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In vivo evolution of an emerging zoonotic bacterial pathogen in an immunocompromised human host

Author

Listed:
  • A. Launay

    (Bacterial Pathogenesis and Antimicrobial Resistance Unit, LCIM, NIAID)

  • C.-J. Wu

    (Bacterial Pathogenesis and Antimicrobial Resistance Unit, LCIM, NIAID)

  • A. Dulanto Chiang

    (Bacterial Pathogenesis and Antimicrobial Resistance Unit, LCIM, NIAID)

  • J.-H. Youn

    (NIH Clinical Center)

  • P. P. Khil

    (Bacterial Pathogenesis and Antimicrobial Resistance Unit, LCIM, NIAID
    NIH Clinical Center)

  • J. P. Dekker

    (Bacterial Pathogenesis and Antimicrobial Resistance Unit, LCIM, NIAID
    NIH Clinical Center)

Abstract

Zoonotic transfer of animal pathogens to human hosts can generate novel agents, but the genetic events following such host jumps are not well studied. Here we characterize the mechanisms driving adaptive evolution of the emerging zoonotic pathogen Bordetella hinzii in a patient with interleukin-12 receptor β1 deficiency. Genomic sequencing of 24 B. hinzii isolates cultured from blood and stool over 45 months revealed a clonal lineage that had undergone extensive within-host genetic and phenotypic diversification. Twenty of 24 isolates shared an E9G substitution in the DNA polymerase III ε-subunit active site, resulting in a proofreading deficiency. Within this proofreading-deficient clade, multiple lineages with mutations in DNA repair genes and altered mutational spectra emerged and dominated clinical cultures for more than 12 months. Multiple enzymes of the tricarboxylic acid cycle and gluconeogenesis pathways were repeatedly mutated, suggesting rapid metabolic adaptation to the human environment. Furthermore, an excess of G:C > T:A transversions suggested that oxidative stress shaped genetic diversification during adaptation. We propose that inactivation of DNA proofreading activity in combination with prolonged, but sub-lethal, oxidative attack resulting from the underlying host immunodeficiency facilitated rapid genomic adaptation. These findings suggest a fundamental role for host immune phenotype in shaping pathogen evolution following zoonotic infection.

Suggested Citation

  • A. Launay & C.-J. Wu & A. Dulanto Chiang & J.-H. Youn & P. P. Khil & J. P. Dekker, 2021. "In vivo evolution of an emerging zoonotic bacterial pathogen in an immunocompromised human host," Nature Communications, Nature, vol. 12(1), pages 1-12, December.
  • Handle: RePEc:nat:natcom:v:12:y:2021:i:1:d:10.1038_s41467-021-24668-7
    DOI: 10.1038/s41467-021-24668-7
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