Microorganisms (Apr 2021)

Phage Resistance Is Associated with Decreased Virulence in KPC-Producing <i>Klebsiella pneumoniae</i> of the Clonal Group 258 Clade II Lineage

  • Lucia Henrici De Angelis,
  • Noemi Poerio,
  • Vincenzo Di Pilato,
  • Federica De Santis,
  • Alberto Antonelli,
  • Maria Cristina Thaller,
  • Maurizio Fraziano,
  • Gian Maria Rossolini,
  • Marco Maria D’Andrea

DOI
https://doi.org/10.3390/microorganisms9040762
Journal volume & issue
Vol. 9, no. 4
p. 762

Abstract

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Phage therapy is now reconsidered with interest in the treatment of bacterial infections. A major piece of information for this application is the definition of the molecular targets exploited by phages to infect bacteria. Here, the genetic basis of resistance to the lytic phage φBO1E by its susceptible host Klebsiella pneumoniae KKBO-1 has been investigated. KKBO-1 phage-resistant mutants were obtained by infection at high multiplicity. One mutant, designated BO-FR-1, was selected for subsequent experiments, including virulence assessment in a Galleria mellonella infection model and characterization by whole-genome sequencing. Infection with BO-FR-1 was associated with a significantly lower mortality when compared to that of the parental strain. The BO-FR-1 genome differed from KKBO-1 by a single nonsense mutation into the wbaP gene, which encodes a glycosyltransferase involved in the first step of the biosynthesis of the capsular polysaccharide (CPS). Phage susceptibility was restored when BO-FR-1 was complemented with the constitutive wbaP gene. Our results demonstrated that φBO1E infects KKBO-1 targeting the bacterial CPS. Interestingly, BO-FR-1 was less virulent than the parental strain, suggesting that in the context of the interplay among phage, bacterial pathogen and host, the emergence of phage resistance may be beneficial for the host.

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