Within-host genotypic and phenotypic diversity of contemporaneous carbapenem-resistant <i>Klebsiella pneumoniae</i> from blood cultures of patients with bacteremia

Cheng, Shaoji; Fleres, Giuseppe; Chen, Liang; Liu, Guonjun; Hao, Binghua; Newbrough, Anthony; Driscoll, Eileen; Shields, Ryan K.; Squires, Kevin; Chu, Tingyu; Kreiswirth, Barry N.; Nguyen, M. Hong; Clancy, Cornelius J.

doi:10.1101/2022.05.26.493675

Cited by 1 publication

(1 citation statement)

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“…Repeating this work in other hospitals would provide valuable insights as to drivers of infection and resistance since S. aureus incidence can vary substantially within and between countries, and population structures such as dominant lineages vary geographically [25]. In particular, extending into adult populations and comparing hospitals with overlapping patient networks would improve generalisability, understanding how such diversity may be transmitted across hospital networks, as well as expanding to other key clinical pathogens [61][62][63][64][65].…”

Section: Implications and Next Stepsmentioning

confidence: 99%

Quantifying patient- and hospital-level antimicrobial resistance dynamics inStaphylococcus aureusfrom routinely collected data

Leclerc

Clements

Dunn

et al. 2023

Preprint

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Antimicrobial resistance (AMR) to all antibiotic classes has been found in the pathogenStaphylococcus aureus. The reported prevalence of these resistances vary, driven by within-host AMR evolution at the patient level, and between-host transmission at the hospital level. Without dense longitudinal sampling, pragmatic analysis of AMR dynamics at multiple levels using routine surveillance data is essential to inform control measures. We exploredS. aureusAMR diversity in 70,000 isolates from a UK paediatric hospital between 2000-2020, using electronic datasets containing multiple routinely collected isolates per patient with phenotypic antibiograms, hospitalisation information, and antibiotic consumption. At the hospital-level, the proportion of isolates that were meticillin-resistant (MRSA) increased between 2014-2020 from 25 to 50%, before sharply decreasing to 30%, likely due to a change in inpatient demographics. Temporal trends in the proportion of isolates resistant to different antibiotics were often correlated in MRSA, but independent in meticillin-susceptibleS. aureus. Ciprofloxacin resistance in MRSA decreased from 70% to 40% of tested isolates between 2007-2020, likely linked to a national policy to reduce fluoroquinolone usage in 2007. At the patient level, we identified frequent AMR diversity, with 4% of patients ever positive forS. aureussimultaneously carrying, at some point, multiple isolates with different resistances. We detected changes over time in AMR diversity in 3% of patients ever positive forS. aureus. These changes equally represented gain and loss of resistance. Within this routinely collected dataset, we found that 65% of changes in resistance within a patient'sS. aureuspopulation could not be explained by antibiotic exposure or between-patient transmission of bacteria, suggesting that within-host evolution via frequent gain and loss of AMR genes may be responsible for these changing AMR profiles. Our study highlights the value of exploring existing routine surveillance data to determine underlying mechanisms of AMR. These insights may substantially improve our understanding of the importance of antibiotic exposure variation, and the success of singleS. aureusclones.

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