BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Doxorubicin, rs4950928, VEGFA, glucose metabolic process, Allergy to pollen, Neuron)
Bookmark Forward

Mutations in dnaA and a cryptic interaction site increase drug resistance in Mycobacterium tuberculosis.

Nathan D Hicks, Samantha R Giffen, Peter H Culviner, Michael C Chao, Charles L Dulberger, Qingyun Liu, Sydney Stanley, Jessica Brown, Jaimie Sixsmith, Ian D Wolf, Sarah M Fortune

PLoS pathogens 2020 Nov


filter terms:
  • antitubercular agents (2)
  • dnaA (9)
  • dnaa protein, bacteria (1)
  • drug m (1)
  • essential (1)
  • humans (1)
  • isoniazid (5)
  • katG (1)
  • mycobacterium tuberculosis (3)
  • patients (1)
  • phenotypes (1)
  • protein bacteria (1)
  • treatment failure (1)
  • treatment outcomes (1)
  • tuberculosis (5)
    • Sizes of these terms reflect their relevance to your search.

    Genomic dissection of antibiotic resistance in bacterial pathogens has largely focused on genetic changes conferring growth above a single critical concentration of drug. However, reduced susceptibility to antibiotics-even below this breakpoint-is associated with poor treatment outcomes in the clinic, including in tuberculosis. Clinical strains of Mycobacterium tuberculosis exhibit extensive quantitative variation in antibiotic susceptibility but the genetic basis behind this spectrum of drug susceptibility remains ill-defined. Through a genome wide association study, we show that non-synonymous mutations in dnaA, which encodes an essential and highly conserved regulator of DNA replication, are associated with drug resistance in clinical M. tuberculosis strains. We demonstrate that these dnaA mutations specifically enhance M. tuberculosis survival during isoniazid treatment via reduced expression of katG, the activator of isoniazid. To identify DnaA interactors relevant to this phenotype, we perform the first genome-wide biochemical mapping of DnaA binding sites in mycobacteria which reveals a DnaA interaction site that is the target of recurrent mutation in clinical strains. Reconstructing clinically prevalent mutations in this DnaA interaction site reproduces the phenotypes of dnaA mutants, suggesting that clinical strains of M. tuberculosis have evolved mutations in a previously uncharacterized DnaA pathway that quantitatively increases resistance to the key first-line antibiotic isoniazid. Discovering genetic mechanisms that reduce drug susceptibility and support the evolution of high-level drug resistance will guide development of biomarkers capable of prospectively identifying patients at risk of treatment failure in the clinic.

    Citation

    Nathan D Hicks, Samantha R Giffen, Peter H Culviner, Michael C Chao, Charles L Dulberger, Qingyun Liu, Sydney Stanley, Jessica Brown, Jaimie Sixsmith, Ian D Wolf, Sarah M Fortune. Mutations in dnaA and a cryptic interaction site increase drug resistance in Mycobacterium tuberculosis. PLoS pathogens. 2020 Nov;16(11):e1009063

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 33253310

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.