MIC datasets, we predicted MIC and converted values to binary for an external set of 15,239 isolates with binary phenotypes, and compare their performance against a previously validated mutation catalogue, the expected performance of existing molecular assays, and World Health Organization Target Product Profiles. The sensitivity of the model on the external dataset was greater than 90% for all drugs except ethionamide, clofazimine and linezolid. Specificity was greater than 95% for all drugs except ethambutol, ethionamide, bedaquiline, delamanid and clofazimine. The proposed system can provide quantitative susceptibility phenotyping to help guide antimicrobial therapy, although further data collection and validation are required before machine learning can be used clinically for all drugs.

AB - There remains a clinical need for better approaches to rapid drug susceptibility testing in view of the increasing burden of multidrug resistant tuberculosis. Binary susceptibility phenotypes only capture changes in minimum inhibitory concentration when these cross the critical concentration, even though other changes may be clinically relevant. We developed a machine learning system to predict minimum inhibitory concentration from unassembled whole-genome sequencing data for 13 anti-tuberculosis drugs. We trained, validated and tested the system on 10,859 isolates from the CRyPTIC dataset. Essential agreement rates (predicted MIC within one doubling dilution of observed MIC) were above 92% for first-line drugs, 91% for fluoroquinolones and aminoglycosides, and 90% for new and repurposed drugs, albeit with a significant drop in performance for the very few phenotypically resistant isolates in the latter group. To further validate the model in the absence of external MIC datasets, we predicted MIC and converted values to binary for an external set of 15,239 isolates with binary phenotypes, and compare their performance against a previously validated mutation catalogue, the expected performance of existing molecular assays, and World Health Organization Target Product Profiles. The sensitivity of the model on the external dataset was greater than 90% for all drugs except ethionamide, clofazimine and linezolid. Specificity was greater than 95% for all drugs except ethambutol, ethionamide, bedaquiline, delamanid and clofazimine. The proposed system can provide quantitative susceptibility phenotyping to help guide antimicrobial therapy, although further data collection and validation are required before machine learning can be used clinically for all drugs.

UR - https://www.scopus.com/pages/publications/85200992115

U2 - 10.1371/journal.pcbi.1012260

DO - 10.1371/journal.pcbi.1012260

M3 - Artículo

C2 - 39102420

AN - SCOPUS:85200992115

SN - 1553-734X

VL - 20

JO - PLoS Computational Biology

JF - PLoS Computational Biology

IS - 8 August

M1 - e1012260

ER -

Quantitative drug susceptibility testing for Mycobacterium tuberculosis using unassembled sequencing data and machine learning

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