TY - JOUR
T1 - Bedaquiline and clofazimine resistance in Mycobacterium tuberculosis
T2 - an in-vitro and in-silico data analysis
AU - Comprehensive Resistance Prediction for Tuberculosis: an International Consortium
AU - Sonnenkalb, Lindsay
AU - Carter, Joshua James
AU - Spitaleri, Andrea
AU - Iqbal, Zamin
AU - Hunt, Martin
AU - Malone, Kerri Marie
AU - Utpatel, Christian
AU - Cirillo, Daniela Maria
AU - Rodrigues, Camilla
AU - Nilgiriwala, Kayzad Soli
AU - Fowler, Philip William
AU - Merker, Matthias
AU - Niemann, Stefan
AU - Barilar, Ivan
AU - Battaglia, Simone
AU - Borroni, Emanuele
AU - Brandao, Angela Pires
AU - Brankin, Alice
AU - Cabibbe, Andrea Maurizio
AU - Carter, Joshua
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 - Fu Gao, George
AU - Gardy, Jennifer
AU - Gharbia, Saheer
AU - Ghisi, Kelen Teixeira
AU - Ghodousi, Arash
AU - Gibertoni Cruz, Ana Luíza
AU - Grandjean, Louis
AU - Grazian, Clara
AU - Groenheit, Ramona
AU - Guthrie, Jennifer L.
AU - He, Wencong
AU - Hoffmann, Harald
AU - Hoosdally, Sarah J.
AU - Ismail, Nazir Ahmed
AU - Jarrett, Lisa
AU - Joseph, Lavania
AU - Jou, Ruwen
AU - Kambli, Priti
AU - Rathod, Priti
AU - Smith, Grace
N1 - Publisher Copyright:
© 2023 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license
PY - 2023/5
Y1 - 2023/5
N2 - Background: Bedaquiline is a core drug for the treatment of multidrug-resistant tuberculosis; however, the understanding of resistance mechanisms is poor, which is hampering rapid molecular diagnostics. Some bedaquiline-resistant mutants are also cross-resistant to clofazimine. To decipher bedaquiline and clofazimine resistance determinants, we combined experimental evolution, protein modelling, genome sequencing, and phenotypic data. Methods: For this in-vitro and in-silico data analysis, we used a novel in-vitro evolutionary model using subinhibitory drug concentrations to select bedaquiline-resistant and clofazimine-resistant mutants. We determined bedaquiline and clofazimine minimum inhibitory concentrations and did Illumina and PacBio sequencing to characterise selected mutants and establish a mutation catalogue. This catalogue also includes phenotypic and genotypic data of a global collection of more than 14 000 clinical Mycobacterium tuberculosis complex isolates, and publicly available data. We investigated variants implicated in bedaquiline resistance by protein modelling and dynamic simulations. Findings: We discerned 265 genomic variants implicated in bedaquiline resistance, with 250 (94%) variants affecting the transcriptional repressor (Rv0678) of the MmpS5–MmpL5 efflux system. We identified 40 new variants in vitro, and a new bedaquiline resistance mechanism caused by a large-scale genomic rearrangement. Additionally, we identified in vitro 15 (7%) of 208 mutations found in clinical bedaquiline-resistant isolates. From our in-vitro work, we detected 14 (16%) of 88 mutations so far identified as being associated with clofazimine resistance and also seen in clinically resistant strains, and catalogued 35 new mutations. Structural modelling of Rv0678 showed four major mechanisms of bedaquiline resistance: impaired DNA binding, reduction in protein stability, disruption of protein dimerisation, and alteration in affinity for its fatty acid ligand. Interpretation: Our findings advance the understanding of drug resistance mechanisms in M tuberculosis complex strains. We have established an extended mutation catalogue, comprising variants implicated in resistance and susceptibility to bedaquiline and clofazimine. Our data emphasise that genotypic testing can delineate clinical isolates with borderline phenotypes, which is essential for the design of effective treatments. Funding: Leibniz ScienceCampus Evolutionary Medicine of the Lung, Deutsche Forschungsgemeinschaft, Research Training Group 2501 TransEvo, Rhodes Trust, Stanford University Medical Scientist Training Program, National Institute for Health and Care Research Oxford Biomedical Research Centre, Oxford University Hospitals NHS Foundation Trust, Bill & Melinda Gates Foundation, Wellcome Trust, and Marie Skłodowska-Curie Actions.
AB - Background: Bedaquiline is a core drug for the treatment of multidrug-resistant tuberculosis; however, the understanding of resistance mechanisms is poor, which is hampering rapid molecular diagnostics. Some bedaquiline-resistant mutants are also cross-resistant to clofazimine. To decipher bedaquiline and clofazimine resistance determinants, we combined experimental evolution, protein modelling, genome sequencing, and phenotypic data. Methods: For this in-vitro and in-silico data analysis, we used a novel in-vitro evolutionary model using subinhibitory drug concentrations to select bedaquiline-resistant and clofazimine-resistant mutants. We determined bedaquiline and clofazimine minimum inhibitory concentrations and did Illumina and PacBio sequencing to characterise selected mutants and establish a mutation catalogue. This catalogue also includes phenotypic and genotypic data of a global collection of more than 14 000 clinical Mycobacterium tuberculosis complex isolates, and publicly available data. We investigated variants implicated in bedaquiline resistance by protein modelling and dynamic simulations. Findings: We discerned 265 genomic variants implicated in bedaquiline resistance, with 250 (94%) variants affecting the transcriptional repressor (Rv0678) of the MmpS5–MmpL5 efflux system. We identified 40 new variants in vitro, and a new bedaquiline resistance mechanism caused by a large-scale genomic rearrangement. Additionally, we identified in vitro 15 (7%) of 208 mutations found in clinical bedaquiline-resistant isolates. From our in-vitro work, we detected 14 (16%) of 88 mutations so far identified as being associated with clofazimine resistance and also seen in clinically resistant strains, and catalogued 35 new mutations. Structural modelling of Rv0678 showed four major mechanisms of bedaquiline resistance: impaired DNA binding, reduction in protein stability, disruption of protein dimerisation, and alteration in affinity for its fatty acid ligand. Interpretation: Our findings advance the understanding of drug resistance mechanisms in M tuberculosis complex strains. We have established an extended mutation catalogue, comprising variants implicated in resistance and susceptibility to bedaquiline and clofazimine. Our data emphasise that genotypic testing can delineate clinical isolates with borderline phenotypes, which is essential for the design of effective treatments. Funding: Leibniz ScienceCampus Evolutionary Medicine of the Lung, Deutsche Forschungsgemeinschaft, Research Training Group 2501 TransEvo, Rhodes Trust, Stanford University Medical Scientist Training Program, National Institute for Health and Care Research Oxford Biomedical Research Centre, Oxford University Hospitals NHS Foundation Trust, Bill & Melinda Gates Foundation, Wellcome Trust, and Marie Skłodowska-Curie Actions.
UR - http://www.scopus.com/inward/record.url?scp=85151391800&partnerID=8YFLogxK
U2 - 10.1016/S2666-5247(23)00002-2
DO - 10.1016/S2666-5247(23)00002-2
M3 - Article
AN - SCOPUS:85151391800
SN - 2666-5247
VL - 4
SP - e358-e368
JO - The Lancet Microbe
JF - The Lancet Microbe
IS - 5
ER -
